U.S. patent application number 12/166145 was filed with the patent office on 2009-09-10 for phosphonate compounds having immuno-modulatory activity.
Invention is credited to Carina Cannizzaro, James M. Chen, Xiaowu Chen, Aesop Cho, Lee S. Chong, Manoj Desai, Maria Fardis, Alan X. Huang, Thorsten Kirschberg, Christopher P. Lee, Richard L. Mackman, Peter H. Nelson, Hyung-Jung Pyun, Adrian S. Ray, Sundaramoorthi Swaminathan, William J. Watkins, Jennifer R. Zhang.
Application Number | 20090227543 12/166145 |
Document ID | / |
Family ID | 35800745 |
Filed Date | 2009-09-10 |
United States Patent
Application |
20090227543 |
Kind Code |
A1 |
Cannizzaro; Carina ; et
al. |
September 10, 2009 |
PHOSPHONATE COMPOUNDS HAVING IMMUNO-MODULATORY ACTIVITY
Abstract
The invention is related to phosphonate substituted compounds
having immuno-modulatory activity, compositions containing such
compounds, and therapeutic methods that include the administration
of such compounds, as well as to processes and intermediates useful
for preparing such compounds.
Inventors: |
Cannizzaro; Carina; (San
Mateo, CA) ; Chen; James M.; (San Ramon, CA) ;
Chen; Xiaowu; (San Mateo, CA) ; Cho; Aesop;
(Mountain View, CA) ; Chong; Lee S.; (Newark,
CA) ; Desai; Manoj; (Pleasant Hill, CA) ;
Fardis; Maria; (San Carlos, CA) ; Huang; Alan X.;
(San Mateo, CA) ; Kirschberg; Thorsten; (Belmont,
CA) ; Lee; Christopher P.; (San Francisco, CA)
; Mackman; Richard L.; (Millbrae, CA) ; Nelson;
Peter H.; (Los Altos, CA) ; Pyun; Hyung-Jung;
(freemont, CA) ; Ray; Adrian S.; (San Mateo,
CA) ; Watkins; William J.; (Sunnyvale, CA) ;
Zhang; Jennifer R.; (Foster City, CA) ; Swaminathan;
Sundaramoorthi; (Burlingame, CA) |
Correspondence
Address: |
VIKSNINS HARRIS & PADYS PLLP
P.O BOX 111098
St. Paul
MN
55111-1098
US
|
Family ID: |
35800745 |
Appl. No.: |
12/166145 |
Filed: |
July 1, 2008 |
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Current U.S.
Class: |
514/100 ;
549/220 |
Current CPC
Class: |
A61K 47/542 20170801;
A61K 47/548 20170801 |
Class at
Publication: |
514/100 ;
549/220 |
International
Class: |
A61K 31/665 20060101
A61K031/665; C07F 9/655 20060101 C07F009/655 |
Claims
1. A conjugate of formula: [DRUG]-(A.sup.0).sub.nn; wherein: DRUG
is a compound of formula 546: ##STR01112## nn is 1, 2 or 3; A.sup.0
is A.sup.1; A.sup.1 is: ##STR01113## A.sup.3 is: ##STR01114##
Y.sup.1 is independently O, S, N(R.sup.x), N(O)(R.sup.x),
N(OR.sup.x), N(O)(OR.sup.x), or N(N(R.sup.x)(R.sup.x)); Y.sup.2 is
independently a bond, O, N(R.sup.x), N(O)(R.sup.x), N(OR.sup.x),
N(O)(OR.sup.x), N(N(R.sup.x)(R.sup.x)), --S(O).sub.M2--, or
--S(O).sub.M2--S(O).sub.M2--; and when Y.sup.2 joins two
phosphorous atoms Y.sup.2 can also be C(R.sup.2)(R.sup.2); R.sup.x
is H; R.sup.1 is independently H or alkyl of 1 to 18 carbon atoms;
R.sup.2 is independently H, R.sup.1, R.sup.3 or R.sup.4 wherein
each R.sup.4 is independently substituted with 0 to 3 R.sup.3
groups or taken together at a carbon atom, two R.sup.2 groups form
a ring of 3 to 8 carbons and the ring may be substituted with 0 to
3 R.sup.3 groups; R.sup.3 is R.sup.3a, R.sup.3b, R.sup.3c or
R.sup.3d, provided that when R.sup.3 is bound to a heteroatom, then
R.sup.3 is R.sup.3c or R.sup.3d; R.sup.3a is F, Cl, Br, I, --CN,
N.sub.3 or --NO.sub.2; R.sup.3b is Y.sup.1; R.sup.3c is --R.sup.x,
--N(R.sup.x)(R.sup.x), --SR.sup.x, --S(O)R.sup.x,
--S(O).sub.2R.sup.x, --S(O)(OR.sup.x), --S(O).sub.2(OR.sup.x),
--OC(Y.sup.1)R.sup.x, --OC(Y.sup.1)OR.sup.x,
--OC(Y.sup.1)(N(R.sup.x)(R.sup.x)), --SC(Y.sup.1)R.sup.x,
--SC(Y.sup.1)OR.sup.x, --SC(Y.sup.1)(N(R.sup.x)(R.sup.x)),
--N(R.sup.x)C(Y.sup.1)R.sup.x, --N(R.sup.x)C(Y.sup.1)OR.sup.x, or
--N(R.sup.x)C(Y.sup.1)(N(R.sup.x)(R.sup.x)); R.sup.3d is
--C(Y.sup.1)R.sup.x, --C(Y.sup.1)OR.sup.x or
--C(Y.sup.1)(N(R.sup.x)(R.sup.x)); R.sup.4 is an alkyl of 1 to 18
carbon atoms, alkenyl of 2 to 18 carbon atoms, or alkynyl of 2 to
18 carbon atoms; R.sup.5 is R.sup.4 wherein each R.sup.4 is
substituted with 0 to 3 R.sup.3 groups; W.sup.3 is W.sup.4 or
W.sup.1; W.sup.4 is R.sup.5, --C(Y.sup.1)R.sup.5,
--C(Y.sup.1)W.sup.5, --SO.sub.M2R.sup.5, or --SO.sub.M2W.sup.5;
W.sup.5 is carbocycle wherein W.sup.5 is independently substituted
with 0 to 3 R.sup.2 groups; W.sup.6 is W.sup.3 independently
substituted with 1, 2, or 3 A3 groups; M2 is 0, 1 or 2; M12a is 1,
2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12; and M12b is 0, 1, 2, 3, 4, 5,
6, 7, 8, 9, 10, 11 or 12; or a pharmaceutically acceptable salt or
solvate thereof.
2. The conjugate of claim 1 wherein Y.sup.2 is O.
3. The conjugate of claim 1 wherein each A.sup.3 is of the formula:
##STR01115##
4. The conjugate of claim 1 wherein each A.sup.3 is of the formula:
##STR01116##
5. The conjugate of claim 1 wherein each A.sup.3 is of the formula:
##STR01117## wherein: Y.sup.1a is O or S; and Y.sup.2a is O,
N(R.sup.x) or S.
6. The conjugate of claim 1 wherein each A.sup.3 is of the formula:
##STR01118## wherein Y.sup.2b is O or N(R.sup.x).
7. The conjugate of claim 1 wherein each A.sup.3 is of the formula:
##STR01119## wherein: Y.sup.2b is O or N(R.sup.x); and M12d is 1,
2, 3, 4, 5, 6, 7 or 8.
8. The conjugate of claim 1 wherein each A.sup.3 is of the formula:
##STR01120## wherein: Y.sup.2b is O or N(R.sup.x); and M12d is 1,
2, 3, 4, 5, 6, 7 or 8.
9. The conjugate of claim 1, wherein each A.sup.3 is of the
formula: ##STR01121##
10. The conjugate of claim 1 wherein A.sup.0 is of the formula:
##STR01122## wherein each R is independently alkyl.
11. A pharmaceutical composition comprising a pharmaceutical
excipient and a conjugate as described in claim 1, or a
pharmaceutically acceptable salt or solvate thereof.
Description
[0001] This non-provisional application claims the benefit of
priority under 35 U.S.C. .sctn. 119(e) from U.S. Provisional Patent
Application Ser. Nos. 60/465,424, 60/465,373, 60/465,420,
60/465,380, 60/465,433, 60/465,481, 60/465,377, 60/465,581,
60/465,532, 60/465,844, 60/465,531, and 60/465,574, all filed Apr.
25, 2003; and to U.S. Provisional Patent Application Ser. Nos.
60/493,303, 60/493,310, 60/493,309, and 60/493,302, all filed Aug.
7, 2003; and to U.S. Provisional Patent Application Ser. Nos.
60/495,533, 60/495,529, 60/495,455, 60/495,537, 60/495,456,
60/495,398, 60/495,425, 60/495,427, 60/495,661, 60/495,393,
60/495,416, 60/495,614, and 60/495,417, all filed Aug. 15, 2003;
and to U.S. Provisional Patent Application Ser. Nos. 60/514,054,
60/513,971, 60/514,394, 60/513,975, 60/514,453, 60/514,202,
60/513,948, 60/514,424, 60/514,280, 60/514,144, 60/513,979,
60/514,075, 60/513,946, 60/514,051, 60/514,161, 60/514,325,
60/514,044, 60/514,201, 60/514,522, 60/514,140, 60/514,175,
60/514,113, 60/513,562, 60/513,592, 60/513,563, 60/513,579,
60/513,561, 60/513,589, 60/513,593, 60/513,588, 60/514,258,
60/514,021, and 60/514,298, all filed Oct. 24, 2003; and to U.S.
Provisional Patent Application Ser. Nos. 60/532,230, 60/531,960,
60/532,160, 60/531,940, and 60/531,932, all filed Dec. 1, 2003; and
to U.S. Provisional Patent Application Ser. No. 60/532,591, filed
Dec. 23, 2003; and to U.S. Provisional Patent Application Ser. No.
60/536,005, filed Jan. 12, 2004. The entirety of all Provisional
Applications listed above are incorporated herein by reference.
FIELD OF THE INVENTION
[0002] The invention relates generally to compounds with
immuno-modulatory (e.g., immunosuppressant) activity.
BACKGROUND OF THE INVENTION
[0003] Improving the delivery of drugs and other agents to target
cells and tissues has been the focus of considerable research for
many years. Though many attempts have been made to develop
effective methods for importing biologically active molecules into
cells, both in vivo and in vitro, none has proved to be entirely
satisfactory. Optimizing the association of the inhibitory drug
with its intracellular target, while minimizing intercellular
redistribution of the drug, e.g., to neighboring cells, is often
difficult or inefficient.
[0004] Most agents currently administered to a patient parenterally
are not targeted, resulting in systemic delivery of the agent to
cells and tissues of the body where it is unnecessary, and often
undesirable. This may result in adverse drug side effects, and
often limits the dose of a drug (e.g., glucocorticoids and other
anti-inflammatory drugs) that can be administered. By comparison,
although oral administration of drugs is generally recognized as a
convenient and economical method of administration, oral
administration can result in either (a) uptake of the drug through
the cellular and tissue barriers, e.g., blood/brain, epithelial,
cell membrane, resulting in undesirable systemic distribution, or
(b) temporary residence of the drug within the gastrointestinal
tract. Accordingly, a major goal has been to develop methods for
specifically targeting agents to cells and tissues. Benefits of
such treatment includes avoiding the general physiological effects
of inappropriate delivery of such agents to other cells and
tissues, such as uninfected cells.
[0005] Autoimmune diseases and transplantation rejection remain
major public health problems worldwide. Although drugs with
immunosuppressive activity are in wide use and have shown
effectiveness, there clinical usefulness has been limited due to
their toxicity and other side effects. Currently there is a need
for new immunosuppressant agents, i.e. drugs, having improved
immunosuppressant activity and pharmacokinetic properties, improved
oral bioavailability, greater potency, and extended effective
half-life in vivo. New immunosuppressant agents should have fewer
side effects, less complicated dosing schedules, and/or be orally
active.
SUMMARY OF THE INVENTION
[0006] Intracellular targeting may be achieved by methods and
compositions that allow accumulation or retention of biologically
active agents inside cells. The present invention provides novel
phosphonate containing analogs of immuno-modulatory (e.g.,
immunosuppressant) compounds. These compounds possess the utilities
of the related immuno-modulatory compounds, but due to the presence
of the phosphonate group(s) they typically provide cellular
accumulation of the phosphonate compound. Thus, compounds of the
invention may demonstrate improved immuno-modulatory properties,
pharmacokinetic properties, oral bioavailability, potency, or
extended effective half-life in vivo, or a combination thereof. The
compounds of the invention may also have distinct resistance
profiles, fewer side effects, less complicated dosing schedules, or
have increased oral activity.
[0007] The present invention relates generally to the accumulation
or retention of therapeutic compounds inside cells. The invention
is more particularly related to attaining high concentrations of
phosphonate-containing molecules in target cells. Such effective
targeting may be applicable to a variety of therapeutic
formulations and procedures.
[0008] Accordingly, in one embodiment the invention provides a
compound of the invention which is a conjugate comprising an
immuno-modulatory compound (e.g., an immunosuppressant compound)
linked to one or more phosphonate groups.
[0009] Compositions of the invention include immuno-modulatory
compounds having at least one phosphonate group. Accordingly, in
one embodiment the invention provides a conjugate comprising an
immuno-modulatory compound (e.g., an immunosuppressant compound)
linked to one or more phosphonate groups or a pharmaceutically
acceptable salt thereof.
[0010] In another embodiment the invention provides a compound of
any one of formulae 500-547:
##STR00001## ##STR00002## ##STR00003## ##STR00004## ##STR00005##
##STR00006##
[0011] that is substituted with one or more phosphonate groups
either directly or indirectly through a linker; and that is
optionally substituted with one or more groups A.sup.0; or a
pharmaceutically acceptable salt thereof, wherein:
[0012] A.sup.0 is A.sup.1, A.sup.2 or W.sup.3 with the proviso that
the conjugate includes at least one A.sup.1;
[0013] A.sup.1 is:
##STR00007##
[0014] A.sup.2 is:
##STR00008##
[0015] A.sup.3 is:
##STR00009##
[0016] Y.sup.1 is independently O, S, N(R.sup.x), N(O)(R.sup.x),
N(OR.sup.x), N(O)(OR.sup.x), or N(N(R.sup.x)(R.sup.x));
[0017] Y.sup.2 is independently a bond, O, N(R.sup.x),
N(O)(R.sup.x), N(OR.sup.x), N(O)(OR.sup.x), N(N(R.sup.x)(R.sup.x)),
--S(O).sub.M2--, or --S(O).sub.M2--S(O).sub.M2--; and when Y.sup.2
joins two phosphorous atoms Y.sup.2 can also be
C(R.sup.2)(R.sup.2);
[0018] R.sup.x is independently H, R.sup.1, R.sup.2, W.sup.3, a
protecting group, or the formula:
##STR00010##
[0019] wherein:
[0020] R.sup.y is independently H, W.sup.3, R.sup.2 or a protecting
group;
[0021] R.sup.1 is independently H or alkyl of 1 to 18 carbon
atoms;
[0022] R.sup.2 is independently H, R.sup.1, R.sup.3 or R.sup.4
wherein each R.sup.4 is independently substituted with 0 to 3
R.sup.3 groups or taken together at a carbon atom, two R.sup.2
groups form a ring of 3 to 8 carbons and the ring may be
substituted with 0 to 3 R.sup.3 groups;
[0023] R.sup.3 is R.sup.3a, R.sup.3b, R.sup.3c or R.sup.3d,
provided that when R.sup.3 is bound to a heteroatom, then R.sup.3
is R.sup.3c or R.sup.3d;
[0024] R.sup.3a is F, Cl, Br, I, --CN, N.sub.3 or --NO.sub.2;
[0025] R.sup.3b is Y.sup.1;
[0026] R.sup.3c is R.sup.x, N(R.sup.x)(R.sup.x), --SR.sup.x,
--S(O)R.sup.x, --S(O).sub.2R.sup.x, --S(O)(OR.sup.x),
--S(O).sub.2(OR.sup.x), --OC(Y.sup.1)R.sup.x,
--OC(Y.sup.1)OR.sup.x, --OC(Y.sup.1)(N(R.sup.x)(R.sup.x)),
--SC(Y.sup.1)R.sup.x, --SC(Y.sup.1)OR.sup.x,
--SC(Y.sup.x)(N(R.sup.x)(R.sup.x)), --N(R.sup.x)C(Y.sup.1)R.sup.x,
--N(R.sup.x)C(Y.sup.1)OR.sup.x, or
--N(R.sup.x)C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0027] R.sup.3d is --C(Y.sup.1)R.sup.x, --C(Y.sup.1)OR.sup.x or
--C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0028] R.sup.4 is an alkyl of 1 to 18 carbon atoms, alkenyl of 2 to
18 carbon atoms, or alkynyl of 2 to 18 carbon atoms;
[0029] R.sup.5 is R.sup.4 wherein each R.sup.4 is substituted with
0 to 3 R.sup.3 groups;
[0030] W.sup.3 is W.sup.4 or W.sup.5;
[0031] W.sup.4 is R.sup.5, --C(Y.sup.1)R.sup.5,
--C(Y.sup.1)W.sup.5, --SO.sub.M2R.sup.5, or --SO.sub.M2W.sup.5;
[0032] W.sup.5 is carbocycle or heterocycle wherein W.sup.5 is
independently substituted with 0 to 3 R.sup.2 groups;
[0033] W.sup.6 is W.sup.3 independently substituted with 1, 2, or 3
A.sup.3 groups;
[0034] M2 is 0, 1 or 2;
[0035] M12a is 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0036] M12b is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0037] M1a, M1c, and M1d are independently 0 or 1; and
[0038] M12c is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12.
[0039] In another embodiment the invention provides a compound of
the formula:
[DRUG]-(A.sup.0).sub.nn
or a pharmaceutically acceptable salt thereof wherein;
[0040] DRUG is a compound of any one of formulae 500-547;
[0041] nn is 1, 2, or 3;
wherein:
[0042] A.sup.0 is A.sup.1, A.sup.2 or W.sup.3 with the proviso that
the conjugate includes at least one A.sup.1;
[0043] A.sup.1 is:
##STR00011##
[0044] A.sup.2 is:
##STR00012##
[0045] A.sup.3 is:
##STR00013##
[0046] Y.sup.1 is independently O, S, N(R.sup.x), N(O)(R.sup.x),
N(OR.sup.x), N(O)(OR.sup.x), or N(N(R.sup.x)(R.sup.x));
[0047] Y.sup.2 is independently a bond, O, N(R.sup.x),
N(O)(R.sup.x), N(OR.sup.x), N(O)(OR.sup.x), N(N(R.sup.x)(R.sup.x)),
--S(O).sub.M2--, or --S(O).sub.M2--S(O).sub.M2--; and when Y.sup.2
joins two phosphorous atoms Y.sup.2 can also be
C(R.sup.2)(R.sup.2);
[0048] R.sup.x is independently H, R.sup.1, R.sup.2, W.sup.3, a
protecting group, or the formula:
##STR00014##
[0049] wherein:
[0050] R.sup.y is independently H, W.sup.3, R.sup.2 or a protecting
group;
[0051] R.sup.1 is independently H or alkyl of 1 to 18 carbon
atoms;
[0052] R.sup.2 is independently H, R.sup.1, R.sup.3 or R.sup.4
wherein each R.sup.4 is independently substituted with 0 to 3
R.sup.3 groups or taken together at a carbon atom, two R.sup.2
groups form a ring of 3 to 8 carbons and the ring may be
substituted with 0 to 3 R.sup.3 groups;
[0053] R.sup.3 is R.sup.3a, R.sup.3b, R.sup.3c or R.sup.3d,
provided that when R.sup.3 is bound to a heteroatom, then R.sup.3
is R.sup.3c or R.sup.3d;
[0054] R.sup.3a is F, Cl, Br, I, --CN, N.sub.3 or --NO.sub.2;
[0055] R.sup.3b is Y;
[0056] R.sup.3c is R.sup.x, --N(R.sup.x)(R.sup.x), --SR.sup.x,
--S(O)R.sup.x, --S(O).sub.2R.sup.x, --S(O)(OR.sup.x),
--S(O).sub.2(OR.sup.x), --OC(Y.sup.1)R.sup.x,
--OC(Y.sup.1)OR.sup.x, --OC(Y.sup.1)(N(R.sup.x)(R.sup.x)),
--SC(Y.sup.1)R.sup.x, --SC(Y.sup.1)OR.sup.x,
--SC(Y.sup.1)(N(R.sup.x)(R.sup.x)), --N(R.sup.x)C(Y.sup.1)R.sup.x,
N(R.sup.x)C(Y.sup.1)OR.sup.x, or
--N(R.sup.x)C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0057] R.sup.3d is --C(Y.sup.1)R.sup.x, --C(Y.sup.1)OR.sup.x or
--C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0058] R.sup.4 is an alkyl of 1 to 18 carbon atoms, alkenyl of 2 to
18 carbon atoms, or alkynyl of 2 to 18 carbon atoms;
[0059] R.sup.5 is R.sup.4 wherein each R.sup.4 is substituted with
0 to 3 R.sup.3 groups;
[0060] W.sup.3 is W.sup.4 or W.sup.5;
[0061] W.sup.4 is R.sup.5, --C(Y.sup.1)R.sup.5,
--C(Y.sup.1)W.sup.5, --SO.sub.M2R.sup.5, or --SO.sub.M2W.sup.5;
[0062] W.sup.5 is carbocycle or heterocycle wherein W.sup.5 is
independently substituted with 0 to 3 R.sup.2 groups;
[0063] W.sup.6 is W.sup.3 independently substituted with 1, 2, or 3
A.sup.3 groups;
[0064] M2 is 0, 1 or 2;
[0065] M12a is 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0066] M12b is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0067] M1a, M1c, and M1d are independently 0 or 1; and
[0068] M12c is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12.
[0069] In another embodiment the invention provides a compound of
any one of formulae 1-151:
##STR00015## ##STR00016## ##STR00017## ##STR00018## ##STR00019##
##STR00020## ##STR00021## ##STR00022## ##STR00023## ##STR00024##
##STR00025## ##STR00026## ##STR00027## ##STR00028##
##STR00029##
wherein:
[0070] A.sup.0 is A.sup.1;
[0071] A.sup.1 is:
##STR00030##
[0072] A.sup.3 is:
##STR00031##
[0073] Y.sup.1 is independently O, S, N(R.sup.x), N(O)(R.sup.x),
N(OR.sup.x), N(O)(OR.sup.x), or N(N(R.sup.x)(R.sup.x));
[0074] Y.sup.2 is independently a bond, O, N(R.sup.x),
N(O)(R.sup.x), N(OR.sup.x), N(O)(OR.sup.x), N(N(R.sup.x)(R.sup.x)),
--S(O).sub.M2--, or --S(O).sub.M2--S(O).sub.M2--; and when Y.sup.2
joins two phosphorous atoms Y.sup.2 can also be
C(R.sup.2)(R.sup.2);
[0075] R.sup.x is independently H, R.sup.2, W.sup.3, a protecting
group, or the formula:
##STR00032##
[0076] R.sup.y is independently H, W.sup.3, R.sup.2 or a protecting
group;
[0077] R.sup.1 is independently H or alkyl of 1 to 18 carbon
atoms;
[0078] R.sup.2 is independently H, R.sup.3 or R.sup.4 wherein each
R.sup.4 is independently substituted with 0 to 3 R.sup.3
groups;
[0079] R.sup.3 is R.sup.3a, R.sup.3b, R.sup.3c or R.sup.3d,
provided that when R.sup.3 is bound to a heteroatom, then R.sup.3
is R.sup.3c or R.sup.3d;
[0080] R.sup.3a is F, Cl, Br, I, --CN, N.sub.3 or --NO.sub.2;
[0081] R.sup.3b is Y.sup.1;
[0082] R.sup.3c is R.sup.x, N(R.sup.x)(R.sup.x), --SR.sup.x,
--S(O)R.sup.x, --S(O).sub.2R.sup.x, --S(O)(OR.sup.x),
--S(O).sub.2(OR.sup.x), --OC(Y.sup.1)R.sup.x,
--OC(Y.sup.1)OR.sup.x, --OC(Y.sup.1)(N(R.sup.x)(R.sup.x)),
--SC(Y.sup.1)R.sup.x, SC(Y.sup.1)OR.sup.x,
--SC(Y.sup.1)(N(R.sup.x)(R.sup.x)), --N(R.sup.x)C(Y.sup.1)R.sup.x,
--N(R.sup.x)C(Y.sup.1)OR.sup.x, or
--N(R.sup.x)C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0083] R.sup.3d is --C(Y.sup.1)R.sup.x, --C(Y.sup.1)OR.sup.x or
--C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0084] R.sup.4 is an alkyl of 1 to 18 carbon atoms, alkenyl of 2 to
18 carbon atoms, or alkynyl of 2 to 18 carbon atoms;
[0085] R.sup.5 is R.sup.4 wherein each R.sup.4 is substituted with
0 to 3 R.sup.3 groups;
[0086] R.sup.5a is independently alkylene of 1 to 18 carbon atoms,
alkenylene of 2 to 18 carbon atoms, or alkynylene of 2-18 carbon
atoms any one of which alkylene, alkenylene or alkynylene is
substituted with 0-3 R.sup.3 groups;
[0087] W.sup.3 is W.sup.4 or W.sup.5;
[0088] W.sup.4 is R.sup.5, --C(Y.sup.1)R.sup.5,
--C(Y.sup.1)W.sup.5, --SO.sub.2R.sup.5, or --SO.sub.2W.sup.5;
[0089] W.sup.5 is carbocycle or heterocycle wherein W.sup.5 is
independently substituted with 0 to 3 R.sup.2 groups;
[0090] W.sup.6 is W.sup.3 independently substituted with 1, 2, or 3
A.sup.3 groups;
[0091] M2 is 0, 1 or 2;
[0092] M12a is 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0093] M12b is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0094] M1a, M1c, and M1d are independently 0 or 1;
[0095] M12c is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0096] each X.sup.50 is independently hydrogen, F, Cl, CF.sub.3,
CN, methyl, or tert-butyl;
[0097] X.sup.51 is hydrogen, halo, trifluoromethyl, (C1-C3)alkyl,
cyano, or (C1-C3)alkoxy;
[0098] X.sup.52 is hydrogen, fluoro, chloro, bromo, methyl, or
trifluoromethyl;
[0099] X.sup.53 is --O--, or --S--;
[0100] X.sup.54 and X.sup.55 are independently selected from
hydrogen or a C.sub.1-C.sub.18 acyl;
[0101] X.sup.56 is hydrogen, a C.sub.1-C.sub.18 acyl, or
##STR00033##
[0102] or X.sup.54 is hydrogen and together X.sup.55 and X.sup.56
are
##STR00034##
[0103] X.sup.57 is H, amino, hydroxy, or a halogen selected from Cl
and Br;
[0104] X.sup.58 is hydrogen, F, Cl, CF3, cyano, methyl, or
t-butyl;
[0105] X.sup.59 is hydrogen, CH.sub.2OH;
[0106] X.sup.60 is
CO(CH.sub.2).sub.6CONMe(CH.sub.2)2.sub.sO.sub.3H;
[0107] X.sup.62 is methyl, chloro, or trifluoromethyl;
[0108] X.sup.63 is H, methyl, ethyl, cyclopropyl, vinyl, or
trifluoromethyl;
[0109] X.sup.64 is H, methyl, ethyl, cyclopropyl, chloro, vinyl,
allyl, 3-methyl-1-buten-1-yl;
[0110] X.sup.65 is hydrogen or F; and
[0111] Ar is aryl or heteroaryl.
[0112] The invention provides a pharmaceutical composition
comprising an effective amount of a compound of the invention, or a
pharmaceutically acceptable salt thereof, in combination with a
pharmaceutically acceptable diluent or carrier.
[0113] This invention pertains to a method of increasing cellular
accumulation and retention of drug compounds, thus improving their
therapeutic and diagnostic value, comprising linking the compound
to one or more phosphonate groups.
[0114] The invention also provides a method for the maintenance of
immunosuppression, for example, following transplant surgery,
comprising administering to an animal (e.g. a mammal) an effective
amount of a compound of the invention.
[0115] The invention also provides a method for modulating an
immune response in vitro or in vivo comprising contacting a sample
in need of such treatment with a compound of the invention.
[0116] The invention also provides a method of inhibiting an immune
response in an animal (e.g. a mammal), comprising administering an
effective amount of a compound of the invention to the animal.
[0117] The invention also provides a method of treating the
symptoms or effects of an autoimmune disease (e.g. psoriasis,
rheumatoid arthritis, lupus erythematosus, multiple sclerosis,
diabetes, Chron's disease, etc.) in an animal (e.g. a mammal),
comprising administering an effective amount of a compound of the
invention to the animal.
[0118] The invention also provides a method of treating the
symptoms or effects of transplant rejection in an animal (e.g. a
mammal), comprising administering an effective amount of a compound
of the invention to the animal.
[0119] The invention also provides a method for inhibiting the
proliferation of human T cells and/or downregulating the production
of Th1 or Th2 type cytokines in an animal (e.g. a mammal)
comprising administering a compound of the invention to the
animal.
[0120] The invention also provides a method for treating atopic
dermatitis in an animal (e.g. a mammal), comprising administering
an effective amount of a compound of the invention to the
animal.
[0121] The invention also provides a method for inhibiting one or
more T-lymphocyte functions in an animal (e.g. a mammal),
comprising administering an effective amount of a compound of the
invention to the animal.
[0122] The invention also provides a method for inhibiting
dihydroorotate dehydrogenase in an animal (e.g. a mammal),
comprising administering an effective amount of a compound of the
invention to the animal.
[0123] The invention also provides a compound of the invention for
use in medical therapy (preferably for use in the maintenance of
immunosuppression following transplant surgery, inhibiting an
immune response, treating an autoimmune disease, treating atopic
dermatitis, inhibiting the proliferation of human T cells, or
downregulating the production of Th1 or Th2 type cytokines), as
well as the use of a compound of the invention for the manufacture
of a medicament useful for maintenance of immunosuppression
following transplant surgery in an animal (e.g. a mammal). The
invention also provides the use of a compound of the invention for
the manufacture of a medicament useful for inhibiting an immune
response in an animal (e.g. a mammal). The invention also provides
the use of a compound of the invention for the manufacture of a
medicament useful for treating an autoimmune disease in an animal
(e.g. a mammal). The invention also provides the use of a compound
of the invention for the manufacture of a medicament useful for
inhibiting the proliferation of human T cells or downregulating the
production of Th1 or Th2 type cytokines in an animal.
[0124] The invention also provides a method for the maintenance of
immunosuppression, for example, following transplant surgery,
comprising administering to an animal (e.g., a mammal) an effective
amount of a compound of the invention.
[0125] The invention also provides processes and novel
intermediates disclosed herein which are useful for preparing
compounds of the invention. Some of the compounds of the invention
are useful to prepare other compounds of the invention.
DETAILED DESCRIPTION OF THE INVENTION
[0126] Reference will now be made in detail to certain claims of
the invention, examples of which are illustrated in the
accompanying structures and formulas. While the invention will be
described in conjunction with the enumerated claims, it will be
understood that they are not intended to limit the invention to
those claims. On the contrary, the invention is intended to cover
all alternatives, modifications, and equivalents, which may be
included within the scope of the present invention as defined by
the claims.
DEFINITIONS
[0127] Unless stated otherwise, the following terms and phrases as
used herein are intended to have the following meanings:
[0128] When tradenames are used herein, applicants intend to
independently include the tradename product and the active
pharmaceutical ingredient(s) of the tradename product.
[0129] "Bioavailability" is the degree to which the
pharmaceutically active agent becomes available to the target
tissue after the agent's introduction into the body. Enhancement of
the bioavailability of a pharmaceutically active agent can provide
a more efficient and effective treatment for patients because, for
a given dose, more of the pharmaceutically active agent will be
available at the targeted tissue sites.
[0130] The terms "phosphonate" and "phosphonate group" include
functional groups or moieties within a molecule that comprises a
phosphorous that is 1) single-bonded to a carbon, 2) double-bonded
to a heteroatom, 3) single-bonded to a heteroatom, and 4)
single-bonded to another heteroatom, wherein each heteroatom can be
the same or different. The terms "phosphonate" and "phosphonate
group" also include functional groups or moieties that comprise a
phosphorous in the same oxidation state as the phosphorous
described above, as well as functional groups or moieties that
comprise a prodrug moiety that can separate from a compound so that
the compound retains a phosphorous having the characteristics
described above. For example, the terms "phosphonate" and
"phosphonate group" include phosphonic acid, phosphonic monoester,
phosphonic diester, phosphonamidate, and phosphonthioate functional
groups. In one specific embodiment of the invention, the terms
"phosphonate" and "phosphonate group" include functional groups or
moieties within a molecule that comprises a phosphorous that is 1)
single-bonded to a carbon, 2) double-bonded to an oxygen, 3)
single-bonded to an oxygen, and 4) single-bonded to another oxygen,
as well as functional groups or moieties that comprise a prodrug
moiety that can separate from a compound so that the compound
retains a phosphorous having such characteristics. In another
specific embodiment of the invention, the terms "phosphonate" and
"phosphonate group" include functional groups or moieties within a
molecule that comprises a phosphorous that is 1) single-bonded to a
carbon, 2) double-bonded to an oxygen, 3) single-bonded to an
oxygen or nitrogen, and 4) single-bonded to another oxygen or
nitrogen, as well as functional groups or moieties that comprise a
prodrug moiety that can separate from a compound so that the
compound retains a phosphorous having such characteristics.
[0131] The term "prodrug" as used herein refers to any compound
that when administered to a biological system generates the drug
substance, i.e. active ingredient, as a result of spontaneous
chemical reaction(s), enzyme catalyzed chemical reaction(s),
photolysis, and/or metabolic chemical reaction(s). A prodrug is
thus a covalently modified analog or latent form of a
therapeutically-active compound.
[0132] "Prodrug moiety" refers to a labile functional group which
separates from the active inhibitory compound during metabolism,
systemically, inside a cell, by hydrolysis, enzymatic cleavage, or
by some other process (Bundgaard, Hans, "Design and Application of
Prodrugs" in A Textbook of Drug Design and Development (1991), P.
Krogsgaard-Larsen and H. Bundgaard, Eds. Harwood Academic
Publishers, pp. 113-191). Enzymes which are capable of an enzymatic
activation mechanism with the phosphonate prodrug compounds of the
invention include, but are not limited to, amidases, esterases,
microbial enzymes, phospholipases, cholinesterases, and
phosphotases. Prodrug moieties can serve to enhance solubility,
absorption and lipophilicity to optimize drug delivery,
bioavailability and efficacy. A prodrug moiety may include an
active metabolite or drug itself.
[0133] Exemplary prodrug moieties include the hydrolytically
sensitive or labile acyloxymethyl esters --CH.sub.2C(.dbd.O)R.sup.9
and acyloxymethyl carbonates --CH.sub.2C(.dbd.O)OR.sup.9 where
R.sup.9 is C.sub.1-C.sub.6 alkyl, C.sub.1-C.sub.6 substituted
alkyl, C.sub.6-C.sub.20 aryl or C.sub.6-C.sub.20 substituted aryl.
The acyloxyalkyl ester was first used as a prodrug strategy for
carboxylic acids and then applied to phosphates and phosphonates by
Farquhar et al. (1983) J. Pharm. Sci. 72: 324; also U.S. Pat. Nos.
4,816,570, 4,968,788, 5,663,159 and 5,792,756. Subsequently, the
acyloxyalkyl ester was used to deliver phosphonic acids across cell
membranes and to enhance oral bioavailability. A close variant of
the acyloxyalkyl ester, the alkoxycarbonyloxyalkyl ester
(carbonate), may also enhance oral bioavailability as a prodrug
moiety in the compounds of the combinations of the invention. An
exemplary acyloxymethyl ester is pivaloyloxymethoxy, (POM)
--CH.sub.2C(.dbd.O)C(CH.sub.3).sub.3. An exemplary acyloxymethyl
carbonate prodrug moiety is pivaloyloxymethylcarbonate
(POC)--CH.sub.2C(.dbd.O)OC(CH.sub.3).sub.3.
[0134] The phosphonate group may be a phosphonate prodrug moiety.
The prodrug moiety may be sensitive to hydrolysis, such as, but not
limited to a pivaloyloxymethyl carbonate (POC) or POM group.
Alternatively, the prodrug moiety may be sensitive to enzymatic
potentiated cleavage, such as a lactate ester or a
phosphonamidate-ester group.
[0135] Aryl esters of phosphorus groups, especially phenyl esters,
are reported to enhance oral bioavailability (De Lombaert et al.
(1994) J. Med. Chem. 37: 498). Phenyl esters containing a
carboxylic ester ortho to the phosphate have also been described
(Khamnei and Torrence, (1996) J. Med. Chem. 39:4109-4115). Benzyl
esters are reported to generate the parent phosphonic acid. In some
cases, substituents at the ortho- or para-position may accelerate
the hydrolysis. Benzyl analogs with an acylated phenol or an
alkylated phenol may generate the phenolic compound through the
action of enzymes, e.g., esterases, oxidases, etc., which in turn
undergoes cleavage at the benzylic C--O bond to generate the
phosphoric acid and the quinone methide intermediate. Examples of
this class of prodrugs are described by Mitchell et al. (1992) J.
Chem. Soc. Perkin Trans. II 2345; Glazier WO 91/19721. Still other
benzylic prodrugs have been described containing a carboxylic
ester-containing group attached to the benzylic methylene (Glazier
WO 91/19721). Thio-containing prodrugs are reported to be useful
for the intracellular delivery of phosphonate drugs. These
proesters contain an ethylthio group in which the thiol group is
either esterified with an acyl group or combined with another thiol
group to form a disulfide. Deesterification or reduction of the
disulfide generates the free thio intermediate which subsequently
breaks down to the phosphoric acid and episulfide (Puech et al.
(1993) Antiviral Res., 22: 155-174; Benzaria et al. (1996) J. Med.
Chem. 39: 4958). Cyclic phosphonate esters have also been described
as prodrugs of phosphorus-containing compounds (Erion et al., U.S.
Pat. No. 6,312,662).
[0136] "Protecting group" refers to a moiety of a compound that
masks or alters the properties of a functional group or the
properties of the compound as a whole. Chemical protecting groups
and strategies for protection/deprotection are well known in the
art. See e.g., Protective Groups in Organic Chemistry, Theodora W.
Greene, John Wiley & Sons, Inc., New York, 1991. Protecting
groups are often utilized to mask the reactivity of certain
functional groups, to assist in the efficiency of desired chemical
reactions, e.g., making and breaking chemical bonds in an ordered
and planned fashion. Protection of functional groups of a compound
alters other physical properties besides the reactivity of the
protected functional group, such as the polarity, lipophilicity
(hydrophobicity), and other properties which can be measured by
common analytical tools. Chemically protected intermediates may
themselves be biologically active or inactive.
[0137] Protected compounds may also exhibit altered, and in some
cases, optimized properties in vitro and in vivo, such as passage
through cellular membranes and resistance to enzymatic degradation
or sequestration. In this role, protected compounds with intended
therapeutic effects may be referred to as prodrugs. Another
function of a protecting group is to convert the parental drug into
a prodrug, whereby the parental drug is released upon conversion of
the prodrug in vivo. Because active prodrugs may be absorbed more
effectively than the parental drug, prodrugs may possess greater
potency in vivo than the parental drug. Protecting groups are
removed either in vitro, in the instance of chemical intermediates,
or in vivo, in the case of prodrugs. With chemical intermediates,
it is not particularly important that the resulting products after
deprotection, e.g., alcohols, be physiologically acceptable,
although in general it is more desirable if the products are
pharmacologically innocuous.
[0138] Any reference to any of the compounds of the invention also
includes a reference to a physiologically acceptable salt thereof.
Examples of physiologically acceptable salts of the compounds of
the invention include salts derived from an appropriate base, such
as an alkali metal (for example, sodium), an alkaline earth (for
example, magnesium), ammonium and NX.sub.4.sup.+ (wherein X is
C.sub.1-C.sub.4 alkyl). Physiologically acceptable salts of an
hydrogen atom or an amino group include salts of organic carboxylic
acids such as acetic, benzoic, lactic, fumaric, tartaric, maleic,
malonic, malic, isethionic, lactobionic and succinic acids; organic
sulfonic acids, such as methanesulfonic, ethanesulfonic,
benzenesulfonic and p-toluenesulfonic acids; and inorganic acids,
such as hydrochloric, sulfuric, phosphoric and sulfamic acids.
Physiologically acceptable salts of a compound of an hydroxy group
include the anion of said compound in combination with a suitable
cation such as Na.sup.+ and NX.sub.4.sup.+ (wherein X is
independently selected from H or a C.sub.1-C.sub.4 alkyl
group).
[0139] For therapeutic use, salts of active ingredients of the
compounds of the invention will be physiologically acceptable, i.e.
they will be salts derived from a physiologically acceptable acid
or base. However, salts of acids or bases which are not
physiologically acceptable may also find use, for example, in the
preparation or purification of a physiologically acceptable
compound. All salts, whether or not derived form a physiologically
acceptable acid or base, are within the scope of the present
invention.
[0140] "Alkyl" is C.sub.1-C.sub.18 hydrocarbon containing normal,
secondary, tertiary or cyclic carbon atoms. Examples are methyl
(Me, --CH.sub.3), ethyl (Et, --CH.sub.2CH.sub.3), 1-propyl (n-Pr,
n-propyl, --CH.sub.2CH.sub.2CH.sub.3), 2-propyl (i-Pr, i-propyl,
--CH(CH.sub.3).sub.2), 1-butyl (n-Bu, n-butyl,
--CH.sub.2CH.sub.2CH.sub.2CH.sub.3), 2-methyl-1-propyl (i-Bu,
i-butyl, --CH.sub.2CH(CH.sub.3).sub.2), 2-butyl (s-Bu, s-butyl,
--CH(CH.sub.3)CH.sub.2CH.sub.3), 2-methyl-2-propyl (t-Bu, t-butyl,
--C(CH.sub.3).sub.3), 1-pentyl (n-pentyl,
--CH.sub.2CH.sub.2CH.sub.2CH.sub.2CH.sub.3), 2-pentyl
(--CH(CH.sub.3)CH.sub.2CH.sub.2CH.sub.3), 3-pentyl
(--CH(CH.sub.2CH.sub.3).sub.2), 2-methyl-2-butyl
(--C(CH.sub.3).sub.2CH.sub.2CH.sub.3), 3-methyl-2-butyl
(--CH(CH.sub.3)CH(CH.sub.3).sub.2), 3-methyl-1-butyl
(--CH.sub.2CH.sub.2CH(CH.sub.3).sub.2), 2-methyl-1-butyl
(--CH.sub.2CH(CH.sub.3)CH.sub.2CH.sub.3), 1-hexyl
(--CH.sub.2CH.sub.2CH.sub.2CH.sub.2CH.sub.2CH.sub.3), 2-hexyl
(--CH(CH.sub.3)CH.sub.2CH.sub.2CH.sub.2CH.sub.3), 3-hexyl
(--CH(CH.sub.2CH.sub.3)(CH.sub.2CH.sub.2CH.sub.3)),
2-methyl-2-pentyl (--C(CH.sub.3).sub.2CH.sub.2CH.sub.2CH.sub.3),
3-methyl-2-pentyl (--CH(CH.sub.3)CH(CH.sub.3)CH.sub.2CH.sub.3),
4-methyl-2-pentyl (--CH(CH.sub.3)CH.sub.2CH(CH.sub.3).sub.2),
3-methyl-3-pentyl (--C(CH.sub.3)(CH.sub.2CH.sub.3).sub.2),
2-methyl-3-pentyl (--CH(CH.sub.2CH.sub.3)CH(CH.sub.3).sub.2),
2,3-dimethyl-2-butyl (--C(CH.sub.3).sub.2CH(CH.sub.3).sub.2),
3,3-dimethyl-2-butyl (--CH(CH.sub.3)C(CH.sub.3).sub.3.
[0141] "Alkenyl" is C.sub.2-C.sub.18 hydrocarbon containing normal,
secondary, tertiary or cyclic carbon atoms with at least one site
of unsaturation, i.e. a carbon-carbon, sp.sup.2 double bond.
Examples include, but are not limited to, ethylene or vinyl
(--CH.dbd.CH.sub.2), allyl (--CH.sub.2CH.dbd.CH.sub.2),
cyclopentenyl (--C.sub.5H.sub.7), and 5-hexenyl (--CH.sub.2
CH.sub.2CH.sub.2CH.sub.2CH.dbd.CH.sub.2).
[0142] "Alkynyl" is C.sub.2-C.sub.18 hydrocarbon containing normal,
secondary, tertiary or cyclic carbon atoms with at least one site
of unsaturation, i.e. a carbon-carbon, sp triple bond. Examples
include, but are not limited to, acetylenic (--C.ident.CH) and
propargyl (--CH.sub.2C.ident.CH),
[0143] "Alkylene" refers to a saturated, branched or straight chain
or cyclic hydrocarbon radical of 1-18 carbon atoms, and having two
monovalent radical centers derived by the removal of two hydrogen
atoms from the same or two different carbon atoms of a parent
alkane. Typical alkylene radicals include, but are not limited to,
methylene (--CH.sub.2--) 1,2-ethyl (--CH.sub.2CH.sub.2--),
1,3-propyl (--CH.sub.2CH.sub.2CH.sub.2--), 1,4-butyl
(--CH.sub.2CH.sub.2CH.sub.2CH.sub.2--), and the like.
[0144] "Alkenylene" refers to an unsaturated, branched or straight
chain or cyclic hydrocarbon radical of 2-18 carbon atoms, and
having two monovalent radical centers derived by the removal of two
hydrogen atoms from the same or two different carbon atoms of a
parent alkene. Typical alkenylene radicals include, but are not
limited to, 1,2-ethylene (--CH.dbd.CH--).
[0145] "Alkynylene" refers to an unsaturated, branched or straight
chain or cyclic hydrocarbon radical of 2-18 carbon atoms, and
having two monovalent radical centers derived by the removal of two
hydrogen atoms from the same or two different carbon atoms of a
parent alkyne. Typical alkynylene radicals include, but are not
limited to, acetylene (--C.ident.C--), propargyl
(--CH.sub.2C.ident.C--), and 4-pentynyl
(--CH.sub.2CH.sub.2CH.sub.2C.ident.CH--).
[0146] "Aryl" means a monovalent aromatic hydrocarbon radical of
6-20 carbon atoms derived by the removal of one hydrogen atom from
a single carbon atom of a parent aromatic ring system. Typical aryl
groups include, but are not limited to, radicals derived from
benzene, substituted benzene, naphthalene, anthracene, biphenyl,
and the like.
[0147] "Arylalkyl" refers to an acyclic alkyl radical in which one
of the hydrogen atoms bonded to a carbon atom, typically a terminal
or sp.sup.3 carbon atom, is replaced with an aryl radical. Typical
arylalkyl groups include, but are not limited to, benzyl,
2-phenylethan-1-yl, naphthylmethyl, 2-naphthylethan-1-yl,
naphthobenzyl, 2-naphthophenylethan-1-yl and the like. The
arylalkyl group comprises 6 to 20 carbon atoms, e.g., the alkyl
moiety, including alkanyl, alkenyl or alkynyl groups, of the
arylalkyl group is 1 to 6 carbon atoms and the aryl moiety is 5 to
14 carbon atoms.
[0148] "Substituted alkyl", "substituted aryl", and "substituted
arylalkyl" mean alkyl, aryl, and arylalkyl respectively, in which
one or more hydrogen atoms are each independently replaced with a
non-hydrogen substituent. Typical substituents include, but are not
limited to, --X, --R, --O.sup.-, --OR, --SR, --S.sup.-, --NR.sub.2,
--NR.sub.3, .dbd.NR, --CX.sub.3, --CN, --OCN, --SCN,
--N.dbd.C.dbd.O, --NCS, --NO, --NO.sub.2, .dbd.N.sub.2, --N.sub.3,
NC(.dbd.O)R, --C(.dbd.O)R, --C(.dbd.O)NRR--S(.dbd.O).sub.2O--,
--S(.dbd.O).sub.2OH, --S(.dbd.O).sub.2R, --OS(.dbd.O).sub.2OR,
--S(.dbd.O).sub.2NR, --S(.dbd.O)R, --OP(.dbd.O)O.sub.2R,
--P(.dbd.O)O.sub.2RRR--P(.dbd.O)(O.sup.-).sub.2,
--P(.dbd.O)(OH).sub.2, --C(.dbd.O)R, --C(.dbd.O)X, --C(S)R,
--C(O)OR, --C(O)O.sup.-, --C(S)OR, --C(O)SR, --C(S)SR, --C(O)NRR,
--C(S)NRR, --C(NR)NRR, where each X is independently a halogen: F,
Cl, Br, or I; and each R is independently --H, alkyl, aryl,
heterocycle, protecting group or prodrug moiety. Alkylene,
alkenylene, and alkynylene groups may also be similarly
substituted.
[0149] "Heterocycle" as used herein includes by way of example and
not limitation these heterocycles described in Paquette, Leo A.;
Principles of Modern Heterocyclic Chemistry (W. A. Benjamin, New
York, 1968), particularly Chapters 1, 3, 4, 6, 7, and 9; The
Chemistry of Heterocyclic Compounds, A Series of Monographs" (John
Wiley & Sons, New York, 1950 to present), in particular Volumes
13, 14, 16, 19, and 28; and J. Am. Chem. Soc. (1960) 82:5566. In
one specific embodiment of the invention "heterocycle" includes a
"carbocycle" as defined herein, wherein one or more (e.g. 1, 2, 3,
or 4) carbon atoms have been replaced with a heteroatom (e.g. O, N,
or S).
[0150] Examples of heterocycles include by way of example and not
limitation pyridyl, dihydroypyridyl, tetrahydropyridyl (piperidyl),
thiazolyl, tetrahydrothiophenyl, sulfur oxidized
tetrahydrothiophenyl, pyrimidinyl, furanyl, thienyl, pyrrolyl,
pyrazolyl, imidazolyl, tetrazolyl, benzofuranyl, thianaphthalenyl,
indolyl, indolenyl, quinolinyl, isoquinolinyl, benzimidazolyl,
piperidinyl, 4-piperidonyl, pyrrolidinyl, 2-pyrrolidonyl,
pyrrolinyl, tetrahydrofuranyl, tetrahydroquinolinyl,
tetrahydroisoquinolinyl, decahydroquinolinyl,
octahydroisoquinolinyl, azocinyl, triazinyl, 6H-1,2,5-thiadiazinyl,
2H,6H-1,5,2-dithiazinyl, thienyl, thianthrenyl, pyranyl,
isobenzofuranyl, chromenyl, xanthenyl, phenoxathinyl, 2H-pyrrolyl,
isothiazolyl, isoxazolyl, pyrazinyl, pyridazinyl, indolizinyl,
isoindolyl, 3H-indolyl, 1H-indazoly, purinyl, 4H-quinolizinyl,
phthalazinyl, naphthyridinyl, quinoxalinyl, quinazolinyl,
cinnolinyl, pteridinyl, 4aH-carbazolyl, carbazolyl,
.beta.-carbolinyl, phenanthridinyl, acridinyl, pyrimidinyl,
phenanthrolinyl, phenazinyl, phenothiazinyl, furazanyl,
phenoxazinyl, isochromanyl, chromanyl, imidazolidinyl,
imidazolinyl, pyrazolidinyl, pyrazolinyl, piperazinyl, indolinyl,
isoindolinyl, quinuclidinyl, morpholinyl, oxazolidinyl,
benzotriazolyl, benzisoxazolyl, oxindolyl, benzoxazolinyl,
isatinoyl, and bis-tetrahydrofuranyl:
##STR00035##
[0151] By way of example and not limitation, carbon bonded
heterocycles are bonded at position 2, 3, 4, 5, or 6 of a pyridine,
position 3, 4, 5, or 6 of a pyridazine, position 2, 4, 5, or 6 of a
pyrimidine, position 2, 3, 5, or 6 of a pyrazine, position 2, 3, 4,
or 5 of a furan, tetrahydrofuran, thiofuran, thiophene, pyrrole or
tetrahydropyrrole, position 2, 4, or 5 of an oxazole, imidazole or
thiazole, position 3, 4, or 5 of an isoxazole, pyrazole, or
isothiazole, position 2 or 3 of an aziridine, position 2, 3, or 4
of an azetidine, position 2, 3, 4, 5, 6, 7, or 8 of a quinoline or
position 1, 3, 4, 5, 6, 7, or 8 of an isoquinoline. Still more
typically, carbon bonded heterocycles include 2-pyridyl, 3-pyridyl,
4-pyridyl, 5-pyridyl, 6-pyridyl, 3-pyridazinyl, 4-pyridazinyl,
5-pyridazinyl, 6-pyridazinyl, 2-pyrimidinyl, 4-pyrimidinyl,
5-pyrimidinyl, 6-pyrimidinyl, 2-pyrazinyl, 3-pyrazinyl,
5-pyrazinyl, 6-pyrazinyl, 2-thiazolyl, 4-thiazolyl, or
5-thiazolyl.
[0152] By way of example and not limitation, nitrogen bonded
heterocycles are bonded at position 1 of an aziridine, azetidine,
pyrrole, pyrrolidine, 2-pyrroline, 3-pyrroline, imidazole,
imidazolidine, 2-imidazoline, 3-imidazoline, pyrazole, pyrazoline,
2-pyrazoline, 3-pyrazoline, piperidine, piperazine, indole,
indoline, 1H-indazole, position 2 of a isoindole, or isoindoline,
position 4 of a morpholine, and position 9 of a carbazole, or
.beta.-carboline. Still more typically, nitrogen bonded
heterocycles include 1-aziridyl, 1-azetedyl, 1-pyrrolyl,
1-imidazolyl, 1-pyrazolyl, and 1-piperidinyl.
[0153] "Carbocycle" refers to a saturated, unsaturated or aromatic
ring having 3 to 7 carbon atoms as a monocycle, 7 to 12 carbon
atoms as a bicycle, and up to about 20 carbon atoms as a polycycle.
Monocyclic carbocycles have 3 to 6 ring atoms, still more typically
5 or 6 ring atoms. Bicyclic carbocycles have 7 to 12 ring atoms,
e.g., arranged as a bicyclo [4,5], [5,5], [5,6] or [6,6] system, or
9 or 10 ring atoms arranged as a bicyclo [5,6] or [6,6] system.
Examples of monocyclic carbocycles include cyclopropyl, cyclobutyl,
cyclopentyl, 1-cyclopent-1-enyl, 1-cyclopent-2-enyl,
1-cyclopent-3-enyl, cyclohexyl, 1-cyclohex-1-enyl,
1-cyclohex-2-enyl, 1-cyclohex-3-enyl, phenyl, spiryl and
naphthyl.
[0154] "Linker" or "link" refers to a chemical moiety comprising a
covalent bond or a chain or group of atoms that covalently attaches
a phosphonate group to a drug. Linkers include portions of
substituents A.sup.1 and A.sup.3, which include moieties such as:
repeating units of alkyloxy (e.g., polyethylenoxy, PEG,
polymethyleneoxy) and alkylamino (e.g., polyethyleneamino,
Jeffamine.TM.); and diacid ester and amides including succinate,
succinamide, diglycolate, malonate, and caproamide.
[0155] The term "chiral" refers to molecules which have the
property of non-superimposability of the mirror image partner,
while the term "achiral" refers to molecules which are
superimposable on their mirror image partner.
[0156] The term "stereoisomers" refers to compounds which have
identical chemical constitution, but differ with regard to the
arrangement of the atoms or groups in space.
[0157] "Diastereomer" refers to a stereoisomer with two or more
centers of chirality and whose molecules are not mirror images of
one another. Diastereomers have different physical properties,
e.g., melting points, boiling points, spectral properties, and
reactivities. Mixtures of diastereomers may separate under high
resolution analytical procedures such as electrophoresis and
chromatography.
[0158] "Enantiomers" refer to two stereoisomers of a compound which
are non-superimposable mirror images of one another.
[0159] The term "treatment" or "treating," to the extent it relates
to a disease or condition includes preventing the disease or
condition from occurring, inhibiting the disease or condition,
eliminating the disease or condition, and/or relieving one or more
symptoms of the disease or condition.
[0160] Stereochemical definitions and conventions used herein
generally follow S. P. Parker, Ed., McGraw-Hill Dictionary of
Chemical Terms (1984) McGraw-Hill Book Company, New York; and
Eliel, E. and Wilen, S., Stereochemistry of Organic Compounds
(1994) John Wiley & Sons, Inc., New York. Many organic
compounds exist in optically active forms, i.e., they have the
ability to rotate the plane of plane-polarized light. In describing
an optically active compound, the prefixes D and L or R and S are
used to denote the absolute configuration of the molecule about its
chiral center(s). The prefixes d and l or (+) and (-) are employed
to designate the sign of rotation of plane-polarized light by the
compound, with (-) or l meaning that the compound is levorotatory.
A compound prefixed with (+) or d is dextrorotatory. For a given
chemical structure, these stereoisomers are identical except that
they are mirror images of one another. A specific stereoisomer may
also be referred to as an enantiomer, and a mixture of such isomers
is often called an enantiomeric mixture. A 50:50 mixture of
enantiomers is referred to as a racemic mixture or a racemate,
which may occur where there has been no stereoselection or
stereospecificity in a chemical reaction or process. The terms
"racemic mixture" and "racemate" refer to an equimolar mixture of
two enantiomeric species, devoid of optical activity.
Protecting Groups
[0161] In the context of the present invention, protecting groups
include prodrug moieties and chemical protecting groups.
[0162] Protecting groups are available, commonly known and used,
and are optionally used to prevent side reactions with the
protected group during synthetic procedures, i.e. routes or methods
to prepare the compounds of the invention. For the most part the
decision as to which groups to protect, when to do so, and the
nature of the chemical protecting group "PG" will be dependent upon
the chemistry of the reaction to be protected against (e.g.,
acidic, basic, oxidative, reductive or other conditions) and the
intended direction of the synthesis. The PG groups do not need to
be, and generally are not, the same if the compound is substituted
with multiple PG. In general, PG will be used to protect functional
groups such as carboxyl, hydroxyl, thio, or amino groups and to
thus prevent side reactions or to otherwise facilitate the
synthetic efficiency. The order of deprotection to yield free,
deprotected groups is dependent upon the intended direction of the
synthesis and the reaction conditions to be encountered, and may
occur in any order as determined by the artisan.
[0163] Various functional groups of the compounds of the invention
may be protected. For example, protecting groups for --OH groups
(whether hydroxyl, carboxylic acid, phosphonic acid, or other
functions) include "ether- or ester-forming groups". Ether- or
ester-forming groups are capable of functioning as chemical
protecting groups in the synthetic schemes set forth herein.
However, some hydroxyl and thio protecting groups are neither
ether-nor ester-forming groups, as will be understood by those
skilled in the art, and are included with amides, discussed
below.
[0164] A very large number of hydroxyl protecting groups and
amide-forming groups and corresponding chemical cleavage reactions
are described in Protective Groups in Organic Synthesis, Theodora
W. Greene (John Wiley & Sons, Inc., New York, 1991, ISBN
0-471-62301-6) ("Greene"). See also Kocienski, Philip J.;
Protecting Groups (Georg Thieme Verlag Stuttgart, N.Y., 1994),
which is incorporated by reference in its entirety herein. In
particular Chapter 1, Protecting Groups: An Overview, pages 1-20,
Chapter 2, Hydroxyl Protecting Groups, pages 21-94, Chapter 3, Diol
Protecting Groups, pages 95-117, Chapter 4, Carboxyl Protecting
Groups, pages 118-154, Chapter 5, Carbonyl Protecting Groups, pages
155-184. For protecting groups for carboxylic acid, phosphonic
acid, phosphonate, sulfonic acid and other protecting groups for
acids see Greene as set forth below. Such groups include by way of
example and not limitation, esters, amides, hydrazides, and the
like.
Ether- and Ester-Forming Protecting Groups
[0165] Ester-forming groups include: (1) phosphonate ester-forming
groups, such as phosphonamidate esters, phosphorothioate esters,
phosphonate esters, and phosphon-bis-amidates; (2) carboxyl
ester-forming groups, and (3) sulphur ester-forming groups, such as
sulphonate, sulfate, and sulfinate.
[0166] The phosphonate moieties of the compounds of the invention
may or may not be prodrug moieties, i.e. they may or may not be
susceptible to hydrolytic or enzymatic cleavage or modification.
Certain phosphonate moieties are stable under most or nearly all
metabolic conditions. For example, a dialkylphosphonate, where the
alkyl groups are two or more carbons, may have appreciable
stability in vivo due to a slow rate of hydrolysis.
[0167] Within the context of phosphonate prodrug moieties, a large
number of structurally-diverse prodrugs have been described for
phosphonic acids (Freeman and Ross in Progress in Medicinal
Chemistry 34: 112-147 (1997)) and are included within the scope of
the present invention. An exemplary phosphonate ester-forming group
is the phenyl carbocycle in substructure A.sub.3 having the
formula:
##STR00036##
[0168] wherein R.sub.1 may be H or C.sub.1-C.sub.12 alkyl; m1 is 1,
2, 3, 4, 5, 6, 7 or 8, and the phenyl carbocycle is substituted
with 0 to 3 R.sub.2 groups. Where Y.sub.1 is O, a lactate ester is
formed, and where Y.sub.1 is N(R.sub.2), N(OR.sub.2) or
N(N(R.sub.2).sub.2, a phosphonamidate ester results.
[0169] In its ester-forming role, a protecting group typically is
bound to any acidic group such as, by way of example and not
limitation, a --CO.sub.2H or --C(S)OH group, thereby resulting in
--CO.sub.2R.sup.x where R.sup.x is defined herein. Also, R.sup.x
for example includes the enumerated ester groups of WO
95/07920.
[0170] Examples of protecting groups include:
[0171] C.sub.3-C.sub.12 heterocycle (described above) or aryl.
These aromatic groups optionally are polycyclic or monocyclic.
Examples include phenyl, spiryl, 2- and 3-pyrrolyl, 2- and
3-thienyl, 2- and 4-imidazolyl, 2-, 4- and 5-oxazolyl, 3- and
4-isoxazolyl, 2-, 4- and 5-thiazolyl, 3-, 4- and 5-isothiazolyl, 3-
and 4-pyrazolyl, 1-, 2-, 3- and 4-pyridinyl, and 1-, 2-, 4- and
5-pyrimidinyl,
[0172] C.sub.3-C.sub.12 heterocycle or aryl substituted with halo,
R.sup.1, R.sup.1--O--C.sub.1-C.sub.12 alkylene, C.sub.1-C.sub.12
alkoxy, CN, NO.sub.2, OH, carboxy, carboxyester, thiol, thioester,
C.sub.1-C.sub.12 haloalkyl (1-6 halogen atoms), C.sub.2-C.sub.12
alkenyl or C.sub.2-C.sub.12 alkynyl. Such groups include 2-, 3- and
4-alkoxyphenyl (C.sub.1-C.sub.12 alkyl), 2-, 3- and
4-methoxyphenyl, 2-, 3- and 4-ethoxyphenyl, 2,3-, 2,4-, 2,5-, 2,6-,
3,4- and 3,5-diethoxyphenyl, 2- and 3-carboethoxy-4-hydroxyphenyl,
2- and 3-ethoxy-4-hydroxyphenyl, 2- and 3-ethoxy-5-hydroxyphenyl,
2- and 3-ethoxy-6-hydroxyphenyl, 2-, 3- and 4-O-acetylphenyl, 2-,
3- and 4-dimethylaminophenyl, 2-, 3- and 4-methylmercaptophenyl,
2-, 3- and 4-halophenyl (including 2-, 3- and 4-fluorophenyl and
2-, 3- and 4-chlorophenyl), 2,3-, 2,4-, 2,5-, 2,6-, 3,4- and
3,5-dimethylphenyl, 2,3-, 2,4-, 2,5-, 2,6-, 3,4- and
3,5-biscarboxyethylphenyl, 2,3-, 2,4-, 2,5-, 2,6-, 3,4- and
3,5-dimethoxyphenyl, 2,3-, 2,4-, 2,5-, 2,6-, 3,4- and
3,5-dihalophenyl (including 2,4-difluorophenyl and
3,5-difluorophenyl), 2-, 3- and 4-haloalkylphenyl (1 to 5 halogen
atoms, C.sub.1-C.sub.12 alkyl including 4-trifluoromethylphenyl),
2-, 3- and 4-cyanophenyl, 2-, 3- and 4-nitrophenyl, 2-, 3- and
4-haloalkylbenzyl (1 to 5 halogen atoms, C.sub.1-C.sub.12 alkyl
including 4-trifluoromethylbenzyl and 2-, 3- and
4-trichloromethylphenyl and 2-, 3- and 4-trichloromethylphenyl),
4-N-methylpiperidinyl, 3-N-methylpiperidinyl, 1-ethylpiperazinyl,
benzyl, alkylsalicylphenyl (C.sub.1-C.sub.4 alkyl, including 2-, 3-
and 4-ethylsalicylphenyl), 2-, 3- and 4-acetylphenyl,
1,8-dihydroxynaphthyl (--C.sub.10H.sub.6--OH) and aryloxy ethyl
[C.sub.6-C.sub.8 aryl (including phenoxy ethyl)],
2,2'-dihydroxybiphenyl, 2-, 3- and 4-N,N-dialkylaminophenol,
--C.sub.6H.sub.4CH.sub.2--N(CH.sub.3).sub.2, trimethoxybenzyl,
triethoxybenzyl, 2-alkyl pyridinyl (C.sub.1-4 alkyl);
##STR00037##
esters of 2-carboxyphenyl; and C.sub.1-C.sub.4
alkylene-C.sub.3-C.sub.6 aryl (including benzyl,
--CH.sub.2-pyrrolyl, --CH.sub.2-thienyl, --CH.sub.2-imidazolyl,
--CH.sub.2-oxazolyl, --CH.sub.2-isoxazolyl, --CH.sub.2-thiazolyl,
--CH.sub.2-isothiazolyl, --CH.sub.2-pyrazolyl, --CH.sub.2-pyridinyl
and --CH.sub.2-pyrimidinyl) substituted in the aryl moiety by 3 to
5 halogen atoms or 1 to 2 atoms or groups selected from halogen,
C.sub.1-C.sub.12 alkoxy (including methoxy and ethoxy), cyano,
nitro, OH, C.sub.1-C.sub.12 haloalkyl (1 to 6 halogen atoms;
including --CH.sub.2CCl.sub.3), C.sub.1-C.sub.12 alkyl (including
methyl and ethyl), C.sub.2-C.sub.12 alkenyl or C.sub.2-C.sub.12
alkynyl; alkoxy ethyl [C.sub.1-C.sub.6 alkyl including
--CH.sub.2--CH.sub.2--O--CH.sub.3 (methoxy ethyl)]; alkyl
substituted by any of the groups set forth above for aryl, in
particular OH or by 1 to 3 halo atoms (including --CH.sub.3,
--CH(CH.sub.3).sub.2, --C(CH.sub.3).sub.3, --CH.sub.2CH.sub.3,
--(CH.sub.2).sub.2CH.sub.3, --(CH.sub.2).sub.3CH.sub.3,
--(CH.sub.2).sub.4CH.sub.3, --(CH.sub.2).sub.5CH.sub.3,
--CH.sub.2CH.sub.2F, --CH.sub.2CH.sub.2Cl, --CH.sub.2CF.sub.3, and
--CH.sub.2CCl.sub.3);
##STR00038##
propylmorpholino, 2,3-dihydro-6-hydroxyindene, sesamol, catechol
monoester, --CH.sub.2--C(O)--N(R.sup.1).sub.2,
--CH.sub.2--S(O)(R.sup.1), --CH.sub.2--S(O).sub.2(R.sup.1),
--CH.sub.2--CH(OC(O)CH.sub.2R.sup.1)--CH.sub.2(OC(O)CH.sub.2R.sup.1),
cholesteryl, enolpyruvate (HOOC--C(.dbd.CH.sub.2)--), glycerol;
[0173] a 5 or 6 carbon monosaccharide, disaccharide or
oligosaccharide (3 to 9 monosaccharide residues);
[0174] triglycerides such as .alpha.-D-.beta.-diglycerides (wherein
the fatty acids composing glyceride lipids generally are naturally
occurring saturated or unsaturated C.sub.6-26, C.sub.6-18 or
C.sub.6-10 fatty acids such as linoleic, lauric, myristic,
palmitic, stearic, oleic, palmitoleic, linolenic and the like fatty
acids) linked to acyl of the parental compounds herein through a
glyceryl oxygen of the triglyceride;
[0175] phospholipids linked to the carboxyl group through the
phosphate of the phospholipid;
[0176] phthalidyl (shown in FIG. 1 of Clayton et al., Antimicrob.
Agents Chemo. (1974) 5(6):670-671);
[0177] cyclic carbonates such as
(5-R.sub.d-2-oxo-1,3-dioxolen-4-yl)methyl esters (Sakamoto et al.,
Chem. Pharm. Bull. (1984) 32(6)2241-2248) where R.sub.d is R.sub.1,
R.sub.4 or aryl; and
##STR00039##
[0178] The hydroxyl groups of the compounds of this invention
optionally are substituted with one of groups III, IV or V
disclosed in WO 94/21604, or with isopropyl.
[0179] Table A lists examples of protecting group ester moieties
that for example can be bonded via oxygen to --C(O)O-- and
--P(O)(O--).sub.2 groups. Several amidates also are shown, which
are bound directly to --C(O)-- or --P(O).sub.2. Esters of
structures 1-5, 8-10 and 16, 17, 19-22 are synthesized by reacting
the compound herein having a free hydroxyl with the corresponding
halide (chloride or acyl chloride and the like) and
N,N-dicyclohexyl-N-morpholine carboxamidine (or another base such
as DBU, triethylamine, CsCO.sub.3, N,N-dimethylaniline and the
like) in DMF (or other solvent such as acetonitrile or
N-methylpyrrolidone). When the compound to be protected is a
phosphonate, the esters of structures 5-7, 11, 12, 21, and 23-26
are synthesized by reaction of the alcohol or alkoxide salt (or the
corresponding amines in the case of compounds such as 13, 14 and
15) with the monochlorophosphonate or dichlorophosphonate (or
another activated phosphonate).
TABLE-US-00001 TABLE A 1. --CH.sub.2--C(O)--N(R.sub.1).sub.2* 2.
--CH.sub.2--S(O)(R.sub.1) 3. --CH.sub.2--S(O).sub.2(R.sub.1) 4.
--CH.sub.2--O--C(O)--CH.sub.2--C.sub.6H.sub.5 5. 3-cholesteryl 6.
3-pyridyl 7. N-ethylmorpholino 8.
--CH.sub.2--O--C(O)--C.sub.6H.sub.5 9.
--CH.sub.2--O--C(O)--CH.sub.2CH.sub.3 10.
--CH.sub.2--O--C(O)--C(CH.sub.3).sub.3 11. --CH.sub.2--CCl.sub.3
12. --C.sub.6H.sub.5 13. --NH--CH.sub.2--C(O)O--CH.sub.2CH.sub.3
14. --N(CH.sub.3)--CH.sub.2--C(O)O--CH.sub.2CH.sub.3 15.
--NHR.sub.1 16. --CH.sub.2--O--C(O)--C.sub.10H.sub.15 17.
--CH.sub.2--O--C(O)--CH(CH.sub.3).sub.2 18.
--CH.sub.2--C*H(OC(O)CH.sub.2R.sub.1)--CH.sub.2--(OC(O)CH.sub.2R.sub.-
1)* 19. ##STR00040## 20. ##STR00041## 21. ##STR00042## 22.
##STR00043## 23. ##STR00044## 24. ##STR00045## 25. ##STR00046## 26.
##STR00047## #-chiral center is (R), (S) or racemate.
[0180] Other esters that are suitable for use herein are described
in EP 632048.
[0181] Protecting groups also includes "double ester" forming
profunctionalities such as --CH.sub.2OC(O)OCH.sub.3,
##STR00048##
--CH.sub.2SCOCH.sub.3, --CH.sub.2OCON(CH.sub.3).sub.2, or alkyl- or
aryl-acyloxyalkyl groups of the structure --CH(R.sup.1 or
W.sup.5)O((CO)R.sup.37) or --CH(R.sup.1 or W.sup.5)((CO)OR.sup.38)
(linked to oxygen of the acidic group) wherein R.sup.37 and
R.sup.38 are alkyl, aryl, or alkylaryl groups (see U.S. Pat. No.
4,968,788). Frequently R.sup.37 and R.sup.38 are bulky groups such
as branched alkyl, ortho-substituted aryl, meta-substituted aryl,
or combinations thereof, including normal, secondary, iso- and
tertiary alkyls of 1-6 carbon atoms. An example is the
pivaloyloxymethyl group. These are of particular use with prodrugs
for oral administration. Examples of such useful protecting groups
are alkylacyloxymethyl esters and their derivatives, including
--CH(CH.sub.2CH.sub.2OCH.sub.3)OC(O)C(CH.sub.3).sub.3,
##STR00049##
CH.sub.2OC(O)C.sub.10H.sub.15, --CH.sub.2OC(O)C(CH.sub.3).sub.3,
--CH(CH.sub.2OCH.sub.3)OC(O)C(CH.sub.3).sub.3,
--CH(CH(CH.sub.3).sub.2)OC(O)C(CH.sub.3).sub.3,
--CH.sub.2OC(O)CH.sub.2CH(CH.sub.3).sub.2,
--CH.sub.2OC(O)C.sub.6H.sub.11, --CH.sub.2OC(O)C.sub.6H.sub.5,
--CH.sub.2OC(O)C.sub.10H.sub.15, --CH.sub.2OC(O)CH.sub.2CH.sub.3,
--CH.sub.2OC(O)CH(CH.sub.3).sub.2, --CH.sub.2OC(O)C(CH.sub.3).sub.3
and --CH.sub.2OC(O)CH.sub.2C.sub.6H.sub.5.
[0182] In some claims the protected acidic group is an ester of the
acidic group and is the residue of a hydroxyl-containing
functionality. In other claims, an amino compound is used to
protect the acid functionality. The residues of suitable hydroxyl
or amino-containing functionalities are set forth above or are
found in WO 95/07920. Of particular interest are the residues of
amino acids, amino acid esters, polypeptides, or aryl alcohols.
Typical amino acid, polypeptide and carboxyl-esterified amino acid
residues are described on pages 11-18 and related text of WO
95/07920 as groups L1 or L2. WO 95/07920 expressly teaches the
amidates of phosphonic acids, but it will be understood that such
amidates are formed with any of the acid groups set forth herein
and the amino acid residues set forth in WO 95/07920.
[0183] Typical esters for protecting acidic functionalities are
also described in WO 95/07920, again understanding that the same
esters can be formed with the acidic groups herein as with the
phosphonate of the '920 publication. Typical ester groups are
defined at least on WO 95/07920 pages 89-93 (under R.sup.31 or
R.sup.35), the table on page 105, and pages 21-23 (as R). Of
particular interest are esters of unsubstituted aryl such as phenyl
or arylalkyl such benzyl, or hydroxy-, halo-, alkoxy-, carboxy-
and/or alkylestercarboxy-substituted aryl or alkylaryl, especially
phenyl, ortho-ethoxyphenyl, or C.sub.1-C.sub.4
alkylestercarboxyphenyl (salicylate C.sub.1-C.sub.12
alkylesters).
[0184] The protected acidic groups, particularly when using the
esters or amides of WO 95/07920, are useful as prodrugs for oral
administration. However, it is not essential that the acidic group
be protected in order for the compounds of this invention to be
effectively administered by the oral route. When the compounds of
the invention having protected groups, in particular amino acid
amidates or substituted and unsubstituted aryl esters are
administered systemically or orally they are capable of hydrolytic
cleavage in vivo to yield the free acid.
[0185] One or more of the acidic hydroxyls are protected. If more
than one acidic hydroxyl is protected then the same or a different
protecting group is employed, e.g., the esters may be different or
the same, or a mixed amidate and ester may be used.
[0186] Typical hydroxy protecting groups described in Greene (pages
14-118) include substituted methyl and alkyl ethers, substituted
benzyl ethers, silyl ethers, esters including sulfonic acid esters,
and carbonates. For example: [0187] Ethers (methyl, t-butyl,
allyl); [0188] Substituted Methyl Ethers (Methoxymethyl,
Methylthiomethyl, t-Butylthiomethyl,
(Phenyldimethylsilyl)methoxymethyl, Benzyloxymethyl,
p-Methoxybenzyloxymethyl, (4-Methoxyphenoxy)methyl, Guaiacolmethyl,
t-Butoxymethyl, 4-Pentenyloxymethyl, Siloxymethyl,
2-Methoxyethoxymethyl, 2,2,2-Trichloroethoxymethyl,
Bis(2-chloroethoxy)methyl, 2-(Trimethylsilyl)ethoxymethyl,
Tetrahydropyranyl, 3-Bromotetrahydropyranyl,
Tetrahydropthiopyranyl, 1-Methoxycyclohexyl,
4-Methoxytetrahydropyranyl, 4-Methoxytetrahydrothiopyranyl,
4-Methoxytetrahydropthiopyranyl S,S-Dioxido,
1-[(2-Chloro-4-methyl)phenyl]-4-methoxypiperidin-4-yl,
1,4-Dioxan-2-yl, Tetrahydrofuranyl, Tetrahydrothiofuranyl,
2,3,3a,4,5,6,7,7a-Octahydro-7,8,8-trimethyl-4,7-methanobenzofuran-2-yl));
[0189] Substituted Ethyl Ethers (1-Ethoxyethyl,
1-(2-Chloroethoxy)ethyl, 1-Methyl-1-methoxyethyl,
1-Methyl-1-benzyloxyethyl, 1-Methyl-1-benzyloxy-2-fluoroethyl,
2,2,2-Trichloroethyl, 2-Trimethylsilylethyl,
2-(Phenylselenyl)ethyl, [0190] p-Chlorophenyl, p-Methoxyphenyl,
2,4-Dinitrophenyl, Benzyl); [0191] Substituted Benzyl Ethers
(p-Methoxybenzyl, 3,4-Dimethoxybenzyl, o-Nitrobenzyl,
p-Nitrobenzyl, p-Halobenzyl, 2,6-Dichlorobenzyl, p-Cyanobenzyl,
p-Phenylbenzyl, 2- and 4-Picolyl, 3-Methyl-2-picolyl N-Oxido,
Diphenylmethyl, p,p'-Dinitrobenzhydryl, 5-Dibenzosuberyl,
Triphenylmethyl, .alpha.-Naphthyldiphenylmethyl,
p-methoxyphenyldiphenylmethyl, Di(p-methoxyphenyl)phenylmethyl,
Tri(p-methoxyphenyl)methyl,
4-(4'-Bromophenacyloxy)phenyldiphenylmethyl,
4,4',4''-Tris(4,5-dichlorophthalimidophenyl)methyl,
4,4',4''-Tris(levulinoyloxyphenyl)methyl,
4,4',4''-Tris(benzoyloxyphenyl)methyl,
3-(Imidazol-1-ylmethyl)bis(4',4''-dimethoxyphenyl)methyl,
1,1-Bis(4-methoxyphenyl)-1'-pyrenylmethyl, 9-Anthryl,
9-(9-Phenyl)xanthenyl, 9-(9-Phenyl-10-oxo)anthryl,
1,3-Benzodithiolan-2-yl, Benzisothiazolyl S,S-Dioxido); [0192]
Silyl Ethers (Trimethylsilyl, Triethylsilyl, Triisopropylsilyl,
Dimethylisopropylsilyl, Diethylisopropylsilyl, Dimethylthexylsilyl,
t-Butyldimethylsilyl, t-Butyldiphenylsilyl, Tribenzylsilyl,
Tri-p-xylylsilyl, Triphenylsilyl, Diphenylmethylsilyl,
t-Butylmethoxyphenylsilyl); [0193] Esters (Formate, Benzoylformate,
Acetate, Choroacetate, Dichloroacetate, Trichloroacetate,
Trifluoroacetate, Methoxyacetate, Triphenylmethoxyacetate,
Phenoxyacetate, p-Chlorophenoxyacetate, p-poly-Phenylacetate,
3-Phenylpropionate, 4-Oxopentanoate (Levulinate),
4,4-(Ethylenedithio)pentanoate, Pivaloate, Adamantoate, Crotonate,
4-Methoxycrotonate, Benzoate, p-Phenylbenzoate,
2,4,6-Trimethylbenzoate (Mesitoate)); [0194] Carbonates (Methyl,
9-Fluorenylmethyl, Ethyl, 2,2,2-Trichloroethyl,
2-(Trimethylsilyl)ethyl, 2-(Phenylsulfonyl)ethyl,
2-(Triphenylphosphonio)ethyl, Isobutyl, Vinyl, Allyl,
p-Nitrophenyl, Benzyl, p-Methoxybenzyl, 3,4-Dimethoxybenzyl,
o-Nitrobenzyl, p-Nitrobenzyl, S-Benzyl Thiocarbonate,
4-Ethoxy-1-naphthyl, Methyl Dithiocarbonate); [0195] Groups With
Assisted Cleavage (2-Iodobenzoate, 4-Azidobutyrate,
4-Nitro-4-methylpentanoate, o-(Dibromomethyl)benzoate,
2-Formylbenzenesulfonate, 2-(Methylthiomethoxy)ethyl Carbonate,
4-(Methylthiomethoxy)butyrate,
2-(Methylthiomethoxymethyl)benzoate); Miscellaneous Esters
(2,6-Dichloro-4-methylphenoxyacetate, 2,6-Dichloro-4-(1,1,3,3
tetramethylbutyl)phenoxyacetate,
2,4-Bis(1,1-dimethylpropyl)phenoxyacetate, Chlorodiphenylacetate,
Isobutyrate, Monosuccinate, (E)-2-Methyl-2-butenoate (Tigloate),
o-(Methoxycarbonyl)benzoate, p-poly-Benzoate, .alpha.-Naphthoate,
Nitrate, Alkyl N,N,N',N'-Tetramethylphosphorodiamidate,
N-Phenylcarbamate, Borate, Dimethylphosphinothioyl,
2,4-Dinitrophenylsulfenate); and [0196] Sulfonates (Sulfate,
Methanesulfonate (Mesylate), Benzylsulfonate, Tosylate).
[0197] Typical 1,2-diol protecting groups (thus, generally where
two OH groups are taken together with the protecting functionality)
are described in Greene at pages 118-142 and include Cyclic Acetals
and Ketals (Methylene, Ethylidene, 1-t-Butylethylidene,
1-Phenylethylidene, (4-Methoxyphenyl)ethylidene,
2,2,2-Trichloroethylidene, Acetonide (Isopropylidene),
Cyclopentylidene, Cyclohexylidene, Cycloheptylidene, Benzylidene,
p-Methoxybenzylidene, 2,4-Dimethoxybenzylidene,
3,4-Dimethoxybenzylidene, 2-Nitrobenzylidene); Cyclic Ortho Esters
(Methoxymethylene, Ethoxymethylene, Dimethoxymethylene,
1-Methoxyethylidene, 1-Ethoxyethylidine, 1,2-Dimethoxyethylidene,
.alpha.-Methoxybenzylidene, 1-(N,N-Dimethylamino)ethylidene
Derivative, .alpha.-(N,N-Dimethylamino)benzylidene Derivative,
2-Oxacyclopentylidene); Silyl Derivatives (Di-t-butylsilylene
Group, 1,3-(1,1,3,3-Tetraisopropyldisiloxanylidene), and
Tetra-t-butoxydisiloxane-1,3-diylidene), Cyclic Carbonates, Cyclic
Boronates, Ethyl Boronate and Phenyl Boronate.
[0198] More typically, 1,2-diol protecting groups include those
shown in Table B, still more typically, epoxides, acetonides,
cyclic ketals and aryl acetals.
TABLE-US-00002 TABLE B ##STR00050## ##STR00051## ##STR00052##
##STR00053## ##STR00054## ##STR00055## ##STR00056## ##STR00057##
##STR00058## ##STR00059## ##STR00060## wherein R.sup.9 is
C.sub.1-C.sub.6 alkyl.
Amino Protecting Groups
[0199] Another set of protecting groups include any of the typical
amino protecting groups described by Greene at pages 315-385. They
include: [0200] Carbamates: (methyl and ethyl, 9-fluorenylmethyl,
9(2-sulfo)fluorenylmethyl, 9-(2,7-dibromo)fluorenylmethyl,
2,7-di-t-butyl-[9-(10,10-dioxo-10,10,10,10-tetrahydrothioxanthyl)]methyl,
4-methoxyphenacyl); [0201] Substituted Ethyl: (2,2,2-trichoroethyl,
2-trimethylsilylethyl, 2-phenylethyl,
1-(1-adamantyl)-1-methylethyl, 1,1-dimethyl-2-haloethyl,
1,1-dimethyl-2,2-dibromoethyl, 1,1-dimethyl-2,2,2-trichloroethyl,
1-methyl-1-(4-biphenylyl)ethyl,
1-(3,5-di-t-butylphenyl)-1-methylethyl, 2-(2'- and
4'-pyridyl)ethyl, 2-(N,N-dicyclohexylcarboxamido)ethyl, t-butyl,
1-adamantyl, vinyl, allyl, 1-isopropylallyl, cinnamyl,
4-nitrocinnamyl, 8-quinolyl, N-hydroxypiperidinyl, alkyldithio,
benzyl, p-methoxybenzyl, p-nitrobenzyl, p-bromobenzyl,
p-chlorobenzyl, 2,4-dichlorobenzyl, 4-methylsulfinylbenzyl,
9-anthrylmethyl, diphenylmethyl); [0202] Groups With Assisted
Cleavage: (2-methylthioethyl, 2-methylsulfonylethyl,
2-(p-toluenesulfonyl)ethyl, [2-(1,3-dithianyl)]methyl,
4-methylthiophenyl, 2,4-dimethylthiophenyl, 2-phosphonioethyl,
2-triphenylphosphonioisopropyl, 1,1-dimethyl-2-cyanoethyl,
m-choro-p-acyloxybenzyl, p-(dihydroxyboryl)benzyl,
5-benzisoxazolylmethyl, 2-(trifluoromethyl)-6-chromonylmethyl);
[0203] Groups Capable of Photolytic Cleavage: (m-nitrophenyl,
3,5-dimethoxybenzyl, o-nitrobenzyl, 3,4-dimethoxy-6-nitrobenzyl,
phenyl(o-nitrophenyl)methyl); Urea-Type Derivatives
(phenothiazinyl-(10)-carbonyl, N-p-toluenesulfonylaminocarbonyl,
N'-phenylaminothiocarbonyl); [0204] Miscellaneous Carbamates:
(t-amyl, S-benzyl thiocarbamate, p-cyanobenzyl, cyclobutyl,
cyclohexyl, cyclopentyl, cyclopropylmethyl, p-decyloxybenzyl,
diisopropylmethyl, 2,2-dimethoxycarbonylvinyl,
o-(N,N-dimethylcarboxamido)benzyl,
1,1-dimethyl-3-(N,N-dimethylcarboxamido)propyl,
1,1-dimethylpropynyl, di(2-pyridyl)methyl, 2-furanylmethyl,
2-Iodoethyl, Isobornyl, Isobutyl, Isonicotinyl,
p-(p'-Methoxyphenylazo)benzyl, 1-methylcyclobutyl,
1-methylcyclohexyl, 1-methyl-1-cyclopropylmethyl,
1-methyl-1-(3,5-dimethoxyphenyl)ethyl,
1-methyl-1-(p-phenylazophenyl)ethyl, 1-methyl-1-phenylethyl,
1-methyl-1-(4-pyridyl)ethyl, phenyl, p-(phenylazo)benzyl,
2,4,6-tri-t-butylphenyl, 4-(trimethylammonium)benzyl,
2,4,6-trimethylbenzyl); [0205] Amides: (N-formyl, N-acetyl,
N-choroacetyl, N-trichoroacetyl, N-trifluoroacetyl, N-phenylacetyl,
N-3-phenylpropionyl, N-picolinoyl, N-3-pyridylcarboxamide,
N-benzoylphenylalanyl, N-benzoyl, N-p-phenylbenzoyl); [0206] Amides
With Assisted Cleavage: (N-o-nitrophenylacetyl,
N-o-nitrophenoxyacetyl, N-acetoacetyl,
(N'-dithiobenzyloxycarbonylamino)acetyl,
N-3-(p-hydroxyphenyl)propionyl, N-3-(o-nitrophenyl)propionyl,
N-2-methyl-2-(o-nitrophenoxy)propionyl,
N-2-methyl-2-(o-phenylazophenoxy)propionyl, N-4-chlorobutyryl,
N-3-methyl-3-nitrobutyryl, N-o-nitrocinnamoyl, N-acetylmethionine,
N-o-nitrobenzoyl, N-o-(benzoyloxymethyl)benzoyl,
4,5-diphenyl-3-oxazolin-2-one); [0207] Cyclic Imide Derivatives:
(N-phthalimide, N-dithiasuccinoyl, N-2,3-diphenylmaleoyl,
N-2,5-dimethylpyrrolyl, N-1,1,4,4-tetramethyldisilylazacyclopentane
adduct, 5-substituted 1,3-dimethyl-1,3,5-triazacyclohexan-2-one,
5-substituted 1,3-dibenzyl-1,3-5-triazacyclohexan-2-one,
1-substituted 3,5-dinitro-4-pyridonyl); [0208] N-Alkyl and N-Aryl
Amines: (N-methyl, N-allyl, N-[2-(trimethylsilyl)ethoxy]methyl,
N-3-acetoxypropyl, N-(1-isopropyl-4-nitro-2-oxo-3-pyrrolin-3-yl),
Quaternary Ammonium Salts, N-benzyl, N-di(4-methoxyphenyl)methyl,
N-5-dibenzosuberyl, N-triphenylmethyl,
N-(4-methoxyphenyl)diphenylmethyl, N-9-phenylfluorenyl,
N-2,7-dichloro-9-fluorenylmethylene, N-ferrocenylmethyl,
N-2-picolylamine N'-oxide); [0209] Imine Derivatives:
(N-1,1-dimethylthiomethylene, N-benzylidene,
N-p-methoxybenzylidene, N-diphenylmethylene,
N-[(2-pyridyl)mesityl]methylene, N,(N',N'-dimethylaminomethylene,
N,N-isopropylidene, N-p-nitrobenzylidene, N-salicylidene,
N-5-chlorosalicylidene,
N-(5-chloro-2-hydroxyphenyl)phenylmethylene, N-cyclohexylidene);
[0210] Enamine Derivatives:
(N-(5,5-dimethyl-3-oxo-1-cyclohexenyl)); [0211] N-Metal Derivatives
(N-borane derivatives, N-diphenylborinic acid derivatives,
N-[phenyl(pentacarbonylchromium- or -tungsten)]carbenzyl, N-copper
or N-zinc chelate); [0212] N--N Derivatives: (N-nitro, N-nitroso,
N-oxide); [0213] N--P Derivatives: (N-diphenylphosphinyl,
N-dimethylthiophosphinyl, N-diphenylthiophosphinyl, N-dialkyl
phosphoryl, N-dibenzyl phosphoryl, N-diphenyl phosphoryl); [0214]
N--Si Derivatives, N--S Derivatives, and N-Sulfenyl Derivatives:
(N-benzenesulfenyl, N-o-nitrobenzenesulfenyl,
N-2,4-dinitrobenzenesulfenyl, N-pentachlorobenzenesulfenyl,
N-2-nitro-4-methoxybenzenesulfenyl, N-triphenylmethylsulfenyl,
N-3-nitropyridinesulfenyl); and N-sulfonyl Derivatives
(N-p-toluenesulfonyl, N-benzenesulfonyl,
N-2,3,6-trimethyl-4-methoxybenzenesulfonyl,
N-2,4,6-trimethoxybenzenesulfonyl,
N-2,6-dimethyl-4-methoxybenzenesulfonyl,
N-pentamethylbenzenesulfonyl,
N-2,3,5,6,-tetramethyl-4-methoxybenzenesulfonyl,
N-4-methoxybenzenesulfonyl, N-2,4,6-trimethylbenzenesulfonyl,
N-2,6-dimethoxy-4-methylbenzenesulfonyl,
N-2,2,5,7,8-pentamethylchroman-6-sulfonyl, N-methanesulfonyl,
N-.beta.-trimethylsilyethanesulfonyl, N-9-anthracenesulfonyl,
N-4-(4',8'-dimethoxynaphthylmethyl)benzenesulfonyl,
N-benzylsulfonyl, N-trifluoromethylsulfonyl,
N-phenacylsulfonyl).
[0215] More typically, protected amino groups include carbamates
and amides, still more typically, --NHC(O)R.sup.1 or
--N.dbd.CR.sup.1N(R.sup.1).sub.2. Another protecting group, also
useful as a prodrug for amino or --NH(R.sup.5), is:
##STR00061##
See for example Alexander, J. et al. (1996) J. Med. Chem.
39:480-486.
Amino Acid and Polypeptide Protecting Group and Conjugates
[0216] An amino acid or polypeptide protecting group of a compound
of the invention has the structure R.sup.15NHCH(R.sup.16)C(O)--,
where R.sup.15 is H, an amino acid or polypeptide residue, or
R.sup.5, and R.sup.16 is defined below.
[0217] R.sup.16 is lower alkyl or lower alkyl (C.sub.1-C.sub.6)
substituted with amino, carboxyl, amide, carboxyl ester, hydroxyl,
C.sub.6-C.sub.7 aryl, guanidinyl, imidazolyl, indolyl, sulfhydryl,
sulfoxide, and/or alkylphosphate. R.sup.10 also is taken together
with the amino acid .alpha. N to form a proline residue
(R.sup.10=--CH.sub.2).sub.3--). However, R.sup.10 is generally the
side group of a naturally-occurring amino acid such as H,
--CH.sub.3, --CH(CH.sub.3).sub.2, --CH.sub.2--CH(CH.sub.3).sub.2,
--CHCH.sub.3--CH.sub.2--CH.sub.3, --CH.sub.2--C.sub.6H.sub.5,
--CH.sub.2CH.sub.2--S--CH.sub.3, --CH.sub.2OH, --CH(OH)--CH.sub.3,
--CH.sub.2--SH, --CH.sub.2--C.sub.6H.sub.4OH,
--CH.sub.2--CO--NH.sub.2, --CH.sub.2--CH.sub.2--CO--NH.sub.2,
--CH.sub.2--COOH, --CH.sub.2--CH.sub.2--COOH,
--(CH.sub.2).sub.4--NH.sub.2 and
--(CH.sub.2).sub.3--NH--C(NH.sub.2)--NH.sub.2. R.sub.10 also
includes 1-guanidinoprop-3-yl, benzyl, 4-hydroxybenzyl,
imidazol-4-yl, indol-3-yl, methoxyphenyl and ethoxyphenyl.
[0218] Another set of protecting groups include the residue of an
amino-containing compound, in particular an amino acid, a
polypeptide, a protecting group, --NHSO.sub.2R, NHC(O)R,
--N(R).sub.2, NH.sub.2 or --NH(R)(H), whereby for example a
carboxylic acid is reacted, i.e. coupled, with the amine to form an
amide, as in C(O)NR.sub.2. A phosphonic acid may be reacted with
the amine to form a phosphonamidate, as in
--P(O)(OR)(NR.sub.2).
[0219] In general, amino acids have the structure
R.sup.17C(O)CH(R.sup.16)NH--, where R.sup.17 is --OH, --OR, an
amino acid or a polypeptide residue. Amino acids are low molecular
weight compounds, on the order of less than about 1000 MW and which
contain at least one amino or imino group and at least one carboxyl
group. Generally the amino acids will be found in nature, i.e., can
be detected in biological material such as bacteria or other
microbes, plants, animals or man. Suitable amino acids typically
are alpha amino acids, i.e. compounds characterized by one amino or
imino nitrogen atom separated from the carbon atom of one carboxyl
group by a single substituted or unsubstituted alpha carbon atom.
Of particular interest are hydrophobic residues such as mono- or
di-alkyl or aryl amino acids, cycloalkylamino acids and the like.
These residues contribute to cell permeability by increasing the
partition coefficient of the parental drug. Typically, the residue
does not contain a sulfhydryl or guanidino substituent.
[0220] Naturally-occurring amino acid residues are those residues
found naturally in plants, animals or microbes, especially proteins
thereof. Polypeptides most typically will be substantially composed
of such naturally-occurring amino acid residues. These amino acids
are glycine, alanine, valine, leucine, isoleucine, serine,
threonine, cysteine, methionine, glutamic acid, aspartic acid,
lysine, hydroxylysine, arginine, histidine, phenylalanine,
tyrosine, tryptophan, proline, asparagine, glutamine and
hydroxyproline. Additionally, unnatural amino acids, for example,
valanine, phenylglycine and homoarginine are also included.
Commonly encountered amino acids that are not gene-encoded may also
be used in the present invention. All of the amino acids used in
the present invention may be either the D- or L-optical isomer. In
addition, other peptidomimetics are also useful in the present
invention. For a general review, see Spatola, A. F., in Chemistry
and Biochemistry of Amino Acids, Peptides and Proteins, B.
Weinstein, eds., Marcel Dekker, New York, p. 267 (1983).
[0221] When protecting groups are single amino acid residues or
polypeptides they optionally are substituted at R.sup.3 of
substituents A.sup.1, A.sup.2 or A.sup.3 in Formula I. These
conjugates are produced by forming an amide bond between a carboxyl
group of the amino acid (or C-terminal amino acid of a polypeptide
for example). Similarly, conjugates are formed between R.sup.3
(Formula I) and an amino group of an amino acid or polypeptide.
Generally, only one of any site in the parental molecule is
amidated with an amino acid as described herein, although it is
within the scope of this invention to introduce amino acids at more
than one permitted site. Usually, a carboxyl group of R.sup.3 is
amidated with an amino acid. In general, the .alpha.-amino or
.alpha.-carboxyl group of the amino acid or the terminal amino or
carboxyl group of a polypeptide are bonded to the parental
functionalities, i.e., carboxyl or amino groups in the amino acid
side chains generally are not used to form the amide bonds with the
parental compound (although these groups may need to be protected
during synthesis of the conjugates as described further below).
[0222] With respect to the carboxyl-containing side chains of amino
acids or polypeptides it will be understood that the carboxyl group
optionally will be blocked, e.g., by R.sup.1, esterified with
R.sup.5 or amidated. Similarly, the amino side chains R.sup.16
optionally will be blocked with R.sup.1 or substituted with
R.sup.5.
[0223] Such ester or amide bonds with side chain amino or carboxyl
groups, like the esters or amides with the parental molecule,
optionally are hydrolyzable in vivo or in vitro under acidic
(pH<3) or basic (pH>10) conditions. Alternatively, they are
substantially stable in the gastrointestinal tract of humans but
are hydrolyzed enzymatically in blood or in intracellular
environments. The esters or amino acid or polypeptide amidates also
are useful as intermediates for the preparation of the parental
molecule containing free amino or carboxyl groups. The free acid or
base of the parental compound, for example, is readily formed from
the esters or amino acid or polypeptide conjugates of this
invention by conventional hydrolysis procedures.
[0224] When an amino acid residue contains one or more chiral
centers, any of the D, L, meso, threo or erythro (as appropriate)
racemates, scalemates or mixtures thereof may be used. In general,
if the intermediates are to be hydrolyzed non-enzymatically (as
would be the case where the amides are used as chemical
intermediates for the free acids or free amines), D isomers are
useful. On the other hand, L isomers are more versatile since they
can be susceptible to both non-enzymatic and enzymatic hydrolysis,
and are more efficiently transported by amino acid or dipeptidyl
transport systems in the gastrointestinal tract.
[0225] Examples of suitable amino acids whose residues are
represented by R.sup.x or R.sup.y include the following:
[0226] Glycine;
[0227] Aminopolycarboxylic acids, e.g., aspartic acid,
.beta.-hydroxyaspartic acid, glutamic acid, .beta.-hydroxyglutamic
acid, .beta.-methylaspartic acid, .beta.-methylglutamic acid,
.beta.,.beta.-dimethylaspartic acid, .gamma.-hydroxyglutamic acid,
.beta.,.gamma.-dihydroxyglutamic acid, .beta.-phenylglutamic acid,
.gamma.-methyleneglutamic acid, 3-aminoadipic acid, 2-aminopimelic
acid, 2-aminosuberic acid and 2-aminosebacic acid;
[0228] Amino acid amides such as glutamine and asparagine;
[0229] Polyamino- or polybasic-monocarboxylic acids such as
arginine, lysine, .beta.-aminoalanine, .gamma.-aminobutyrine,
ornithine, citruline, homoarginine, homocitrulline, hydroxylysine,
allohydroxylsine and diaminobutyric acid;
[0230] Other basic amino acid residues such as histidine;
[0231] Diaminodicarboxylic acids such as
.alpha.,.alpha.'-diaminosuccinic acid,
.alpha.,.alpha.'-diaminoglutaric acid,
.alpha.,.alpha.'-diaminoadipic acid,
.alpha.,.alpha.'-diaminopimelic acid,
.alpha.,.alpha.'-diamino-.beta.-hydroxypimelic acid,
.alpha.,.alpha.'-diaminosuberic acid,
.alpha.,.alpha.'-diaminoazelaic acid, and
.alpha.,.alpha.'-diaminosebacic acid;
[0232] Imino acids such as proline, hydroxyproline,
allohydroxyproline, .gamma.-methylproline, pipecolic acid,
5-hydroxypipecolic acid, and azetidine-2-carboxylic acid;
[0233] A mono- or di-alkyl (typically C.sub.1-C.sub.8 branched or
normal) amino acid such as alanine, valine, leucine, allylglycine,
butyrine, norvaline, norleucine, heptyline, .alpha.-methylserine,
.alpha.-amino-.alpha.-methyl-.gamma.-hydroxyvaleric acid,
.alpha.-amino-.alpha.-methyl-.delta.-hydroxyvaleric acid,
.alpha.-amino-.alpha.-methyl-.epsilon.-hydroxycaproic acid,
isovaline, .alpha.-methylglutamic acid, .alpha.-aminoisobutyric
acid, .alpha.-aminodiethylacetic acid,
.alpha.-aminodiisopropylacetic acid, .alpha.-aminodi-n-propylacetic
acid, .alpha.-aminodiisobutylacetic acid,
.alpha.-aminodi-n-butylacetic acid,
.alpha.-aminoethylisopropylacetic acid,
.alpha.-amino-n-propylacetic acid, .alpha.-aminodiisoamyacetic
acid, .alpha.-methylaspartic acid, .alpha.-methylglutamic acid,
1-aminocyclopropane-1-carboxylic acid, isoleucine, alloisoleucine,
tert-leucine, .alpha.-methyltryptophan and
.alpha.-amino-.beta.-ethyl-.beta.-phenylpropionic acid;
[0234] .beta.-phenylserinyl;
[0235] Aliphatic .alpha.-amino-.beta.-hydroxy acids such as serine,
.beta.-hydroxylcucine, .beta.-hydroxynorleucine,
.beta.-hydroxynorvaline, and .alpha.-amino-.beta.-hydroxystearic
acid;
[0236] .alpha.-Amino, .alpha.-, .gamma.-, .delta.- or
.epsilon.-hydroxy acids such as homoserine,
.delta.-hydroxynorvaline, .gamma.-hydroxynorvaline and
.epsilon.-hydroxynorleucine residues; canavine and canaline;
.gamma.-hydroxyornithine;
[0237] 2-hexosaminic acids such as D-glucosaminic acid or
D-galactosaminic acid;
[0238] .alpha.-Amino-.beta.-thiols such as penicillamine,
.beta.-thiolnorvaline or .beta.-thiolbutyrine;
[0239] Other sulfur containing amino acid residues including
cysteine; homocystine, .beta.-phenylmethionine, methionine,
S-allyl-L-cysteine sulfoxide, 2-thiolhistidine, cystathionine, and
thiol ethers of cysteine or homocysteine;
[0240] Phenylalanine, tryptophan and ring-substituted .alpha.-amino
acids such as the phenyl- or cyclohexylamino acids
.alpha.-aminophenylacetic acid, .alpha.-aminocyclohexylacetic acid
and .alpha.-amino-.beta.-cyclohexylpropionic acid; phenylalanine
analogues and derivatives comprising aryl, lower alkyl, hydroxy,
guanidino, oxyalkylether, nitro, sulfur or halo-substituted phenyl
(e.g., tyrosine, methyltyrosine and o-chloro-, p-chloro-,
3,4-dichloro, o-, m- or p-methyl-, 2,4,6-trimethyl-,
2-ethoxy-5-nitro-, 2-hydroxy-5-nitro- and p-nitro-phenylalanine);
furyl-, thienyl-, pyridyl-, pyrimidinyl-, purinyl- or
naphthyl-alanines; and tryptophan analogues and derivatives
including kynurenine, 3-hydroxykynurenine, 2-hydroxytryptophan and
4-carboxytryptophan;
[0241] .alpha.-Amino substituted amino acids including sarcosine
(N-methylglycine), N-benzylglycine, N-methylalanine,
N-benzylalanine, N-methylphenylalanine, N-benzylphenylalanine,
N-methylvaline and N-benzylvaline; and
[0242] .alpha.-Hydroxy and substituted .alpha.-hydroxy amino acids
including serine, threonine, allothreonine, phosphoserine and
phosphothreonine.
[0243] Polypeptides are polymers of amino acids in which a carboxyl
group of one amino acid monomer is bonded to an amino or imino
group of the next amino acid monomer by an amide bond. Polypeptides
include dipeptides, low molecular weight polypeptides (about
1500-5000 MW) and proteins. Proteins optionally contain 3, 5, 10,
50, 75, 100 or more residues, and suitably are substantially
sequence-homologous with human, animal, plant or microbial
proteins. They include enzymes (e.g., hydrogen peroxidase) as well
as immunogens such as KLH, or antibodies or proteins of any type
against which one wishes to raise an immune response. The nature
and identity of the polypeptide may vary widely.
[0244] The polypeptide amidates are useful as immunogens in raising
antibodies against either the polypeptide (if it is not immunogenic
in the animal to which it is administered) or against the epitopes
on the remainder of the compound of this invention.
[0245] Antibodies capable of binding to the parental non-peptidyl
compound are used to separate the parental compound from mixtures,
for example in diagnosis or manufacturing of the parental compound.
The conjugates of parental compound and polypeptide generally are
more immunogenic than the polypeptides in closely homologous
animals, and therefore make the polypeptide more immunogenic for
facilitating raising antibodies against it. Accordingly, the
polypeptide or protein may not need to be immunogenic in an animal
typically used to raise antibodies, e.g., rabbit, mouse, horse, or
rat, but the final product conjugate should be immunogenic in at
least one of such animals. The polypeptide optionally contains a
peptidolytic enzyme cleavage site at the peptide bond between the
first and second residues adjacent to the acidic heteroatom. Such
cleavage sites are flanked by enzymatic recognition structures,
e.g., a particular sequence of residues recognized by a
peptidolytic enzyme.
[0246] Peptidolytic enzymes for cleaving the polypeptide conjugates
of this invention are well known, and in particular include
carboxypeptidases. Carboxypeptidases digest polypeptides by
removing C-terminal residues, and are specific in many instances
for particular C-terminal sequences. Such enzymes and their
substrate requirements in general are well known. For example, a
dipeptide (having a given pair of residues and a free carboxyl
terminus) is covalently bonded through its .alpha.-amino group to
the phosphorus or carbon atoms of the compounds herein. In claims
where W.sub.1 is phosphonate it is expected that this peptide will
be cleaved by the appropriate peptidolytic enzyme, leaving the
carboxyl of the proximal amino acid residue to autocatalytically
cleave the phosphonoamidate bond.
[0247] Suitable dipeptidyl groups (designated by their single
letter code) are AA, AR, AN, AD, AC, AE, AQ, AG, AH, AI, AL, AK,
AM, AF, AP, AS, AT, AW, AY, AV, RA, RR, RN, RD, RC, RE, RQ, RG, RH,
RI, RL, RK, RM, RF, RP, RS, RT, RW, RY, RV, NA, NR, NN, ND, NC, NE,
NQ, NG, NH, NI, NL, NK, NM, NF, NP, NS, NT, NR, NY, NV, DA, DR, DN,
DD, DC, DE, DQ, DG, DH, DI, DL, DK, DM, DF, DP, DS, DT, DW, DY, DV,
CA, CR, CN, CD, CC, CE, CQ, CG, CH, CI, CL, CK, CM, CF, CP, CS, CT,
CW, CY, CV, EA, ER, EN, ED, EC, EE, EQ, EG, EH, EI, EL, EK, EM, EF,
EP, ES, ET, EW, EY, EV, QA, QR, QN, QD, QC, QE, QQ, QG, QH, QI, QL,
QK, QM, QF, QP, QS, QT, QW, QY, QV, GA, GR, GN, GD, GC, GE, GQ, GG,
GH, GI, GL, GK, GM, GF, GP, GS, GT, GW, GY, GV, HA, HR, HN, HD, HC,
HE, HQ, HG, HH, HI, HL, HK, HM, HF, HP, HS, HT, HW, HY, HV, IA, IR,
IN, ID, IC, IE, IQ, IG, IH, II, IL, IK, IM, IF, IP, IS, IT, IW, IY,
IV, LA, LR, LN, LD, LC, LE, LQ, LG, LH, LI, LL, LK, LM, LF, LP, LS,
LT, LW, LY, LV, KA, KR, KN, KD, KC, KE, KQ, KG, KH, KI, KL, KK, KM,
KF, KP, KS, KT, KW, KY, KV, MA, MR, MN, MD, MC, ME, MQ, MG, MH, MI,
ML, MK, MM, MF, MP, MS, MT, MW, MY, MV, FA, FR, FN, FD, FC, FE, FQ,
FG, FH, FI, FL, FK, FM, FF, FP, FS, FT, FW, FY, FV, PA, PR, PN, PD,
PC, PE, PQ, PG, PH, PI, PL, PK, PM, PF, PP, PS, PT, PW, PY, PV, SA,
SR, SN, SD, SC, SE, SQ, SG, SH, SI, SL, SK, SM, SF, SP, SS, ST, SW,
SY, SV, TA, TR, TN, TD, TC, TE, TQ, TG, TH, TI, TL, TK, TM, TF, TP,
TS, TT, TW, TY, TV, WA, WR, WN, WD, WC, WE, WQ, WG, WH, WI, WL, WK,
WM, WF, WP, WS, WT, WW, WY, WV, YA, YR, YN, YD, YC, YE, YQ, YG, YH,
YI, YL, YK, YM, YF, YP, YS, YT, YW, YY, YV, VA, VR, VN, VD, VC, VE,
VQ, VG, VH, VI, VL, VK, VM, VF, VP, VS, VT, VW, VY and VV.
[0248] Tripeptide residues are also useful as protecting groups.
When a phosphonate is to be protected, the sequence
--X.sup.4-pro-X.sup.5-- (where X.sup.4 is any amino acid residue
and X.sup.5 is an amino acid residue, a carboxyl ester of proline,
or hydrogen) will be cleaved by luminal carboxypeptidase to yield
X.sup.4 with a free carboxyl, which in turn is expected to
autocatalytically cleave the phosphonoamidate bond. The carboxy
group of X.sup.5 optionally is esterified with benzyl.
[0249] Dipeptide or tripeptide species can be selected on the basis
of known transport properties and/or susceptibility to peptidases
that can affect transport to intestinal mucosal or other cell
types. Dipeptides and tripeptides lacking an .alpha.-amino group
are transport substrates for the peptide transporter found in brush
border membrane of intestinal mucosal cells (Bai, J. P. F., (1992)
Pharm Res. 9:969-978). Transport competent peptides can thus be
used to enhance bioavailability of the amidate compounds. Di- or
tripeptides having one or more amino acids in the D configuration
are also compatible with peptide transport and can be utilized in
the amidate compounds of this invention. Amino acids in the D
configuration can be used to reduce the susceptibility of a di- or
tripeptide to hydrolysis by proteases common to the brush border
such as aminopeptidase N. In addition, di- or tripeptides
alternatively are selected on the basis of their relative
resistance to hydrolysis by proteases found in the lumen of the
intestine. For example, tripeptides or polypeptides lacking asp
and/or glu are poor substrates for aminopeptidase A, di- or
tripeptides lacking amino acid residues on the N-terminal side of
hydrophobic amino acids (leu, tyr, phe, val, trp) are poor
substrates for endopeptidase, and peptides lacking a pro residue at
the penultimate position at a free carboxyl terminus are poor
substrates for carboxypeptidase P. Similar considerations can also
be applied to the selection of peptides that are either relatively
resistant or relatively susceptible to hydrolysis by cytosolic,
renal, hepatic, serum or other peptidases. Such poorly cleaved
polypeptide amidates are immunogens or are useful for bonding to
proteins in order to prepare immunogens.
SPECIFIC EMBODIMENTS OF THE INVENTION
[0250] Specific values described for radicals, substituents, and
ranges, as well as specific embodiments of the invention described
herein, are for illustration only; they do not exclude other
defined values or other values within defined ranges.
[0251] In one specific embodiment of the invention, the conjugate
is a compound that is substituted with one or more phosphonate
groups either directly or indirectly through a linker; and that is
optionally substituted with one or more groups A.sup.0; or a
pharmaceutically acceptable salt thereof, wherein:
[0252] A.sup.0 is A.sup.1, A.sup.2 or W.sup.3;
[0253] A.sup.1 is:
##STR00062##
[0254] A.sup.2 is:
##STR00063##
[0255] A.sup.3 is:
##STR00064##
[0256] Y.sup.1 is independently O, S, N(R.sup.x), N(O)(R.sup.x),
N(OR.sup.x), N(O)(OR.sup.x), or N(N(R.sup.x)(R.sup.x));
[0257] Y.sup.2 is independently a bond, O, N(R.sup.x),
N(O)(R.sup.x), N(OR.sup.x), N(O)(OR.sup.x), N(N(R.sup.x)(R.sup.x)),
--S(O).sub.M2--, or --S(O).sub.M2--S(O).sub.M2--;
[0258] R.sup.x is independently H, R.sup.1, W.sup.3, a protecting
group, or the formula:
##STR00065##
[0259] wherein:
[0260] R.sup.y is independently H, W.sup.3, R.sup.2 or a protecting
group;
[0261] R.sup.1 is independently H or alkyl of 1 to 18 carbon
atoms;
[0262] R.sup.2 is independently H, R.sup.1, R.sup.3 or R.sup.4
wherein each R.sup.4 is independently substituted with 0 to 3
R.sup.3 groups or taken together at a carbon atom, two R.sup.2
groups form a ring of 3 to 8 carbons and the ring may be
substituted with 0 to 3 R.sup.3 groups;
[0263] R.sup.3 is R.sup.3a, R.sup.3b, R.sup.3c or R.sup.3d,
provided that when R.sup.3 is bound to a heteroatom, then R.sup.3
is R.sup.3c or R.sup.3d;
[0264] R.sup.3a is F, Cl, Br, I, --CN, N.sub.3 or --NO.sub.2;
[0265] R.sup.3b is Y.sup.1;
[0266] R.sup.3c is R.sup.x, N(R.sup.x)(R.sup.x), --SR.sup.x,
--S(O)R.sup.x, --S(O).sub.2R.sup.x, --S(O)(OR.sup.x),
S(O).sub.2(OR.sup.x), --OC(Y.sup.1)R.sup.x, --OC(Y.sup.1)OR.sup.x,
--OC(Y.sup.1)(N(R.sup.x)(R.sup.x)), --SC(Y.sup.1)R.sup.x,
--SC(Y.sup.1)OR.sup.x, --SC(Y.sup.1)(N(R.sup.x)(R.sup.x)),
--N(R.sup.x)C(Y.sup.1)R.sup.x, N(R.sup.x)C(Y.sup.1)OR.sup.x, or
--N(R.sup.x)C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0267] R.sup.3d is --C(Y.sup.1)R.sup.x, --C(Y.sup.1)OR.sup.x or
--C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0268] R.sup.4 is an alkyl of 1 to 18 carbon atoms, alkenyl of 2 to
18 carbon atoms, or alkynyl of 2 to 18 carbon atoms;
[0269] R.sup.5 is R.sup.4 wherein each R.sup.4 is substituted with
0 to 3 R.sup.3 groups;
[0270] R.sup.5a is independently alkylene of 1 to 18 carbon atoms,
alkenylene of 2 to 18 carbon atoms, or alkynylene of 2-18 carbon
atoms any one of which alkylene, alkenylene or alkynylene is
substituted with 0-3 R.sup.3 groups;
[0271] W.sup.3 is W.sup.4 or W.sup.5;
[0272] W.sup.4 is R.sup.5, --C(Y.sup.1)R.sup.5,
--C(Y.sup.1)W.sup.5, --SO.sub.2R.sup.5, or --SO.sub.2W.sup.5;
[0273] W.sup.5 is carbocycle or heterocycle wherein W.sup.5 is
independently substituted with 0 to 3 R.sup.2 groups;
[0274] W.sup.6 is W.sup.3 independently substituted with 1, 2, or 3
A.sup.3 groups;
[0275] M2 is 0, 1 or 2;
[0276] M12a is 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0277] M12b is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0278] M1a, M1c, and M1d are independently 0 or 1; and
[0279] M12c is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12.
[0280] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00066##
[0281] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00067##
[0282] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00068##
[0283] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00069##
[0284] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00070##
and W.sup.5a is a carbocycle or a heterocycle where W.sup.5a is
independently substituted with 0 or 1 R.sup.2 groups. A specific
value for M12a is 1.
[0285] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00071##
[0286] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00072##
[0287] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00073##
wherein W.sup.5a is a carbocycle independently substituted with 0
or 1 R.sup.2 groups;
[0288] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00074##
wherein Y.sup.2b is O or N(R.sup.2); and M12d is 1, 2, 3, 4, 5, 6,
7 or 8.
[0289] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00075##
wherein W.sup.5a is a carbocycle independently substituted with 0
or 1 R.sup.2 groups;
[0290] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00076##
wherein W.sup.5a is a carbocycle or heterocycle where W.sup.5a is
independently substituted with 0 or 1 R.sup.2 groups.
[0291] In another specific embodiment of the invention A.sup.1 is
of the formula:
##STR00077##
wherein Y.sup.2b is O or N(R.sup.2); and M12d is 1, 2, 3, 4, 5, 6,
7 or 8.
[0292] In a specific embodiment of the invention A.sup.2 is of the
formula:
##STR00078##
[0293] In another specific embodiment of the invention A.sup.2 is
of the formula:
##STR00079##
[0294] In another specific embodiment of the invention M12b is
1.
[0295] In another specific embodiment of the invention M12b is 0,
Y.sup.2 is a bond and W.sup.5 is a carbocycle or heterocycle where
W.sup.5 is optionally and independently substituted with 1, 2, or 3
R.sup.2 groups.
[0296] In another specific embodiment of the invention A.sup.2 is
of the formula:
##STR00080##
wherein W.sup.5a is a carbocycle or heterocycle where W.sup.5a is
optionally and independently substituted with 1, 2, or 3 R.sup.2
groups.
[0297] In another specific embodiment of the invention M12a is
1.
[0298] In another specific embodiment of the invention A.sup.2 is
selected from phenyl, substituted phenyl, benzyl, substituted
benzyl, pyridyl and substituted pyridyl.
[0299] In another specific embodiment of the invention A.sup.2 is
of the formula:
##STR00081##
[0300] In another specific embodiment of the invention A.sup.2 is
of the formula:
##STR00082##
[0301] In another specific embodiment of the invention M12b is
1.
[0302] In a specific embodiment of the invention A.sup.3 is of the
formula:
##STR00083##
[0303] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00084##
[0304] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00085##
wherein Y.sup.1a is O or S; and Y.sup.2a is O, N(R.sup.x) or S.
[0305] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00086##
wherein Y.sup.2b is O or N(R.sup.x).
[0306] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00087##
wherein Y.sup.2b is O or N(R.sup.x); and M12d is 1, 2, 3, 4, 5, 6,
7 or 8.
[0307] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00088##
wherein Y.sup.2b is O or N(R.sup.x); and M12d is 1, 2, 3, 4, 5, 6,
7 or 8.
[0308] In another specific embodiment of the invention M12d is
1.
[0309] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00089##
[0310] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00090##
[0311] In another specific embodiment of the invention W.sup.5 is a
carbocycle.
[0312] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00091##
[0313] In another specific embodiment of the invention W.sup.5 is
phenyl.
[0314] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00092##
wherein Y.sup.1a is O or S; and Y.sup.2a is O, N(R.sup.x) or S.
[0315] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00093##
wherein Y.sup.2b is O or N(R.sup.x).
[0316] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00094##
wherein Y.sup.2b is O or N(R.sup.x); and M12d is 1, 2, 3, 4, 5, 6,
7 or 8.
[0317] In another specific embodiment of the invention R.sup.1 is
H.
[0318] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00095##
wherein the phenyl carbocycle is substituted with 0, 1, 2, or 3
R.sup.2 groups.
[0319] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00096##
[0320] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00097##
[0321] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00098##
[0322] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00099##
[0323] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00100##
wherein Y.sup.1a is O or S; and Y.sup.2a is O, N(R.sup.2) or S.
[0324] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00101##
wherein Y.sup.1a is O or S; Y.sup.2b is O or N(R.sup.2); and
Y.sup.2c is O, N(R.sup.y) or S.
[0325] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00102##
wherein Y.sup.1a is O or S; Y.sup.2b is O or N(R.sup.2); Y.sup.2d
is O or N(R.sup.y); and M12d is 1, 2, 3, 4, 5, 6, 7 or 8.
[0326] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00103##
wherein Y.sup.2b is O or N(R.sup.2); and M12d is 1, 2, 3, 4, 5, 6,
7 or 8.
[0327] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00104##
wherein Y.sup.2b is O or N(R.sup.2).
[0328] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00105##
[0329] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00106##
[0330] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00107##
wherein Y.sup.1a is O or S; and Y.sup.2a is O, N(R.sup.2) or S.
[0331] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00108##
wherein Y.sup.1a is O or S; Y.sup.2b is O or N(R.sup.2); and
Y.sup.2c is O, N(R.sup.y) or S.
[0332] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00109##
wherein Y.sup.1a is O or S; Y.sup.2b is O or N(R.sup.2); Y.sup.2d
is O or N(R.sup.y); and M12d is 1, 2, 3, 4, 5, 6, 7 or 8.
[0333] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00110##
wherein Y.sup.2b is O or N(R.sup.2); and M12d is 1, 2, 3, 4, 5, 6,
7 or 8.
[0334] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00111##
wherein Y.sup.2b is O or N(R.sup.2).
[0335] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00112##
wherein: Y.sup.2b is O or N(R.sup.x); and M12d is 1, 2, 3, 4, 5, 6,
7 or 8.
[0336] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00113##
wherein the phenyl carbocycle is substituted with 0, 1, 2, or 3
R.sup.2 groups.
[0337] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00114##
wherein the phenyl carbocycle is substituted with 0, 1, 2, or 3
R.sup.2 groups.
[0338] In another specific embodiment of the invention A.sup.3 is
of the formula:
##STR00115##
[0339] In a specific embodiment of the invention A.sup.0 is of the
formula:
##STR00116##
wherein each R is independently (C.sub.1-C.sub.6)alkyl.
[0340] In a specific embodiment of the invention R.sup.x is
independently H, R.sup.1, W.sup.3, a protecting group, or the
formula:
##STR00117##
[0341] wherein:
[0342] R.sup.y is independently H, W.sup.3, R.sup.2 or a protecting
group;
[0343] R.sup.1 is independently H or alkyl of 1 to 18 carbon
atoms;
[0344] R.sup.2 is independently H, R.sup.1, R.sup.3 or R.sup.4
wherein each R.sup.4 is independently substituted with 0 to 3
R.sup.3 groups or taken together at a carbon atom, two R.sup.2
groups form a ring of 3 to 8 carbons and the ring may be
substituted with 0 to 3 R.sup.3 groups;
[0345] In a specific embodiment of the invention R.sup.x is of the
formula:
##STR00118##
wherein Y.sup.1a is O or S; and Y.sup.2c is O, N(R.sup.y) or S.
[0346] In a specific embodiment of the invention R.sup.x is of the
formula:
##STR00119##
wherein Y.sup.1a is O or S; and Y.sup.2d is O or N(R.sup.y).
[0347] In a specific embodiment of the invention R.sup.x is of the
formula:
##STR00120##
[0348] In a specific embodiment of the invention R.sup.y is
hydrogen or alkyl of 1 to 10 carbons.
[0349] In a specific embodiment of the invention R.sup.x is of the
formula:
##STR00121##
[0350] In a specific embodiment of the invention R.sup.x is of the
formula:
##STR00122##
[0351] In a specific embodiment of the invention R.sup.x is of the
formula:
##STR00123##
[0352] In a specific embodiment of the invention Y.sup.1 is O or
S.
[0353] In a specific embodiment of the invention Y.sup.2 is O,
N(R.sup.y) or S.
[0354] In one specific embodiment of the invention R.sup.x is a
group of the formula:
##STR00124##
wherein:
[0355] m1a, m1b, m1c, m1d and m1e are independently 0 or 1;
[0356] m12c is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0357] R.sup.y is H, W.sup.3, R.sup.2 or a protecting group;
provided that:
[0358] if m1a, m12c, and m1d are 0, then m1b, m1c and m1e are
0;
[0359] if m1a and m12c are 0 and m1d is not 0, then m1b and m1c are
0;
[0360] if m1a and m1d are 0 and m12c is not 0, then m1b and at
least one of m1c and m1e are 0;
[0361] if m1a is 0 and m12c and m1d are not 0, then m1b is 0;
[0362] if m12c and m1d are 0 and m1a is not 0, then at least two of
m1b, m1c and m1e are 0;
[0363] if m12c is 0 and m1a and m1d are not 0, then at least one of
m1b and m1c are 0; and
[0364] if m1d is 0 and m1a and m12c are not 0, then at least one of
m1c and m1e are 0.
[0365] In another specific embodiment, the invention provides a
compound of the formula:
[DRUG]-(A.sup.0).sub.nn
or a pharmaceutically acceptable salt thereof wherein,
[0366] DRUG is a compound of any one of formulae 500-547;
[0367] nn is 1, 2, or 3;
[0368] A.sup.0 is A.sup.1, A.sup.2 or W.sup.3 with the proviso that
the compound includes at least one A.sup.1;
[0369] A.sup.1 is:
##STR00125##
[0370] A.sup.2 is:
##STR00126##
[0371] A3 is:
##STR00127##
[0372] Y.sup.1 is independently O, S, N(R.sup.x), N(O)(R.sup.x),
N(OR.sup.x), N(O)(OR.sup.x), or N(N(R.sup.x)(R.sup.x));
[0373] Y.sup.2 is independently a bond, O, N(R.sup.x),
N(O)(R.sup.x), N(OR.sup.x), N(O)(OR.sup.x), N(N(R.sup.x)(R.sup.x)),
--S(O).sub.M2--, or --S(O).sub.M2--S(O).sub.M2--;
[0374] R.sup.x is independently H, R.sup.1, W.sup.3, a protecting
group, or the formula:
##STR00128##
[0375] wherein:
[0376] R.sup.y is independently H, W.sup.3, R.sup.2 or a protecting
group;
[0377] R.sup.1 is independently H or alkyl of 1 to 18 carbon
atoms;
[0378] R.sup.2 is independently H, R.sup.1, R.sup.3 or R.sup.4
wherein each R.sup.4 is independently substituted with 0 to 3
R.sup.3 groups or taken together at a carbon atom, two R.sup.2
groups form a ring of 3 to 8 carbons and the ring may be
substituted with 0 to 3 R.sup.3 groups;
[0379] R.sup.3 is R.sup.3a, R.sup.3h, R.sup.3c or R.sup.3d,
provided that when R.sup.3 is bound to a heteroatom, then R.sup.3
is R.sup.3c or R.sup.3d;
[0380] R.sup.3a is F, Cl, Br, I, --CN, N.sub.3 or --NO.sub.2;
[0381] R.sup.3b is y;
[0382] R.sup.3c is R.sup.x, N(R.sup.x)(R.sup.x), --SR.sup.x,
--S(O)R.sup.x, --S(O).sub.2R.sup.x, --S(O)(OR.sup.x),
--S(O).sub.2(OR.sup.x), --OC(Y.sup.1)R.sup.x,
--OC(Y.sup.1)OR.sup.x, --OC(Y.sup.1)(N(R.sup.x)(R.sup.x)),
--SC(Y.sup.1)R.sup.x, --SC(Y.sup.1)OR.sup.x,
--SC(Y.sup.1)(N(R.sup.x)(R.sup.x)), --N(R.sup.x)C(Y.sup.1)R.sup.x,
--N(R.sup.x)C(Y.sup.1)OR.sup.x, or
--N(R.sup.x)C(Y.sup.1)((R.sup.x)(R.sup.x));
[0383] R.sup.3d is --C(Y.sup.1)R.sup.x, --C(Y.sup.1)OR.sup.x or
--C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0384] R.sup.4 is an alkyl of 1 to 18 carbon atoms, alkenyl of 2 to
18 carbon atoms, or alkynyl of 2 to 18 carbon atoms;
[0385] R.sup.5 is R.sup.4 wherein each R.sup.4 is substituted with
0 to 3 R.sup.3 groups;
[0386] R.sup.5a is independently alkylene of 1 to 18 carbon atoms,
alkenylene of 2 to 18 carbon atoms, or alkynylene of 2-18 carbon
atoms any one of which alkylene, alkenylene or alkynylene is
substituted with 0-3 R.sup.3 groups;
[0387] W.sup.3 is W.sup.4 or W.sup.5;
[0388] W.sup.4 is R.sup.5, --C(Y.sup.1)R.sup.5,
--C(Y.sup.1)W.sup.5, --SO.sub.2R.sup.5, or --SO.sub.2W.sup.5;
[0389] W.sup.5 is carbocycle or heterocycle wherein W.sup.5 is
independently substituted with 0 to 3 R.sup.2 groups;
[0390] W.sup.6 is W.sup.3 independently substituted with 1, 2, or 3
A.sup.3 groups;
[0391] M2 is 0, 1 or 2;
[0392] M12a is 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0393] M12b is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0394] M1a, M1c, and M1d are independently 0 or 1; and
[0395] M12c is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12.
[0396] In another embodiment, the invention provides a compound of
any one of formulae 1-151 wherein:
[0397] A.sup.0 is A.sup.1;
[0398] A.sup.1 is
##STR00129##
[0399] A.sup.3 is:
##STR00130##
[0400] Y.sup.1 is independently O, S, N(R.sup.x), N(O)(R.sup.x),
N(OR.sup.x), N(O)(OR.sup.x), or N(N(R.sup.x)(R.sup.x));
[0401] Y.sup.2 is independently a bond, O, N(R.sup.x),
N(O)(R.sup.x), N(OR.sup.x), N(O)(OR.sup.x), N(N(R.sup.x)(R.sup.x)),
--S(O).sub.M2--, or --S(O).sub.M2--S(O).sub.M2--;
[0402] R.sup.x is independently H, W.sup.3, a protecting group, or
the formula:
##STR00131##
[0403] R.sup.y is independently H, W.sup.3, R.sup.2 or a protecting
group;
[0404] R.sup.1 is independently H or alkyl of 1 to 18 carbon
atoms;
[0405] R.sup.2 is independently H, R.sup.3 or R.sup.4 wherein each
R.sup.4 is independently substituted with 0 to 3 R.sup.3
groups;
[0406] R.sup.3 is R.sup.3, R.sup.3b, R.sup.3c or R.sup.3d, provided
that when R.sup.3 is bound to a heteroatom, then R.sup.3 is
R.sup.3c or R.sup.3d;
[0407] R.sup.3a is F, Cl, Br, I, --CN, N.sub.3 or --NO.sub.2;
[0408] R.sup.3b is Y.sup.1;
[0409] R.sup.3c is --R.sup.x, N(R.sup.x)(R.sup.x), --SR.sup.x,
--S(O)R.sup.x, --S(O).sub.2R.sup.x, --S(O)(OR.sup.x),
--S(O).sub.2(OR.sup.x), --OC(Y.sup.1)R.sup.x,
--OC(Y.sup.1)OR.sup.x, --OC(Y.sup.1)(N(R.sup.x)(R.sup.x)),
--SC(Y.sup.1)R.sup.x, --SC(Y.sup.1)OR.sup.x,
--SC(Y.sup.1)(N(R.sup.x)(R.sup.x)), --N(R.sup.x)C(Y.sup.1)R.sup.x,
N(R.sup.x)C(Y.sup.1)OR.sup.x, or
--N(R.sup.x)C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0410] R.sup.3d is --C(Y.sup.1)R.sup.x, --C(Y.sup.1)OR.sup.x or
--C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0411] R.sup.4 is an alkyl of 1 to 18 carbon atoms, alkenyl of 2 to
18 carbon atoms, or alkynyl of 2 to 18 carbon atoms;
[0412] R.sup.5 is R.sup.4 wherein each R.sup.4 is substituted with
0 to 3 R.sup.3 groups;
[0413] R.sup.5a is independently alkylene of 1 to 18 carbon atoms,
alkenylene of 2 to 18 carbon atoms, or alkynylene of 2-18 carbon
atoms any one of which alkylene, alkenylene or alkynylene is
substituted with 0-3 R.sup.3 groups;
[0414] W.sup.3 is W.sup.4 or W.sup.5;
[0415] W.sup.4 is R.sup.5, --C(Y.sup.1)R.sup.5,
--C(Y.sup.1)W.sup.5, --SO.sub.2R.sup.5, or --SO.sub.2W.sup.5;
[0416] W.sup.5 is carbocycle or heterocycle wherein W.sup.5 is
independently substituted with 0 to 3 R.sup.2 groups;
[0417] W.sup.6 is W.sup.3 independently substituted with 1, 2, or 3
A.sup.3 groups;
[0418] M2 is 0, 1 or 2;
[0419] M12a is 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0420] M12b is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0421] M1a, M1c, and M1d are independently 0 or 1; and
[0422] M12c is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12.
[0423] In another specific embodiment, the invention provides a
compound of the formula:
[DRUG]-[L-P(.dbd.Y.sup.1)--Y.sup.2--R.sup.x].sub.nn
[0424] or a pharmaceutically acceptable salt thereof wherein,
[0425] DRUG is a compound of any one of formulae 500-547;
[0426] Y.sup.1 is independently O, S, N(R.sup.x), N(O)(R.sup.x),
N(OR.sup.x), N(O)(OR.sup.x), or N(N(R.sup.x)(R.sup.x));
[0427] Y.sup.2 is independently a bond, O, N(R.sup.x),
N(O)(R.sup.x), N(OR.sup.x), N(O)(OR.sup.x), N(N(R.sup.x)(R.sup.x)),
--S(O).sub.M2--, or --S(O).sub.M2--S(O).sub.M2--;
[0428] R.sup.x is independently H, W.sup.3, a protecting group, or
the formula:
##STR00132##
[0429] R.sup.y is independently H, W.sup.3, R.sup.2 or a protecting
group;
[0430] R.sup.2 is independently H, R.sup.3 or R.sup.4 wherein each
R.sup.4 is independently substituted with 0 to 3 R.sup.3
groups;
[0431] R.sup.3 is R.sup.3a, R.sup.3b, R.sup.3c or R.sup.3d,
provided that when R.sup.3 is bound to a heteroatom, then R.sup.3
is R.sup.3c or R.sup.3d
[0432] R.sup.3a is F, Cl, Br, I, --CN, N.sub.3 or --NO.sub.2;
[0433] R.sup.3b is Y.sup.1;
[0434] R.sup.3c is R.sup.x, N(R.sup.x)(R.sup.x), --SR.sup.x,
--S(O)R.sup.x, --S(O).sub.2R.sup.x, --S(O)(OR.sup.x),
--S(O).sub.2(OR.sup.x),
--OC(Y.sup.1)R.sup.x, --OC(Y.sup.1)OR.sup.x,
--OC(Y.sup.1)(N(R.sup.x)(R.sup.x)), --SC(Y.sup.1)R.sup.x,
SC(Y.sup.1)OR.sup.x, --SC(Y.sup.1)(N(R.sup.x)(R.sup.x)),
--N(R.sup.x)C(Y.sup.1)R.sup.x, --N(R.sup.x)C(Y.sup.1)OR.sup.x, or
--N(R.sup.x)C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0435] R.sup.3d is --C(Y.sup.1)R.sup.x, --C(Y.sup.1)OR.sup.x or
--C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0436] R.sup.4 is an alkyl of 1 to 18 carbon atoms, alkenyl of 2 to
18 carbon atoms, or alkynyl of 2 to 18 carbon atoms;
[0437] R.sup.5 is R.sup.4 wherein each R.sup.4 is substituted with
0 to 3 R.sup.3 groups;
[0438] W.sup.3 is W.sup.4 or W.sup.5;
[0439] W.sup.4 is R.sup.5, --C(Y.sup.1)R.sup.5,
--C(Y.sup.1)W.sup.5, --SO.sub.2R.sup.5, or --SO.sub.2W.sup.5;
[0440] W.sup.5 is carbocycle or heterocycle wherein W.sup.5 is
independently substituted with 0 to 3 R.sup.2 groups;
[0441] M2 is 1, 2, or 3;
[0442] M1a, M1c, and M1d are independently 0 or 1;
[0443] M12c is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0444] nn is 1, 2, or 3; and
[0445] L is a linking group.
[0446] In another specific embodiment, the invention provides a
compound of which is a compound of the formula:
[DRUG]-(A.sup.0).sub.nn
or a pharmaceutically acceptable salt thereof wherein,
[0447] DRUG is a compound of any one of formulae 500-547;
[0448] nn is 1, 2, or 3;
[0449] A.sup.0 is A.sup.1, A.sup.2, or W.sup.3 with the proviso
that the compound includes at least one A.sup.1;
[0450] A.sup.1 is:
##STR00133##
[0451] A.sup.2 is:
##STR00134##
[0452] A.sup.3 is:
##STR00135##
[0453] Y.sup.1 is independently O, S, N(R.sup.x), N(O)(R.sup.x),
N(OR.sup.x), N(O)(OR.sup.x), or N(N(R.sup.x)(R.sup.x));
[0454] Y.sup.2 is independently a bond, O, N(R.sup.x),
N(O)(R.sup.x), N(OR.sup.x), N(O)(OR.sup.x), N(N(R.sup.x)(R.sup.x)),
--S(O).sub.M2--, or --S(O).sub.M2--S(O).sub.M2--;
[0455] R.sup.x is independently H, W.sup.3, a protecting group, or
the formula:
##STR00136##
[0456] R.sup.y is independently H, W.sup.3, R.sup.2 or a protecting
group;
[0457] R.sup.2 is independently H, R.sup.3 or R.sup.4 wherein each
R.sup.4 is independently substituted with 0 to 3 R.sup.3
groups;
[0458] R.sup.3 is R.sup.3a, R.sup.3b, R.sup.3c or R.sup.3d,
provided that when R.sup.3 is bound to a heteroatom, then R.sup.3
is R.sup.3c or R.sup.3d;
[0459] R.sup.3a is F, Cl, Br, I, --CN, N.sub.3 or --NO.sub.2;
[0460] R.sup.3b is y;
[0461] R.sup.3c is R.sup.x, N(R.sup.x)(R.sup.x), --SR.sup.x,
--S(O)R.sup.x, --S(O).sub.2R.sup.x, --S(O)(OR.sup.x),
--S(O).sub.2(OR.sup.x),
--OC(Y.sup.1)R.sup.x, --OC(Y.sup.1)OR.sup.x,
--OC(Y.sup.1)(N(R.sup.x)(R.sup.x)), --SC(Y.sup.1)R.sup.x,
--SC(Y.sup.1)OR.sup.x, --SC(Y.sup.1)(N(R.sup.x)(R.sup.x)),
--N(R.sup.x)C(Y.sup.1)R.sup.x, --N(R.sup.x)C(Y.sup.1)OR.sup.x, or
--N(R.sup.x)C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0462] R.sup.3d is --C(Y.sup.1)R.sup.x, --C(Y.sup.1)OR.sup.x or
--C(Y.sup.1)(N(R.sup.x)(R.sup.x));
[0463] R.sup.4 is an alkyl of 1 to 18 carbon atoms, alkenyl of 2 to
18 carbon atoms, or alkynyl of 2 to 18 carbon atoms;
[0464] R.sup.5 is R.sup.4 wherein each R.sup.4 is substituted with
0 to 3 R.sup.3 groups;
[0465] W.sup.3 is W.sup.4 or W.sup.5;
[0466] W.sup.4 is R.sup.5, --C(Y.sup.1)R.sup.5,
--C(Y.sup.1)W.sup.5, --SO.sub.2R.sup.5, or --SO.sub.2W.sup.5;
[0467] W.sup.5 is carbocycle or heterocycle wherein W.sup.5 is
independently substituted with 0 to 3 R.sup.2 groups;
[0468] W.sup.6 is W.sup.3 independently substituted with 1, 2, or 3
A.sup.3 groups;
[0469] M2 is 0, 1 or 2;
[0470] M12a is 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0471] M12b is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12;
[0472] M1a, M1e, and M1d are independently 0 or 1; and
[0473] M12c is 0, 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, 11 or 12.
[0474] In compounds of the invention W.sup.5 carbocycles and
W.sup.5 heterocycles may be independently substituted with 0 to 3
R.sup.2 groups. W.sup.5 may be a saturated, unsaturated or aromatic
ring comprising a mono- or bicyclic carbocycle or heterocycle.
W.sup.5 may have 3 to 10 ring atoms, e.g., 3 to 7 ring atoms. The
W.sup.5 rings are saturated when containing 3 ring atoms, saturated
or mono-unsaturated when containing 4 ring atoms, saturated, or
mono- or di-unsaturated when containing 5 ring atoms, and
saturated, mono- or di-unsaturated, or aromatic when containing 6
ring atoms.
[0475] A W.sup.5 heterocycle may be a monocycle having 3 to 7 ring
members (2 to 6 carbon atoms and 1 to 3 heteroatoms selected from
N, O, P, and S) or a bicycle having 7 to 10 ring members (4 to 9
carbon atoms and 1 to 3 heteroatoms selected from N, O, P, and S).
W.sup.5 heterocyclic monocycles may have 3 to 6 ring atoms (2 to 5
carbon atoms and 1 to 2 heteroatoms selected from N, O, and S); or
5 or 6 ring atoms (3 to 5 carbon atoms and 1 to 2 heteroatoms
selected from N and S). W.sup.5 heterocyclic bicycles have 7 to 10
ring atoms (6 to 9 carbon atoms and 1 to 2 heteroatoms selected
from N, O, and S) arranged as a bicyclo [4,5], [5,5], [5,6], or
[6,6] system; or 9 to 10 ring atoms (8 to 9 carbon atoms and 1 to 2
hetero atoms selected from N and S) arranged as a bicyclo [5,6] or
[6,6] system. The W.sup.5 heterocycle may be bonded to Y.sup.2
through a carbon, nitrogen, sulfur or other atom by a stable
covalent bond.
[0476] W.sup.5 heterocycles include for example, pyridyl,
dihydropyridyl isomers, piperidine, pyridazinyl, pyrimidinyl,
pyrazinyl, s-triazinyl, oxazolyl, imidazolyl, thiazolyl,
isoxazolyl, pyrazolyl, isothiazolyl, furanyl, thiofuranyl, thienyl,
and pyrrolyl. W.sup.5 also includes, but is not limited to,
examples such as:
##STR00137##
[0477] W.sup.5 carbocycles and heterocycles may be independently
substituted with 0 to 3 R.sup.2 groups, as defined above. For
example, substituted W.sup.5 carbocycles include:
##STR00138##
[0478] Examples of substituted phenyl carbocycles include:
##STR00139##
Linking Groups and Linkers
[0479] The invention provides conjugates that comprise an
immuno-modulatory compound that is linked to one or more
phosphonate groups either directly (e.g. through a covalent bond)
or through a linking group (i.e. a linker). The nature of the
linker is not critical provided it does not interfere with the
ability of the phosphonate containing compound to function as a
therapeutic agent. The phosphonate or the linker can be linked to
the compound (e.g. a compound of Formulae 500-547) at any
synthetically feasible position on the compound by removing a
hydrogen or any portion of the compound to provide an open valence
for attachment of the phosphonate or the linker.
[0480] In one embodiment of the invention the linking group or
linker (which can be designated "L") can include all or a portions
of the group A.sup.0, A.sup.1, A.sup.2, or W.sup.3 described
herein.
[0481] In another embodiment of the invention the linking group or
linker has a molecular weight of from about 20 daltons to about 400
daltons.
[0482] In another embodiment of the invention the linking group or
linker has a length of about 5 angstroms to about 300
angstroms.
[0483] In another embodiment of the invention the linking group or
linker separates the DRUG and a P(.dbd.Y.sup.1) residue by about 5
angstroms to about 200 angstroms, inclusive, in length.
[0484] In another embodiment of the invention the linking group or
linker is a divalent, branched or unbranched, saturated or
unsaturated, hydrocarbon chain, having from 2 to 25 carbon atoms,
wherein one or more (e.g. 1, 2, 3, or 4) of the carbon atoms is
optionally replaced by (--O--), and wherein the chain is optionally
substituted on carbon with one or more (e.g. 1, 2, 3, or 4)
substituents selected from (C.sub.1-C.sub.6)alkoxy,
(C.sub.3-C.sub.6)cycloalkyl, (C.sub.1-C.sub.6)alkanoyl,
(C.sub.1-C.sub.6)alkanoyloxy, (C.sub.1-C.sub.6)alkoxycarbonyl,
(C.sub.1-C.sub.6)alkylthio, azido, cyano, nitro, halo, hydroxy, oxo
(.dbd.O), carboxy, aryl, aryloxy, heteroaryl, and
heteroaryloxy.
[0485] In another embodiment of the invention the linking group or
linker is of the formula W-A wherein A is (C.sub.1-C.sub.24)alkyl,
(C.sub.2-C.sub.24)alkenyl, (C.sub.2-C.sub.24)alkynyl,
(C.sub.3-C.sub.8)cycloalkyl, (C.sub.6-C.sub.10)aryl or a
combination thereof, wherein W is --N(R)C(.dbd.O)--,
--C(.dbd.O)N(R)--, --OC(.dbd.O)--, --C(.dbd.O)O--, --O--, --S--,
--S(O)--, --S(O).sub.2--, --N(R)--, --C(.dbd.O)--, or a direct
bond; wherein each R is independently H or
(C.sub.1-C.sub.6)alkyl.
[0486] In another embodiment of the invention the linking group or
linker is a divalent radical formed from a peptide.
[0487] In another embodiment of the invention the linking group or
linker is a divalent radical formed from an amino acid.
[0488] In another embodiment of the invention the linking group or
linker is a divalent radical formed from poly-L-glutamic acid,
poly-L-aspartic acid, poly-L-histidine, poly-L-ornithine,
poly-L-serine, poly-L-threonine, poly-L-tyrosine, poly-L-leucine,
poly-L-lysine-L-phenylalanine, poly-L-lysine or
poly-L-lysine-L-tyrosine.
[0489] In another embodiment of the invention the linking group or
linker is of the formula W--(CH.sub.2).sub.n wherein, n is between
about 1 and about 10; and W is --N(R)C(.dbd.O)--,
--C(.dbd.O)N(R)--, --OC(.dbd.O)--, --C(.dbd.O)O--, --O--, --S--,
--S(O)--, --S(O).sub.2--, --C(.dbd.O)--, --N(R)--, or a direct
bond; wherein each R is independently H or
(C.sub.1-C.sub.6)alkyl.
[0490] In another embodiment of the invention the linking group or
linker is methylene, ethylene, or propylene.
[0491] In another embodiment of the invention the linking group or
linker is attached to the phosphonate group through a carbon atom
of the linker.
Compounds
[0492] The compounds of the invention include those with
immuno-modulatory activity. The compounds of the inventions bear
one or more (e.g. 1, 2, 3, or 4) phosphonate groups, which may be a
prodrug moiety.
[0493] Typically, compounds of the invention have a molecular
weight of from about 400 amu to about 10,000 amu; in a specific
embodiment of the invention, compounds have a molecular weight of
less than about 5000 amu; in another specific embodiment of the
invention, compounds have a molecular weight of less than about
2500 amu; in another specific embodiment of the invention,
compounds have a molecular weight of less than about 1000 amu; in
another specific embodiment of the invention, compounds have a
molecular weight of less than about 800 amu; in another specific
embodiment of the invention, compounds have a molecular weight of
less than about 600 amu; and in another specific embodiment of the
invention, compounds have a molecular weight of less than about 600
amu and a molecular weight of greater than about 400 amu.
[0494] The compounds of the invention also typically have a
logD(polarity) less than about 5. In one embodiment the invention
provides compounds having a logD less than about 4; in another one
embodiment the invention provides compounds having a logD less than
about 3; in another one embodiment the invention provides compounds
having a logD greater than about -5; in another one embodiment the
invention provides compounds having a logD greater than about -3;
and in another one embodiment the invention provides compounds
having a logD greater than about 0 and less than about 3.
[0495] Selected substituents within the compounds of the invention
are present to a recursive degree. In this context, "recursive
substituent" means that a substituent may recite another instance
of itself. Because of the recursive nature of such substituents,
theoretically, a large number may be present in any given claim.
For example, R.sup.x contains a R.sup.y substituent. R.sup.y can be
R.sup.2, which in turn can be R.sup.3. If R.sup.3 is selected to be
R.sup.3c, then a second instance of R.sup.x can be selected. One of
ordinary skill in the art of medicinal chemistry understands that
the total number of such substituents is reasonably limited by the
desired properties of the compound intended. Such properties
include, by of example and not limitation, physical properties such
as molecular weight, solubility or log P, application properties
such as activity against the intended target, and practical
properties such as ease of synthesis.
[0496] By way of example and not limitation, W.sup.3, R.sup.y and
R.sup.3 are all recursive substituents in certain claims.
Typically, each of these may independently occur 20, 19, 18, 17,
16, 15, 14, 13, 12, 11, 10, 9, 8, 7, 6, 5, 4, 3, 2, 1, or 0, times
in a given claim. More typically, each of these may independently
occur 12 or fewer times in a given claim. More typically yet,
W.sup.3 will occur 0 to 8 times, R.sup.y will occur 0 to 6 times
and R.sup.3 will occur 0 to 10 times in a given claim. Even more
typically, W.sup.3 will occur 0 to 6 times, R.sup.y will occur 0 to
4 times and R.sup.3 will occur 0 to 8 times in a given claim.
[0497] Recursive substituents are an intended aspect of the
invention. One of ordinary skill in the art of medicinal chemistry
understands the versatility of such substituents. To the degree
that recursive substituents are present in an claim of the
invention, the total number will be determined as set forth
above.
[0498] Whenever a compound described herein is substituted with
more than one of the same designated group, e.g., "R.sup.1" or
"R.sup.6a", then it will be understood that the groups may be the
same or different, i.e., each group is independently selected. Wavy
lines indicate the site of covalent bond attachments to the
adjoining groups, moieties, or atoms.
[0499] The term immuno-modulatory compound also includes
pimecrolimus, everolimus, sirolimus, tacrolimus, prednisolone,
VX-148, merimepodib, brequinar, thalidomide, BCX-1777, revimid,
diprolene, aclometasone dipropionate, hydrocortisone,
dexamethasone, leflunomide, methylprednisolone suleptanate,
prednisone, clobetasol, MNA-715 (FK778), SMP-114, teriflunomide,
halobetasol, ciclesonide, deflazacort, medroxyprogesterone,
budesonide, rimexolone, triamcinolone acetonide, fluticasone,
mometasone furoate, methylprednisolone aceponate, cyclosporin A,
tacrolimus, mycophenolate, ANA-245, immunosuppressive macrolide,
methotrexate, PNP-405, MDL-74428,
9-(3,3-dimethyl-5-phosphonopentyl) guanine, DADMe-IMMG, CP-690,550,
mycophenate, cyclosporin, and mizoribine.
[0500] In one embodiment of the invention, the compound is in
isolated and purified form. Generally, the term "isolated and
purified" means that the compound is significantly free of
biological materials (e.g. blood, cells, etc.). In one specific
embodiment of the invention, the term means that the compound or
conjugate of the invention is at least about 50% pure by weight in
a mixture; in another specific embodiment, the term means that the
compound or conjugate of the invention is at least about 75% pure
by weight in a mixture; in another specific embodiment, the term
means that the compound or conjugate of the invention is at least
about 90% pure by weight in a mixture; in another specific
embodiment, the term means that the compound or conjugate of the
invention is at least about 98% pure by weight in a mixture; and in
another embodiment, the term means that the compound or conjugate
of the invention is at least about 99% pure by weight in a mixture.
In another specific embodiment, the invention provides a compound
or conjugate of the invention that has been synthetically prepared
(e.g. prepared ex vivo).
Intracellular Targeting
[0501] The phosphonate group of the compounds of the invention may
cleave in vivo in stages after they have reached the desired site
of action, i.e. inside a cell. One mechanism of action inside a
cell may entail a first cleavage, e.g. by esterase, to provide a
negatively-charged "locked-in" intermediate. Cleavage of a terminal
ester grouping in a compound of the invention thus affords an
unstable intermediate which releases a negatively charged "locked
in" intermediate.
[0502] After passage inside a cell, intracellular enzymatic
cleavage or modification of the phosphonate or prodrug compound may
result in an intracellular accumulation of the cleaved or modified
compound by a "trapping" mechanism. The cleaved or modified
compound may then be "locked-in" the cell by a significant change
in charge, polarity, or other physical property change which
decreases the rate at which the cleaved or modified compound can
exit the cell, relative to the rate at which it entered as the
phosphonate prodrug. Other mechanisms by which a therapeutic effect
are achieved may be operative as well. Enzymes which are capable of
an enzymatic activation mechanism with the phosphonate prodrug
compounds of the invention include, but are not limited to,
amidases, esterases, microbial enzymes, phospholipases,
cholinesterases, and phosphatases.
[0503] From the foregoing, it will be apparent that many different
drugs can be derivatized in accord with the present invention.
Numerous such drugs are specifically mentioned herein. However, it
should be understood that the discussion of drug families and their
specific members for derivatization according to this invention is
not intended to be exhaustive, but merely illustrative.
[0504] In one embodiment of the invention, the compound is not an
antiviral agent compound. In another embodiment the compound is not
a nucleoside compound. In another embodiment the compound is not an
IMPDH inhibitor compound. In another embodiment the compound is not
an antimetabolite compound. In another embodiment the compound is
not a PNP inhibitor. In another embodiment the compound is not a
substituted compound of any one of formulae 500-533, 535-541, or
543-547. In another embodiment the compound is not a substituted
compound of any one of one of formulae 1-104, 107-124, or
128-151.
Stereoisomers
[0505] The compounds of the invention may have chiral centers,
e.g., chiral carbon or phosphorus atoms. The compounds of the
invention thus include racemic mixtures of all stereoisomers,
including enantiomers, diastereomers, and atropisomers. In
addition, the compounds of the invention include enriched or
resolved optical isomers at any or all asymmetric, chiral atoms. In
other words, the chiral centers apparent from the depictions are
provided as the chiral isomers or racemic mixtures. Both racemic
and diastereomeric mixtures, as well as the individual optical
isomers isolated or synthesized, substantially free of their
enantiomeric or diastereomeric partners, are all within the scope
of the invention. The racemic mixtures are separated into their
individual, substantially optically pure isomers through well-known
techniques such as, for example, the separation of diastereomeric
salts formed with optically active adjuncts, e.g., acids or bases
followed by conversion back to the optically active substances. In
most instances, the desired optical isomer is synthesized by means
of stereospecific reactions, beginning with the appropriate
stereoisomer of the desired starting material.
[0506] The compounds of the invention can also exist as tautomeric
isomers in certain cases. All though only one delocalized resonance
structure may be depicted, all such forms are contemplated within
the scope of the invention. For example, ene-amine tautomers can
exist for purine, pyrimidine, imidazole, guanidine, amidine, and
tetrazole systems and all their possible tautomeric forms are
within the scope of the invention.
Salts and Hydrates
[0507] The compositions of this invention optionally comprise salts
of the compounds herein, especially pharmaceutically acceptable
non-toxic salts containing, for example, Na.sup.+, Li.sup.+,
K.sup.+, Ca.sup.+2 and Mg.sup.+2. Such salts may include those
derived by combination of appropriate cations such as alkali and
alkaline earth metal ions or ammonium and quaternary amino ions
with an acid anion moiety, typically a carboxylic acid. Monovalent
salts are preferred if a water soluble salt is desired.
[0508] Metal salts typically are prepared by reacting the metal
hydroxide with a compound of this invention. Examples of metal
salts which are prepared in this way are salts containing Li.sup.+,
Na.sup.+, and K.sup.+. A less soluble metal salt can be
precipitated from the solution of a more soluble salt by addition
of the suitable metal compound.
[0509] In addition, salts may be formed from acid addition of
certain organic and inorganic acids, e.g., HCl, HBr,
H.sub.2SO.sub.4, H.sub.3PO.sub.4 or organic sulfonic acids, to
basic centers, typically amines, or to acidic groups. Finally, it
is to be understood that the compositions herein comprise compounds
of the invention in their un-ionized, as well as zwitterionic form,
and combinations with stoichiometric amounts of water as in
hydrates.
[0510] Also included within the scope of this invention are the
salts of the parental compounds with one or more amino acids. Any
of the amino acids described above are suitable, especially the
naturally-occurring amino acids found as protein components,
although the amino acid typically is one bearing a side chain with
a basic or acidic group, e.g., lysine, arginine or glutamic acid,
or a neutral group such as glycine, serine, threonine, alanine,
isoleucine, or leucine.
Methods of Inhibition of Immuno-Modulation
[0511] Another aspect of the invention relates to methods of
inhibiting the activity of immuno-modulators comprising the step of
treating a sample suspected of containing an immuno-modulator with
a composition of the invention.
[0512] Compositions of the invention may act as inhibitors of
immune-modulation, as intermediates for such inhibitors or have
other utilities as described below. The inhibitors will bind to
locations on the surface or in a cavity of an immuno-modulator
having a geometry unique to immuno-modulators. Compositions binding
immuno-modulators may bind with varying degrees of reversibility.
Those compounds binding substantially irreversibly are ideal
candidates for use in this method of the invention. Once labeled,
the substantially irreversibly binding compositions are useful as
probes for the detection of immune-modulation. Accordingly, the
invention relates to methods of detecting immune-modulation in a
sample suspected of containing an immuno-modulator comprising the
steps of: treating a sample suspected of containing an
immuno-modulator with a composition comprising a compound of the
invention bound to a label; and observing the effect of the sample
on the activity of the label. Suitable labels are well known in the
diagnostics field and include stable free radicals, fluorophores,
radioisotopes, enzymes, chemiluminescent groups and chromogens. The
compounds herein are labeled in conventional fashion using
functional groups such as hydroxyl or amino.
[0513] Within the context of the invention samples suspected of
containing an immuno-modulator include natural or man-made
materials such as living organisms; tissue or cell cultures;
biological samples such as biological material samples (blood,
serum, urine, cerebrospinal fluid, tears, sputum, saliva, tissue
samples, and the like); laboratory samples; food, water, or air
samples; bioproduct samples such as extracts of cells, particularly
recombinant cells synthesizing a desired glycoprotein; and the
like. Typically the sample will be suspected of containing an
immuno-modulator. Samples can be contained in any medium including
water and organic solvent/water mixtures. Samples include living
organisms such as humans, and man made materials such as cell
cultures.
[0514] The treating step of the invention comprises adding the
composition of the invention to the sample or it comprises adding a
precursor of the composition to the sample. The addition step
comprises any method of administration as described above.
[0515] If desired, the activity of an immuno-modulator, after
application of the composition, can be observed by any method
including direct and indirect methods of detecting imm,
uno-modulator activity. Quantitative, qualitative, and
semiquantitative methods of determining immuno-modulation activity
are all contemplated. Typically one of the screening methods
described above are applied, however, any other method such as
observation of the physiological properties of a living organism
are also applicable.
[0516] However, in screening compounds capable of inhibiting
immuno-modulation it should be kept in mind that the results of
enzyme assays may not correlate with cell culture assays. Thus, a
cell based assay should be the primary screening tool.
Screens for Immuno-Modulating Inhibitors
[0517] Compositions of the invention are screened for inhibitory
activity against immuno-modulators by any of the conventional
techniques for evaluating enzyme activity. Within the context of
the invention, typically compositions are first screened for
inhibition of immuno-modulators in vitro and compositions showing
inhibitory activity are then screened for activity in vivo.
Compositions having in vitro Ki (inhibitory constants) of less then
about 5.times.10.sup.-6 M, typically less than about
1.times.10.sup.-7 M and preferably less than about
5.times.10.sup.-8 M are preferred for in vivo use.
[0518] Useful in vitro screens have been described in detail and
will not be elaborated here. However, the examples describe
suitable in vitro assays.
Pharmaceutical Formulations
[0519] The compounds of this invention are formulated with
conventional carriers and excipients, which will be selected in
accord with ordinary practice. Tablets will contain excipients,
glidants, fillers, binders and the like. Aqueous formulations are
prepared in sterile form, and when intended for delivery by other
than oral administration generally will be isotonic. All
formulations will optionally contain excipients such as those set
forth in the Handbook of Pharmaceutical Excipients (1986).
Excipients include ascorbic acid and other antioxidants, chelating
agents such as EDTA, carbohydrates such as dextrin,
hydroxyalkylcellulose, hydroxyalkylmethylcellulose, stearic acid
and the like. The pH of the formulations ranges from about 3 to
about 11, but is ordinarily about 7 to 10.
[0520] While it is possible for the active ingredients to be
administered alone it may be preferable to present them as
pharmaceutical formulations. The formulations, both for veterinary
and for human use, of the invention comprise at least one active
ingredient, as above defined, together with one or more acceptable
carriers therefor and optionally other therapeutic ingredients. The
carrier(s) must be "acceptable" in the sense of being compatible
with the other ingredients of the formulation and physiologically
innocuous to the recipient thereof.
[0521] The formulations include those suitable for the foregoing
administration routes. The formulations may conveniently be
presented in unit dosage form and may be prepared by any of the
methods well known in the art of pharmacy. Techniques and
formulations generally are found in Remington's Pharmaceutical
Sciences (Mack Publishing Co., Easton, Pa.). Such methods include
the step of bringing into association the active ingredient with
the carrier which constitutes one or more accessory ingredients. In
general the formulations are prepared by uniformly and intimately
bringing into association the active ingredient with liquid
carriers or finely divided solid carriers or both, and then, if
necessary, shaping the product.
[0522] Formulations of the present invention suitable for oral
administration may be presented as discrete units such as capsules,
cachets or tablets each containing a predetermined amount of the
active ingredient; as a powder or granules; as a solution or a
suspension in an aqueous or non-aqueous liquid; or as an
oil-in-water liquid emulsion or a water-in-oil liquid emulsion. The
active ingredient may also be administered as a bolus, electuary or
paste.
[0523] A tablet is made by compression or molding, optionally with
one or more accessory ingredients. Compressed tablets may be
prepared by compressing in a suitable machine the active ingredient
in a free-flowing form such as a powder or granules, optionally
mixed with a binder, lubricant, inert diluent, preservative,
surface active or dispersing agent. Molded tablets may be made by
molding in a suitable machine a mixture of the powdered active
ingredient moistened with an inert liquid diluent. The tablets may
optionally be coated or scored and optionally are formulated so as
to provide slow or controlled release of the active ingredient
therefrom.
[0524] For administration to the eye or other external tissues
e.g., mouth and skin, the formulations are preferably applied as a
topical ointment or cream containing the active ingredient(s) in an
amount of, for example, 0.075 to 20% w/w (including active
ingredient(s) in a range between 0.1% and 20% in increments of 0.1%
w/w such as 0.6% w/w, 0.7% w/w, etc.), preferably 0.2 to 15% w/w
and most preferably 0.5 to 10% w/w. When formulated in an ointment,
the active ingredients may be employed with either a paraffinic or
a water-miscible ointment base. Alternatively, the active
ingredients may be formulated in a cream with an oil-in-water cream
base.
[0525] If desired, the aqueous phase of the cream base may include,
for example, at least 30% w/w of a polyhydric alcohol, i.e. an
alcohol having two or more hydroxyl groups such as propylene
glycol, butane 1,3-diol, mannitol, sorbitol, glycerol and
polyethylene glycol (including PEG 400) and mixtures thereof. The
topical formulations may desirably include a compound which
enhances absorption or penetration of the active ingredient through
the skin or other affected areas. Examples of such dermal
penetration enhancers include dimethyl sulphoxide and related
analogs.
[0526] The oily phase of the emulsions of this invention may be
constituted from known ingredients in a known manner. While the
phase may comprise merely an emulsifier (otherwise known as an
emulgent), it desirably comprises a mixture of at least one
emulsifier with a fat or an oil or with both a fat and an oil.
Preferably, a hydrophilic emulsifier is included together with a
lipophilic emulsifier which acts as a stabilizer. It is also
preferred to include both an oil and a fat. Together, the
emulsifier(s) with or without stabilizer(s) make up the so-called
emulsifying wax, and the wax together with the oil and fat make up
the so-called emulsifying ointment base which forms the oily
dispersed phase of the cream formulations.
[0527] Emulgents and emulsion stabilizers suitable for use in the
formulation of the invention include Tween.RTM. 60, Span.RTM. 80,
cetostearyl alcohol, benzyl alcohol, myristyl alcohol, glyceryl
mono-stearate and sodium lauryl sulfate.
[0528] The choice of suitable oils or fats for the formulation is
based on achieving the desired cosmetic properties. The cream
should preferably be a non-greasy, non-staining and washable
product with suitable consistency to avoid leakage from tubes or
other containers. Straight or branched chain, mono- or dibasic
alkyl esters such as di-isoadipate, isocetyl stearate, propylene
glycol diester of coconut fatty acids, isopropyl myristate, decyl
oleate, isopropyl palmitate, butyl stearate, 2-ethylhexyl palmitate
or a blend of branched chain esters known as Crodamol CAP may be
used, the last three being preferred esters. These may be used
alone or in combination depending on the properties required.
Alternatively, high melting point lipids such as white soft
paraffin and/or liquid paraffin or other mineral oils are used.
[0529] Pharmaceutical formulations according to the present
invention comprise one or more compounds of the invention together
with one or more pharmaceutically acceptable carriers or excipients
and optionally other therapeutic agents. Pharmaceutical
formulations containing the active ingredient may be in any form
suitable for the intended method of administration. When used for
oral use for example, tablets, troches, lozenges, aqueous or oil
suspensions, dispersible powders or granules, emulsions, hard or
soft capsules, syrups or elixirs may be prepared. Compositions
intended for oral use may be prepared according to any method known
to the art for the manufacture of pharmaceutical compositions and
such compositions may contain one or more agents including
sweetening agents, flavoring agents, coloring agents and preserving
agents, in order to provide a palatable preparation. Tablets
containing the active ingredient in admixture with non-toxic
pharmaceutically acceptable excipient which are suitable for
manufacture of tablets are acceptable. These excipients may be, for
example, inert diluents, such as calcium or sodium carbonate,
lactose, lactose monohydrate, croscarmellose sodium, povidone,
calcium or sodium phosphate; granulating and disintegrating agents,
such as maize starch, or alginic acid; binding agents, such as
cellulose, microcrystalline cellulose, starch, gelatin or acacia;
and lubricating agents, such as magnesium stearate, stearic acid or
talc. Tablets may be uncoated or may be coated by known techniques
including microencapsulation to delay disintegration and adsorption
in the gastrointestinal tract and thereby provide a sustained
action over a longer period. For example, a time delay material
such as glyceryl monostearate or glyceryl distearate alone or with
a wax may be employed.
[0530] Formulations for oral use may be also presented as hard
gelatin capsules where the active ingredient is mixed with an inert
solid diluent, for example calcium phosphate or kaolin, or as soft
gelatin capsules wherein the active ingredient is mixed with water
or an oil medium, such as peanut oil, liquid paraffin or olive
oil.
[0531] Aqueous suspensions of the invention contain the active
materials in admixture with excipients suitable for the manufacture
of aqueous suspensions. Such excipients include a suspending agent,
such as sodium carboxymethylcellulose, methylcellulose,
hydroxypropyl methylcelluose, sodium alginate,
polyvinylpyrrolidone, gum tragacanth and gum acacia, and dispersing
or wetting agents such as a naturally occurring phosphatide (e.g.,
lecithin), a condensation product of an alkylene oxide with a fatty
acid (e.g., polyoxyethylene stearate), a condensation product of
ethylene oxide with a long chain aliphatic alcohol (e.g.,
heptadecaethyleneoxycetanol), a condensation product of ethylene
oxide with a partial ester derived from a fatty acid and a hexitol
anhydride (e.g., polyoxyethylene sorbitan monooleate). The aqueous
suspension may also contain one or more preservatives such as ethyl
or n-propyl p-hydroxy-benzoate, one or more coloring agents, one or
more flavoring agents and one or more sweetening agents, such as
sucrose or saccharin.
[0532] Oil suspensions may be formulated by suspending the active
ingredient in a vegetable oil, such as arachis oil, olive oil,
sesame oil or coconut oil, or in a mineral oil such as liquid
paraffin. The oral suspensions may contain a thickening agent, such
as beeswax, hard paraffin or cetyl alcohol. Sweetening agents, such
as those set forth above, and flavoring agents may be added to
provide a palatable oral preparation. These compositions may be
preserved by the addition of an antioxidant such as ascorbic
acid.
[0533] Dispersible powders and granules of the invention suitable
for preparation of an aqueous suspension by the addition of water
provide the active ingredient in admixture with a dispersing or
wetting agent, a suspending agent, and one or more preservatives.
Suitable dispersing or wetting agents and suspending agents are
exemplified by those disclosed above. Additional excipients, for
example sweetening, flavoring and coloring agents, may also be
present.
[0534] The pharmaceutical compositions of the invention may also be
in the form of oil-in-water emulsions. The oily phase may be a
vegetable oil, such as olive oil or arachis oil, a mineral oil,
such as liquid paraffin, or a mixture of these. Suitable
emulsifying agents include naturally-occurring gums, such as gum
acacia and gum tragacanth, naturally occurring phosphatides, such
as soybean lecithin, esters or partial esters derived from fatty
acids and hexitol anhydrides, such as sorbitan monooleate, and
condensation products of these partial esters with ethylene oxide,
such as polyoxyethylene sorbitan monooleate. The emulsion may also
contain sweetening and flavoring agents. Syrups and elixirs may be
formulated with sweetening agents, such as glycerol, sorbitol or
sucrose. Such formulations may also contain a demulcent, a
preservative, a flavoring or a coloring agent.
[0535] The pharmaceutical compositions of the invention may be in
the form of a sterile injectable preparation, such as a sterile
injectable aqueous or oleaginous suspension. This suspension may be
formulated according to the known art using those suitable
dispersing or wetting agents and suspending agents which have been
mentioned above. The sterile injectable preparation may also be a
sterile injectable solution or suspension in a non-toxic
parenterally acceptable diluent or solvent, such as a solution in
1,3-butane-diol or prepared as a lyophilized powder. Among the
acceptable vehicles and solvents that may be employed are water,
Ringer's solution and isotonic sodium chloride solution. In
addition, sterile fixed oils may conventionally be employed as a
solvent or suspending medium. For this purpose any bland fixed oil
may be employed including synthetic mono- or diglycerides. In
addition, fatty acids such as oleic acid may likewise be used in
the preparation of injectables.
[0536] The amount of active ingredient that may be combined with
the carrier material to produce a single dosage form will vary
depending upon the host treated and the particular mode of
administration. For example, a time-release formulation intended
for oral administration to humans may contain approximately 1 to
1000 mg of active material compounded with an appropriate and
convenient amount of carrier material which may vary from about 5
to about 95% of the total compositions (weight:weight). The
pharmaceutical composition can be prepared to provide easily
measurable amounts for administration. For example, an aqueous
solution intended for intravenous infusion may contain from about 3
to 500 .mu.g of the active ingredient per milliliter of solution in
order that infusion of a suitable volume at a rate of about 30
mL/hr can occur.
[0537] Formulations suitable for administration to the eye include
eye drops wherein the active ingredient is dissolved or suspended
in a suitable carrier, especially an aqueous solvent for the active
ingredient. The active ingredient is preferably present in such
formulations in a concentration of 0.5 to 20%, advantageously 0.5
to 10% particularly about 1.5% w/w.
[0538] Formulations suitable for topical administration in the
mouth include lozenges comprising the active ingredient in a
flavored basis, usually sucrose and acacia or tragacanth; pastilles
comprising the active ingredient in an inert basis such as gelatin
and glycerin, or sucrose and acacia; and mouthwashes comprising the
active ingredient in a suitable liquid carrier.
[0539] Formulations for rectal administration may be presented as a
suppository with a suitable base comprising for example cocoa
butter or a salicylate.
[0540] Formulations suitable for intrapulmonary or nasal
administration have a particle size for example in the range of 0.1
to 500 microns (including particle sizes in a range between 0.1 and
500 microns in increments microns such as 0.5, 1, 30 microns, 35
microns, etc.), which is administered by rapid inhalation through
the nasal passage or by inhalation through the mouth so as to reach
the alveolar sacs. Suitable formulations include aqueous or oily
solutions of the active ingredient. Formulations suitable for
aerosol or dry powder administration may be prepared according to
conventional methods and may be delivered with other therapeutic
agents such as compounds heretofore used in the treatment or
prophylaxis of infections as described below.
[0541] Formulations suitable for vaginal administration may be
presented as pessaries, tampons, creams, gels, pastes, foams or
spray formulations containing in addition to the active ingredient
such carriers as are known in the art to be appropriate.
[0542] Formulations suitable for parenteral administration include
aqueous and non-aqueous sterile injection solutions which may
contain anti-oxidants, buffers, bacteriostats and solutes which
render the formulation isotonic with the blood of the intended
recipient; and aqueous and non-aqueous sterile suspensions which
may include suspending agents and thickening agents.
[0543] The formulations are presented in unit-dose or multi-dose
containers, for example sealed ampoules and vials, and may be
stored in a freeze-dried (lyophilized) condition requiring only the
addition of the sterile liquid carrier, for example water for
injection, immediately prior to use. Extemporaneous injection
solutions and suspensions are prepared from sterile powders,
granules and tablets of the kind previously described. Preferred
unit dosage formulations are those containing a daily dose or unit
daily sub-dose, as herein above recited, or an appropriate fraction
thereof, of the active ingredient.
[0544] It should be understood that in addition to the ingredients
particularly mentioned above the formulations of this invention may
include other agents conventional in the art having regard to the
type of formulation in question, for example those suitable for
oral administration may include flavoring agents.
[0545] The invention further provides veterinary compositions
comprising at least one active ingredient as above defined together
with a veterinary carrier therefor.
[0546] Veterinary carriers are materials useful for the purpose of
administering the composition and may be solid, liquid or gaseous
materials which are otherwise inert or acceptable in the veterinary
art and are compatible with the active ingredient. These veterinary
compositions may be administered orally, parenterally or by any
other desired route.
[0547] Compounds of the invention can also be formulated to provide
controlled release of the active ingredient to allow less frequent
dosing or to improve the pharmacokinetic or toxicity profile of the
active ingredient. Accordingly, the invention also provided
compositions comprising one or more compounds of the invention
formulated for sustained or controlled release.
[0548] Effective dose of active ingredient depends at least on the
nature of the condition being treated, toxicity, whether the
compound is being used prophylactically (lower doses) or against an
active infection, the method of delivery, and the pharmaceutical
formulation, and will be determined by the clinician using
conventional dose escalation studies. It can be expected to be from
about 0.0001 to about 100 mg/kg body weight per day. Typically,
from about 0.01 to about 10 mg/kg body weight per day. More
typically, from about 0.01 to about 5 mg/kg body weight per day.
More typically, from about 0.05 to about 0.5 mg/kg body weight per
day. For example, the daily candidate dose for an adult human of
approximately 70 kg body weight will range from 1 mg to 1000 mg,
preferably between 5 mg and 500 mg, and may take the form of single
or multiple doses.
Routes of Administration
[0549] One or more compounds of the invention (herein referred to
as the active ingredients) are administered by any route
appropriate to the condition to be treated. Suitable routes include
oral, rectal, nasal, topical (including buccal and sublingual),
vaginal and parenteral (including subcutaneous, intramuscular,
intravenous, intradermal, intrathecal and epidural), and the like.
It will be appreciated that the preferred route may vary with for
example the condition of the recipient. An advantage of the
compounds of this invention is that they are orally bioavailable
and can be dosed orally.
Combination Therapy
[0550] Active ingredients of the invention are also used in
combination with other active ingredients. Such combinations are
selected based on the condition to be treated, cross-reactivities
of ingredients and pharmaco-properties of the combination.
[0551] It is also possible to combine any compound of the invention
with one or more other active ingredients in a unitary dosage form
for simultaneous or sequential administration to a patient. The
combination therapy may be administered as a simultaneous or
sequential regimen. When administered sequentially, the combination
may be administered in two or more administrations.
[0552] The combination therapy may provide "synergy" and
"synergistic effect", i.e. the effect achieved when the active
ingredients used together is greater than the sum of the effects
that results from using the compounds separately. A synergistic
effect may be attained when the active ingredients are: (1)
co-formulated and administered or delivered simultaneously in a
combined formulation; (2) delivered by alternation or in parallel
as separate formulations; or (3) by some other regimen. When
delivered in alternation therapy, a synergistic effect may be
attained when the compounds are administered or delivered
sequentially, e.g., in separate tablets, pills or capsules, or by
different injections in separate syringes. In general, during
alternation therapy, an effective dosage of each active ingredient
is administered sequentially, i.e. serially, whereas in combination
therapy, effective dosages of two or more active ingredients are
administered together.
Metabolites of the Compounds of the Invention
[0553] Also falling within the scope of this invention are the in
vivo metabolic products of the compounds described herein. Such
products may result for example from the oxidation, reduction,
hydrolysis, amidation, esterification and the like of the
administered compound, primarily due to enzymatic processes.
Accordingly, the invention includes compounds produced by a process
comprising contacting a compound of this invention with a mammal
for a period of time sufficient to yield a metabolic product
thereof. Such products typically are identified by preparing a
radiolabelled (e.g., C.sup.14 or H.sup.3) compound of the
invention, administering it parenterally in a detectable dose
(e.g., greater than about 0.5 mg/kg) to an animal such as rat,
mouse, guinea pig, monkey, or to man, allowing sufficient time for
metabolism to occur (typically about 30 seconds to 30 hours) and
isolating its conversion products from the urine, blood or other
biological samples. These products are easily isolated since they
are labeled (others are isolated by the use of antibodies capable
of binding epitopes surviving in the metabolite). The metabolite
structures are determined in conventional fashion, e.g., by MS or
NMR analysis. In general, analysis of metabolites is done in the
same way as conventional drug metabolism studies well-known to
those skilled in the art. The conversion products, so long as they
are not otherwise found in vivo, are useful in diagnostic assays
for therapeutic dosing of the compounds of the invention even if
they possess no immuno-modulation inhibitory activity of their
own.
[0554] Recipes and methods for determining stability of compounds
in surrogate gastrointestinal secretions are known. Compounds are
defined herein as stable in the gastrointestinal tract where less
than about 50 mole percent of the protected groups are deprotected
in surrogate intestinal or gastric juice upon incubation for 1 hour
at 37.degree. C. Simply because the compounds are stable to the
gastrointestinal tract does not mean that they cannot be hydrolyzed
in vivo. The phosphonate prodrugs of the invention typically will
be stable in the digestive system but are substantially hydrolyzed
to the parental drug in the digestive lumen, liver or other
metabolic organ, or within cells in general.
Exemplary Methods of Making the Compounds of the Invention.
[0555] The invention also relates to methods of making the
compositions of the invention. The compositions are prepared by any
of the applicable techniques of organic synthesis. Many such
techniques are well known in the art. However, many of the known
techniques are elaborated in Compendium of Organic Synthetic
Methods (John Wiley & Sons, New York), Vol. 1, Ian T. Harrison
and Shuyen Harrison, 1971; Vol. 2, Ian T. Harrison and Shuyen
Harrison, 1974; Vol. 3, Louis S. Hegedus and Leroy Wade, 1977; Vol.
4, Leroy G. Wade, jr., 1980; Vol. 5, Leroy G. Wade, Jr., 1984; and
Vol. 6, Michael B. Smith; as well as March, J., Advanced Organic
Chemistry, Third Edition, (John Wiley & Sons, New York, 1985),
Comprehensive Organic Synthesis. Selectivity, Strategy &
Efficiency in Modern Organic Chemistry. In 9 Volumes, Barry M.
Trost, Editor-in-Chief (Pergamon Press, New York, 1993
printing).
[0556] A number of exemplary methods for the preparation of the
compositions of the invention are provided below. These methods are
intended to illustrate the nature of such preparations are not
intended to limit the scope of applicable methods.
[0557] Generally, the reaction conditions such as temperature,
reaction time, solvents, work-up procedures, and the like, will be
those common in the art for the particular reaction to be
performed. The cited reference material, together with material
cited therein, contains detailed descriptions of such conditions.
Typically the temperatures will be -100.degree. C. to 200.degree.
C., solvents will be aprotic or protic, and reaction times will be
10 seconds to 10 days. Work-up typically consists of quenching any
unreacted reagents followed by partition between a water/organic
layer system (extraction) and separating the layer containing the
product.
[0558] Oxidation and reduction reactions are typically carried out
at temperatures near room temperature (about 20.degree. C.),
although for metal hydride reductions frequently the temperature is
reduced to 0.degree. C. to -100.degree. C., solvents are typically
aprotic for reductions and may be either protic or aprotic for
oxidations. Reaction times are adjusted to achieve desired
conversions.
[0559] Condensation reactions are typically carried out at
temperatures near room temperature, although for non-equilibrating,
kinetically controlled condensations reduced temperatures
(0.degree. C. to -100.degree. C.) are also common. Solvents can be
either protic (common in equilibrating reactions) or aprotic
(common in kinetically controlled reactions).
[0560] Standard synthetic techniques such as azeotropic removal of
reaction by-products and use of anhydrous reaction conditions
(e.g., inert gas environments) are common in the art and will be
applied when applicable.
SCHEMES AND EXAMPLES
[0561] General aspects of these exemplary methods are described
below and in the Examples. Each of the products of the following
processes is optionally separated, isolated, and/or purified prior
to its use in subsequent processes.
[0562] Generally, the reaction conditions such as temperature,
reaction time, solvents, work-up procedures, and the like, will be
those common in the art for the particular reaction to be
performed. The cited reference material, together with material
cited therein, contains detailed descriptions of such conditions.
Typically the temperatures will be -100.degree. C. to 200.degree.
C., solvents will be aprotic or protic, and reaction times will be
10 seconds to 10 days. Work-up typically consists of quenching any
unreacted reagents followed by partition between a water/organic
layer system (extraction) and separating the layer containing the
product.
[0563] Oxidation and reduction reactions are typically carried out
at temperatures near room temperature (about 20.degree. C.),
although for metal hydride reductions frequently the temperature is
reduced to 0.degree. C. to -100.degree. C., solvents are typically
aprotic for reductions and may be either protic or aprotic for
oxidations. Reaction times are adjusted to achieve desired
conversions.
[0564] Condensation reactions are typically carried out at
temperatures near room temperature, although for non-equilibrating,
kinetically controlled condensations reduced temperatures
(0.degree. C. to -100.degree. C.) are also common. Solvents can be
either protic (common in equilibrating reactions) or aprotic
(common in kinetically controlled reactions).
[0565] Standard synthetic techniques such as azeotropic removal of
reaction by-products and use of anhydrous reaction conditions
(e.g., inert gas environments) are common in the art and will be
applied when applicable.
[0566] The terms "treated", "treating", "treatment", and the like,
when used in connection with a chemical synthetic operation, mean
contacting, mixing, reacting, allowing to react, bringing into
contact, and other terms common in the art for indicating that one
or more chemical entities is treated in such a manner as to convert
it to one or more other chemical entities. This means that
"treating compound one with compound two" is synonymous with
"allowing compound one to react with compound two", "contacting
compound one with compound two", "reacting compound one with
compound two", and other expressions common in the art of organic
synthesis for reasonably indicating that compound one was
"treated", "reacted", "allowed to react", etc., with compound two.
For example, treating indicates the reasonable and usual manner in
which organic chemicals are allowed to react. Normal concentrations
(0.01M to 10M, typically 0.1M to 1M), temperatures (-100.degree. C.
to 250.degree. C., typically -78.degree. C. to 150.degree. C., more
typically -78.degree. C. to 100.degree. C., still more typically
0.degree. C. to 100.degree. C.), reaction vessels (typically glass,
plastic, metal), solvents, pressures, atmospheres (typically air
for oxygen and water insensitive reactions or nitrogen or argon for
oxygen or water sensitive), etc., are intended unless otherwise
indicated. The knowledge of similar reactions known in the art of
organic synthesis are used in selecting the conditions and
apparatus for "treating" in a given process. In particular, one of
ordinary skill in the art of organic synthesis selects conditions
and apparatus reasonably expected to successfully carry out the
chemical reactions of the described processes based on the
knowledge in the art.
[0567] Modifications of each of the exemplary schemes and in the
examples (hereafter "exemplary schemes") leads to various analogs
of the specific exemplary materials produce. The above-cited
citations describing suitable methods of organic synthesis are
applicable to such modifications.
[0568] In each of the exemplary schemes it may be advantageous to
separate reaction products from one another and/or from starting
materials. The desired products of each step or series of steps is
separated and/or purified (hereinafter separated) to the desired
degree of homogeneity by the techniques common in the art.
Typically such separations involve multiphase extraction,
crystallization from a solvent or solvent mixture, distillation,
sublimation, or chromatography. Chromatography can involve any
number of methods including, for example: reverse-phase and normal
phase; size exclusion; ion exchange; high, medium, and low pressure
liquid chromatography methods and apparatus; small scale
analytical; simulated moving bed (SMB) and preparative thin or
thick layer chromatography, as well as techniques of small scale
thin layer and flash chromatography.
[0569] Another class of separation methods involves treatment of a
mixture with a reagent selected to bind to or render otherwise
separable a desired product, unreacted starting material, reaction
by product, or the like. Such reagents include adsorbents or
absorbents such as activated carbon, molecular sieves, ion exchange
media, or the like. Alternatively, the reagents can be acids in the
case of a basic material, bases in the case of an acidic material,
binding reagents such as antibodies, binding proteins, selective
chelators such as crown ethers, liquid/liquid ion extraction
reagents (LIX), or the like.
[0570] Selection of appropriate methods of separation depends on
the nature of the materials involved. For example, boiling point,
and molecular weight in distillation and sublimation, presence or
absence of polar functional groups in chromatography, stability of
materials in acidic and basic media in multiphase extraction, and
the like. One skilled in the art will apply techniques most likely
to achieve the desired separation.
[0571] A single stereoisomer, e.g., an enantiomer, substantially
free of its stereoisomer may be obtained by resolution of the
racemic mixture using a method such as formation of diastereomers
using optically active resolving agents (Stereochemistry of Carbon
Compounds, (1962) by E. L. Eliel, McGraw Hill; Lochmuller, C. H.,
(1975) J. Chromatogr., 113:(3) 283-302). Racemic mixtures of chiral
compounds of the invention can be separated and isolated by any
suitable method, including: (1) formation of ionic, diastereomeric
salts with chiral compounds and separation by fractional
crystallization or other methods, (2) formation of diastereomeric
compounds with chiral derivatizing reagents, separation of the
diastereomers, and conversion to the pure stereoisomers, and (3)
separation of the substantially pure or enriched stereoisomers
directly under chiral conditions.
[0572] Under method (1), diastereomeric salts can be formed by
reaction of enantiomerically pure chiral bases such as brucine,
quinine, ephedrine, strychnine,
.alpha.-methyl-.beta.-phenylethylamine (amphetamine), and the like
with asymmetric compounds bearing acidic functionality, such as
carboxylic acid and sulfonic acid. The diastereomeric salts may be
induced to separate by fractional crystallization or ionic
chromatography. For separation of the optical isomers of amino
compounds, addition of chiral carboxylic or sulfonic acids, such as
camphorsulfonic acid, tartaric acid, mandelic acid, or lactic acid
can result in formation of the diastereomeric salts.
[0573] Alternatively, by method (2), the substrate to be resolved
is reacted with one enantiomer of a chiral compound to form a
diastereomeric pair (Eliel, E. and Wilen, S. (1994) Stereochemistry
of Organic Compounds, John Wiley & Sons, Inc., p. 322).
Diastereomeric compounds can be formed by reacting asymmetric
compounds with enantiomerically pure chiral derivatizing reagents,
such as menthyl derivatives, followed by separation of the
diastereomers and hydrolysis to yield the free, enantiomerically
enriched xanthene. A method of determining optical purity involves
making chiral esters, such as a menthyl ester, e.g., (-) menthyl
chloroformate in the presence of base, or Mosher ester,
.alpha.-methoxy-.alpha.-(trifluoromethyl)phenyl acetate (Jacob III.
(1982) J. Org. Chem. 47:4165), of the racemic mixture, and
analyzing the NMR spectrum for the presence of the two
atropisomeric diastereomers. Stable diastereomers of atropisomeric
compounds can be separated and isolated by normal- and
reverse-phase chromatography following methods for separation of
atropisomeric naphthyl-isoquinolines (Hoye, T., WO 96/15111). By
method (3), a racemic mixture of two enantiomers can be separated
by chromatography using a chiral stationary phase (Chiral Liquid
Chromatography (1989) W. J. Lough, Ed. Chapman and Hall, New York;
Okamoto, (1990) J. of Chromatogr. 513:375-378). Enriched or
purified enantiomers can be distinguished by methods used to
distinguish other chiral molecules with asymmetric carbon atoms,
such as optical rotation and circular dichroism.
Examples General Section
[0574] A number of exemplary methods for the preparation of
compounds of the invention are provided herein, for example, in the
Examples hereinbelow. These methods are intended to illustrate the
nature of such preparations are not intended to limit the scope of
applicable methods. Certain compounds of the invention can be used
as intermediates for the preparation of other compounds of the
invention. For example, the interconversion of various phosphonate
compounds of the invention is illustrated below.
Interconversions of the Phosphonates R-LINK-P(O)(OR.sup.1).sub.2,
R-LINK-P(O)(OR.sup.1)(OH) AND R-LINK-P(O)(OH).sub.2.
[0575] The following schemes 32-38 described the preparation of
phosphonate esters of the general structure
R-link-P(O)(OR.sup.1).sub.2, in which the groups R.sup.1 may be the
same or different. The R.sup.1 groups attached to a phosphonate
ester, or to precursors thereto, may be changed using established
chemical transformations. The interconversion reactions of
phosphonates are illustrated in Scheme S32. The group R in Scheme
32 represents the substructure, i.e. the drug "scaffold, to which
the substituent link-P(O)(OR.sup.1).sub.2 is attached, either in
the compounds of the invention, or in precursors thereto. At the
point in the synthetic route of conducting a phosphonate
interconversion, certain functional groups in R may be protected.
The methods employed for a given phosphonate transformation depend
on the nature of the substituent R.sup.1, and of the substrate to
which the phosphonate group is attached. The preparation and
hydrolysis of phosphonate esters is described in Organic Phosphorus
Compounds, G. M. Kosolapoff, L. Maeir, eds, Wiley, 1976, p.
9ff.
[0576] In general, synthesis of phosphonate esters is achieved by
coupling a nucleophile amine or alcohol with the corresponding
activated phosphonate electrophilic precursor. For example,
chlorophosphonate addition on to 5'-hydroxy of nucleoside is a well
known method for preparation of nucleoside phosphate monoesters.
The activated precursor can be prepared by several well known
methods. Chlorophosphonates useful for synthesis of the prodrugs
are prepared from the substituted-1,3-propanediol (Wissner, et al,
(1992) J. Med. Chem. 35:1650). Chlorophosphonates are made by
oxidation of the corresponding chlorophospholanes (Anderson, et al,
(1984) J. Org. Chem. 49:1304) which are obtained by reaction of the
substituted diol with phosphorus trichloride. Alternatively, the
chlorophosphonate agent is made by treating substituted-1,3-diols
with phosphorusoxychloride (Patois, et al, (1990) J. Chem. Soc.
Perkin Trans. I, 1577). Chlorophosphonate species may also be
generated in situ from corresponding cyclic phosphites (Silverburg,
et al., (1996) Tetrahedron lett., 37:771-774), which in turn can be
either made from chlorophospholane or phosphoramidate intermediate.
Phosphoroflouridate intermediate prepared either from pyrophosphate
or phosphoric acid may also act as precursor in preparation of
cyclic prodrugs (Watanabe et al., (1988) Tetrahedron lett.,
29:5763-66).
[0577] Phosphonate prodrugs of the present invention may also be
prepared from the free acid by Mitsunobu reactions (Mitsunobu,
(1981) Synthesis, 1; Campbell, (1992) J. Org. Chem. 57:6331), and
other acid coupling reagents including, but not limited to,
carbodiimides (Alexander, et al, (1994) Collect. Czech. Chem.
Commun. 59:1853; Casara et al, (1992) Bioorg. Med. Chem. Lett.
2:145; Ohashi et al, (1988) Tetrahedron Lett., 29:1189), and
benzotriazolyloxytris-(dimethylamino)phosphonium salts (Campagne et
al (1993) Tetrahedron Lett. 34:6743).
[0578] Aryl halides undergo Ni.sup.+2 catalyzed reaction with
phosphite derivatives to give aryl phosphonate containing compounds
(Balthazar, et al (1980) J. Org. Chem. 45:5425). Phosphonates may
also be prepared from the chlorophosphonate in the presence of a
palladium catalyst using aromatic triflates (Petrakis et al (1987)
J. Am. Chem. Soc. 109:2831; Lu et al (1987) Synthesis 726). In
another method, aryl phosphonate esters are prepared from aryl
phosphates under anionic rearrangement conditions (Melvin (1981)
Tetrahedron Lett. 22:3375; Casteel et al (1991) Synthesis, 691).
N-Alkoxy aryl salts with alkali met al derivatives of cyclic alkyl
phosphonate provide general synthesis for heteroaryl-2-phosphonate
linkers (Redmore (1970) J. Org. Chem. 35:4114). These above
mentioned methods can also be extended to compounds where the
W.sup.5 group is a heterocycle. Cyclic-1,3-propanyl prodrugs of
phosphonates are also synthesized from phosphonic diacids and
substituted propane-1,3-diols using a coupling reagent such as
1,3-dicyclohexylcarbodiimide (DCC) in presence of a base (e.g.,
pyridine). Other carbodiimide based coupling agents like
1,3-disopropylcarbodiimide or water soluble reagent,
1-(3-dimethylaminopropyl)-3-ethylcarbodiimide hydrochloride (EDCI)
can also be utilized for the synthesis of cyclic phosphonate
prodrugs.
[0579] The conversion of a phosphonate diester S32.1 into the
corresponding phosphonate monoester S32.2 (Scheme 32, Reaction 1)
is accomplished by a number of methods. For example, the ester
S32.1 in which R.sup.1 is an aralkyl group such as benzyl, is
converted into the monoester compound S32.2 by reaction with a
tertiary organic base such as diazabicyclooctane (DABCO) or
quinuclidine, as described in J. Org. Chem. (1995) 60:2946. The
reaction is performed in an inert hydrocarbon solvent such as
toluene or xylene, at about 110.degree. C. The conversion of the
diester S32.1 in which R.sup.1 is an aryl group such as phenyl, or
an alkenyl group such as allyl, into the monoester S32.2 is
effected by treatment of the ester S32.1 with a base such as
aqueous sodium hydroxide in acetonitrile or lithium hydroxide in
aqueous tetrahydrofuran. Phosphonate diesters S32.1 in which one of
the groups R.sup.1 is aralkyl, such as benzyl, and the other is
alkyl, is converted into the monoesters S32.2 in which R.sup.1 is
alkyl by hydrogenation, for example using a palladium on carbon
catalyst. Phosphonate diesters in which both of the groups R.sup.1
are alkenyl, such as allyl, is converted into the monoester S32.2
in which R.sup.1 is alkenyl, by treatment with
chlorotris(triphenylphosphine)rhodium (Wilkinson's catalyst) in
aqueous ethanol at reflux, optionally in the presence of
diazabicyclooctane, for example by using the procedure described in
J. Org. Chem. (1973) 38:3224, for the cleavage of allyl
carboxylates.
[0580] The conversion of a phosphonate diester S32.1 or a
phosphonate monoester S32.2 into the corresponding phosphonic acid
S32.3 (Scheme 32, Reactions 2 and 3) can be effected by reaction of
the diester or the monoester with trimethylsilyl bromide, as
described in J. Chem. Soc., Chem. Comm., (1979) 739. The reaction
is conducted in an inert solvent such as, for example,
dichloromethane, optionally in the presence of a silylating agent
such as bis(trimethylsilyl)trifluoroacetamide, at ambient
temperature. A phosphonate monoester S32.2 in which R.sup.1 is
aralkyl such as benzyl, is converted into the corresponding
phosphonic acid S32.3 by hydrogenation over a palladium catalyst,
or by treatment with hydrogen chloride in an ethereal solvent such
as dioxane. A phosphonate monoester S32.2 in which R.sup.1 is
alkenyl such as, for example, allyl, is converted into the
phosphonic acid S32.3 by reaction with Wilkinson's catalyst in an
aqueous organic solvent, for example in 15% aqueous acetonitrile,
or in aqueous ethanol, for example using the procedure described in
Helv. Chim. Acta. (1985) 68:618. Palladium catalyzed hydrogenolysis
of phosphonate esters S32.1 in which R.sup.1 is benzyl is described
in J. Org. Chem. (1959) 24:434. Platinum-catalyzed hydrogenolysis
of phosphonate esters S32.1 in which R.sup.1 is phenyl is described
in J. Am. Chem. Soc. (1956) 78:2336.
[0581] The conversion of a phosphonate monoester S32.2 into a
phosphonate diester S32.1 (Scheme 32, Reaction 4) in which the
newly introduced R.sup.1 group is alkyl, aralkyl, haloalkyl such as
chloroethyl, or aralkyl is effected by a number of reactions in
which the substrate S32.2 is reacted with a hydroxy compound
R.sup.1OH, in the presence of a coupling agent. Typically, the
second phosphonate ester group is different than the first
introduced phosphonate ester group, i.e. R.sup.1 is followed by the
introduction of R.sup.2 where each of R.sup.1 and R.sup.2 is alkyl,
aralkyl, haloalkyl such as chloroethyl, or aralkyl (Scheme 32,
Reaction 4a) whereby S32.2 is converted to S32.1a. Suitable
coupling agents are those employed for the preparation of
carboxylate esters, and include a carbodiimide such as
dicyclohexylcarbodiimide, in which case the reaction is preferably
conducted in a basic organic solvent such as pyridine, or
(benzotriazol-1-yloxy)tripyrrolidinophosphonium hexafluorophosphate
(PYBOP, Sigma), in which case the reaction is performed in a polar
solvent such as dimethylformamide, in the presence of a tertiary
organic base such as diisopropylethylamine, or Aldrithiol-2
(Aldrich) in which case the reaction is conducted in a basic
solvent such as pyridine, in the presence of a triaryl phosphine
such as triphenylphosphine. Alternatively, the conversion of the
phosphonate monoester S32.2 to the diester S32.1 is effected by the
use of the Mitsunobu reaction, as described above. The substrate is
reacted with the hydroxy compound R.sup.1OH, in the presence of
diethyl azodicarboxylate and a triarylphosphine such as triphenyl
phosphine. Alternatively, the phosphonate monoester S32.2 is
transformed into the phosphonate diester S32.1, in which the
introduced R.sup.1 group is alkenyl or aralkyl, by reaction of the
monoester with the halide R.sup.1Br, in which R.sup.1 is as alkenyl
or aralkyl. The alkylation reaction is conducted in a polar organic
solvent such as dimethylformamide or acetonitrile, in the presence
of a base such as cesium carbonate. Alternatively, the phosphonate
monoester is transformed into the phosphonate diester in a two step
procedure. In the first step, the phosphonate monoester S32.2 is
transformed into the chloro analog RP(O)(OR.sup.1)Cl by reaction
with thionyl chloride or oxalyl chloride and the like, as described
in Organic Phosphorus Compounds, G. M. Kosolapoff, L. Maeir, eds,
Wiley, 1976, p. 17, and the thus-obtained product RP(O)(OR.sup.1)Cl
is then reacted with the hydroxy compound R.sup.1OH, in the
presence of a base such as triethylamine, to afford the phosphonate
diester S32.1.
[0582] A phosphonic acid R-link-P(O)(OH).sub.2 is transformed into
a phosphonate monoester RP(O)(OR.sup.1)(OH) (Scheme 32, Reaction 5)
by means of the methods described above of for the preparation of
the phosphonate diester R-link-P(O)(OR.sup.1).sub.2 S32.1, except
that only one molar proportion of the component R.sup.1OH or
R.sup.1Br is employed. Dialkyl phosphonates may be prepared
according to the methods of: Quast et al (1974) Synthesis 490;
Stowell et al (1990) Tetrahedron Lett. 3261; U.S. Pat. No.
5,663,159.
[0583] A phosphonic acid R-link-P(O)(OH).sub.2 S32.3 is transformed
into a phosphonate diester R-link-P(O)(OR.sup.1).sub.2 S32.1
(Scheme 32, Reaction 6) by a coupling reaction with the hydroxy
compound R.sup.1OH, in the presence of a coupling agent such as
Aldrithiol-2 (Aldrich) and triphenylphosphine. The reaction is
conducted in a basic solvent such as pyridine. Alternatively,
phosphonic acids S32.3 are transformed into phosphonic esters S32.1
in which R.sup.1 is aryl, by means of a coupling reaction
employing, for example, dicyclohexylcarbodiimide in pyridine at ca
70.degree. C. Alternatively, phosphonic acids S32.3 are transformed
into phosphonic esters S32.1 in which R.sup.1 is alkenyl, by means
of an alkylation reaction. The phosphonic acid is reacted with the
alkenyl bromide R.sup.1Br in a polar organic solvent such as
acetonitrile solution at reflux temperature, the presence of a base
such as cesium carbonate, to afford the phosphonic ester S32.1.
##STR00140##
Preparation of Phosphonate Carbamates.
[0584] Phosphonate esters may contain a carbamate linkage. The
preparation of carbamates is described in Comprehensive Organic
Functional Group Transformations, A. R. Katritzky, ed., Pergamon,
1995, Vol. 6, p. 416ff, and in Organic Functional Group
Preparations, by S. R. Sandler and W. Karo, Academic Press, 1986,
p. 260ff. The carbamoyl group may be formed by reaction of a
hydroxy group according to the methods known in the art, including
the teachings of Ellis, US 2002/0103378 A1 and Hajima, U.S. Pat.
No. 6,018,049.
[0585] Scheme 33 illustrates various methods by which the carbamate
linkage is synthesized. As shown in Scheme 33, in the general
reaction generating carbamates, an alcohol S33.1, is converted into
the activated derivative S33.2 in which Lv is a leaving group such
as halo, imidazolyl, benztriazolyl and the like, as described
herein. The activated derivative S33.2 is then reacted with an
amine S33.3, to afford the carbamate product S33.4. Examples 1-7 in
Scheme 33 depict methods by which the general reaction is effected.
Examples 8-10 illustrate alternative methods for the preparation of
carbamates.
[0586] Scheme 33, Example 1 illustrates the preparation of
carbamates employing a chloroformyl derivative of the alcohol
S33.5. In this procedure, the alcohol S33.5 is reacted with
phosgene, in an inert solvent such as toluene, at about 0.degree.
C., as described in Org. Syn. Coll. Vol. 3, 167, 1965, or with an
equivalent reagent such as trichloromethoxy chloroformate, as
described in Org. Syn. Coll. Vol. 6, 715, 1988, to afford the
chloroformate S33.6. The latter compound is then reacted with the
amine component S33.3, in the presence of an organic or inorganic
base, to afford the carbamate S33.7. For example, the chloroformyl
compound S33.6 is reacted with the amine S33.3 in a water-miscible
solvent such as tetrahydrofuran, in the presence of aqueous sodium
hydroxide, as described in Org. Syn. Coll. Vol. 3, 167, 1965, to
yield the carbamate S33.7. Alternatively, the reaction is performed
in dichloromethane in the presence of an organic base such as
diisopropylethylamine or dimethylaminopyridine.
[0587] Scheme 33, Example 2 depicts the reaction of the
chloroformate compound S33.6 with imidazole to produce the
imidazolide S33.8. The imidazolide product is then reacted with the
amine S33.3 to yield the carbamate S33.7. The preparation of the
imidazolide is performed in an aprotic solvent such as
dichloromethane at 0.degree., and the preparation of the carbamate
is conducted in a similar solvent at ambient temperature,
optionally in the presence of a base such as dimethylaminopyridine,
as described in J. Med. Chem., 1989, 32, 357.
[0588] Scheme 33 Example 3, depicts the reaction of the
chloroformate S33.6 with an activated hydroxyl compound R''OH, to
yield the mixed carbonate ester S33.10. The reaction is conducted
in an inert organic solvent such as ether or dichloromethane, in
the presence of a base such as dicyclohexylamine or triethylamine.
The hydroxyl component R''OH is selected from the group of
compounds S33.19-S33.24 shown in Scheme 33, and similar compounds.
For example, if the component R''OH is hydroxybenztriazole S33.19,
N-hydroxysuccinimide S33.20, or pentachlorophenol, S33.21, the
mixed carbonate S33.10 is obtained by the reaction of the
chloroformate with the hydroxyl compound in an ethereal solvent in
the presence of dicyclohexylamine, as described in Can. J. Chem.,
1982, 60, 976. A similar reaction in which the component R''OH is
pentafluorophenol S33.22 or 2-hydroxypyridine S33.23 is performed
in an ethereal solvent in the presence of triethylamine, as
described in Syn., 1986, 303, and Chem. Ber. 118, 468, 1985.
[0589] Scheme 33 Example 4 illustrates the preparation of
carbamates in which an alkyloxycarbonylimidazole S33.8 is employed.
In this procedure, an alcohol S33.5 is reacted with an equimolar
amount of carbonyl diimidazole S33.11 to prepare the intermediate
S33.8. The reaction is conducted in an aprotic organic solvent such
as dichloromethane or tetrahydrofuran. The acyloxyimidazole S33.8
is then reacted with an equimolar amount of the amine R'NH.sub.2 to
afford the carbamate S33.7. The reaction is performed in an aprotic
organic solvent such as dichloromethane, as described in Tet.
Lett., 42, 2001, 5227, to afford the carbamate S33.7.
[0590] Scheme 33, Example 5 illustrates the preparation of
carbamates by means of an intermediate alkoxycarbonylbenztriazole
S33.13. In this procedure, an alcohol ROH is reacted at ambient
temperature with an equimolar amount of benztriazole carbonyl
chloride S33.12, to afford the alkoxycarbonyl product S33.13. The
reaction is performed in an organic solvent such as benzene or
toluene, in the presence of a tertiary organic amine such as
triethylamine, as described in Synthesis., 1977, 704. The product
is then reacted with the amine R'NH.sub.2 to afford the carbamate
S33.7. The reaction is conducted in toluene or ethanol, at from
ambient temperature to about 80.degree. C. as described in
Synthesis., 1977, 704.
[0591] Scheme 33, Example 6 illustrates the preparation of
carbamates in which a carbonate (R'O).sub.2CO, S33.14, is reacted
with an alcohol S33.5 to afford the intermediate alkyloxycarbonyl
intermediate S33.15. The latter reagent is then reacted with the
amine R'NH.sub.2 to afford the carbamate S33.7. The procedure in
which the reagent S33.15 is derived from hydroxybenztriazole S33.19
is described in Synthesis, 1993, 908; the procedure in which the
reagent S33.15 is derived from N-hydroxysuccinimide S33.20 is
described in Tet. Lett., 1992, 2781; the procedure in which the
reagent S33.15 is derived from 2-hydroxypyridine S33.23 is
described in Tet. Lett., 1991, 4251; the procedure in which the
reagent S33.15 is derived from 4-nitrophenol S33.24 is described in
Synthesis. 1993, 103. The reaction between equimolar amounts of the
alcohol ROH and the carbonate S33.14 is conducted in an inert
organic solvent at ambient temperature.
[0592] Scheme 33, Example 7 illustrates the preparation of
carbamates from alkoxycarbonyl azides S33.16. In this procedure, an
alkyl chloroformate S33.6 is reacted with an azide, for example
sodium azide, to afford the alkoxycarbonyl azide S33.16. The latter
compound is then reacted with an equimolar amount of the amine
R'NH.sub.2 to afford the carbamate S33.7. The reaction is conducted
at ambient temperature in a polar aprotic solvent such as
dimethylsulfoxide, for example as described in Synthesis., 1982,
404.
[0593] Scheme 33, Example 8 illustrates the preparation of
carbamates by means of the reaction between an alcohol ROH and the
chloroformyl derivative of an amine S33.17. In this procedure,
which is described in Synthetic Organic Chemistry, R. B. Wagner, H.
D. Zook, Wiley, 1953, p. 647, the reactants are combined at ambient
temperature in an aprotic solvent such as acetonitrile, in the
presence of a base such as triethylamine, to afford the carbamate
S33.7.
[0594] Scheme 33, Example 9 illustrates the preparation of
carbamates by means of the reaction between an alcohol ROH and an
isocyanate S33.18. In this procedure, which is described in
Synthetic Organic Chemistry, R. B. Wagner, H. D. Zook, Wiley, 1953,
p. 645, the reactants are combined at ambient temperature in an
aprotic solvent such as ether or dichloromethane and the like, to
afford the carbamate S33.7.
[0595] Scheme 33, Example 10 illustrates the preparation of
carbamates by means of the reaction between an alcohol ROH and an
amine R'NH.sub.2. In this procedure, which is described in Chem.
Lett. 1972, 373, the reactants are combined at ambient temperature
in an aprotic organic solvent such as tetrahydrofuran, in the
presence of a tertiary base such as triethylamine, and selenium.
Carbon monoxide is passed through the solution and the reaction
proceeds to afford the carbamate S33.7.
##STR00141## ##STR00142## ##STR00143##
Preparation of Carboalkoxy-Substituted Phosphonate Bisamidates,
Monoamidates, Diesters and Monoesters.
[0596] A number of methods are available for the conversion of
phosphonic acids into amidates and esters. In one group of methods,
the phosphonic acid is either converted into an isolated activated
intermediate such as a phosphoryl chloride, or the phosphonic acid
is activated in situ for reaction with an amine or a hydroxy
compound.
[0597] The conversion of phosphonic acids into phosphoryl chlorides
is accomplished by reaction with thionyl chloride, for example as
described in J. Gen. Chem. USSR, 1983, 53, 480, Zh. Obschei Khim.,
1958, 28, 1063, or J. Org. Chem., 1994, 59, 6144, or by reaction
with oxalyl chloride, as described in J. Am. Chem. Soc., 1994, 116,
3251, or J. Org. Chem., 1994, 59, 6144, or by reaction with
phosphorus pentachloride, as described in J. Org. Chem., 2001, 66,
329, or in J. Med. Chem., 1995, 38, 1372. The resultant phosphoryl
chlorides are then reacted with amines or hydroxy compounds in the
presence of a base to afford the amidate or ester products.
[0598] Phosphonic acids are converted into activated imidazolyl
derivatives by reaction with carbonyl diimidazole, as described in
J. Chem. Soc., Chem. Comm. (1991) 312, or Nucleosides &
Nucleotides (2000) 19:1885. Activated sulfonyloxy derivatives are
obtained by the reaction of phosphonic acids with
trichloromethylsulfonyl chloride or with
triisopropylbenzenesulfonyl chloride, as described in Tet. Lett.
(1996) 7857, or Bioorg. Med. Chem. Lett. (1998) 8:663. The
activated sulfonyloxy derivatives are then reacted with amines or
hydroxy compounds to afford amidates or esters.
[0599] Alternatively, the phosphonic acid and the amine or hydroxy
reactant are combined in the presence of a diimide coupling agent.
The preparation of phosphonic amidates and esters by means of
coupling reactions in the presence of dicyclohexyl carbodiimide is
described, for example, in J. Chem. Soc., Chem. Comm. (1991) 312 or
Coll. Czech. Chem. Comm. (1987) 52:2792. The use of ethyl
dimethylaminopropyl carbodiimide for activation and coupling of
phosphonic acids is described in Tet. Lett., (2001) 42:8841, or
Nucleosides & Nucleotides (2000) 19:1885.
[0600] A number of additional coupling reagents have been described
for the preparation of amidates and esters from phosphonic acids.
The agents include Aldrithiol-2, and PYBOP and BOP, as described in
J. Org. Chem., 1995, 60, 5214, and J. Med. Chem. (1997) 40:3842,
mesitylene-2-sulfonyl-3-nitro-1,2,4-triazole (MSNT), as described
in J. Med. Chem. (1996) 39:4958, diphenylphosphoryl azide, as
described in J. Org. Chem. (1984) 49:1158,
1-(2,4,6-triisopropylbenzenesulfonyl-3-nitro-1,2,4-triazole (TPSNT)
as described in Bioorg. Med. Chem. Lett. (1998) 8:1013,
bromotris(dimethylamino)phosphonium hexafluorophosphate (BroP), as
described in Tet. Lett., (1996) 37:3997,
2-chloro-5,5-dimethyl-2-oxo-1,3,2-dioxaphosphinane, as described in
Nucleosides Nucleotides 1995, 14, 871, and diphenyl
chlorophosphate, as described in J. Med. Chem., 1988, 31, 1305.
[0601] Phosphonic acids are converted into amidates and esters by
means of the Mitsunobu reaction, in which the phosphonic acid and
the amine or hydroxy reactant are combined in the presence of a
triaryl phosphine and a dialkyl azodicarboxylate. The procedure is
described in Org. Lett., 2001, 3, 643, or J. Med. Chem., 1997, 40,
3842.
[0602] Phosphonic esters are also obtained by the reaction between
phosphonic acids and halo compounds, in the presence of a suitable
base. The method is described, for example, in Anal. Chem., 1987,
59, 1056, or J. Chem. Soc. Perkin Trans., I, 1993, 19, 2303, or J.
Med. Chem., 1995, 38, 1372, or Tet. Lett., 2002, 43, 1161.
[0603] Schemes 34-37 illustrate the conversion of phosphonate
esters and phosphonic acids into carboalkoxy-substituted
phosphonbisamidates (Scheme 34), phosphonamidates (Scheme 35),
phosphonate monoesters (Scheme 36) and phosphonate diesters,
(Scheme 37). Scheme 38 illustrates synthesis of gem-dialkyl amino
phosphonate reagents.
[0604] Scheme 34 illustrates various methods for the conversion of
phosphonate diesters S34.1 into phosphonbisamidates S34.5. The
diester S34.1, prepared as described previously, is hydrolyzed,
either to the monoester S34.2 or to the phosphonic acid S34.6. The
methods employed for these transformations are described above. The
monoester S34.2 is converted into the monoamidate S34.3 by reaction
with an aminoester S34.9, in which the group R.sup.2 is H or alkyl;
the group R.sup.4b is a divalent alkylene moiety such as, for
example, CHCH.sub.3, CHCH.sub.2CH.sub.3, CH(CH(CH.sub.3).sub.2),
CH(CH.sub.2Ph), and the like, or a side chain group present in
natural or modified aminoacids; and the group R.sup.5b is
C.sub.1-C.sub.12 alkyl, such as methyl, ethyl, propyl, isopropyl,
or isobutyl; C.sub.6-C.sub.20 aryl, such as phenyl or substituted
phenyl; or C.sub.6-C.sub.20 arylalkyl, such as benzyl or
benzyhydryl. The reactants are combined in the presence of a
coupling agent such as a carbodiimide, for example dicyclohexyl
carbodiimide, as described in J. Am. Chem. Soc., (1957) 79:3575,
optionally in the presence of an activating agent such as
hydroxybenztriazole, to yield the amidate product S34.3. The
amidate-forming reaction is also effected in the presence of
coupling agents such as BOP, as described in J. Org. Chem. (1995)
60:5214, Aldrithiol, PYBOP and similar coupling agents used for the
preparation of amides and esters. Alternatively, the reactants
S34.2 and S34.9 are transformed into the monoamidate S34.3 by means
of a Mitsunobu reaction. The preparation of amidates by means of
the Mitsunobu reaction is described in J. Med. Chem. (1995)
38:2742. Equimolar amounts of the reactants are combined in an
inert solvent such as tetrahydrofuran in the presence of a triaryl
phosphine and a dialkyl azodicarboxylate. The thus-obtained
monoamidate ester S34.3 is then transformed into amidate phosphonic
acid S34.4. The conditions used for the hydrolysis reaction depend
on the nature of the R.sup.1 group, as described previously. The
phosphonic acid amidate S34.4 is then reacted with an aminoester
S34.9, as described above, to yield the bisamidate product S34.5,
in which the amino substituents are the same or different.
Alternatively, the phosphonic acid S34.6 may be treated with two
different amino ester reagents simulataneously, i.e. S34.9 where
R.sup.2, R.sup.4b or R.sup.5b are different. The resulting mixture
of bisamidate products S34.5 may then be separable, e.g. by
chromatography.
##STR00144##
[0605] An example of this procedure is shown in Scheme 34, Example
1. In this procedure, a dibenzyl phosphonate S34.14 is reacted with
diazabicyclooctane (DABCO) in toluene at reflux, as described in J.
Org. Chem., 1995, 60, 2946, to afford the monobenzyl phosphonate
S34.15. The product is then reacted with equimolar amounts of ethyl
alaninate S34.16 and dicyclohexyl carbodiimide in pyridine, to
yield the amidate product S34.17. The benzyl group is then removed,
for example by hydrogenolysis over a palladium catalyst, to give
the monoacid product S34.18 which may be unstable according to J.
Med. Chem. (1997) 40(23):3842. This compound S34.18 is then reacted
in a Mitsunobu reaction with ethyl leucinate S34.19, triphenyl
phosphine and diethylazodicarboxylate, as described in J. Med.
Chem., 1995, 38, 2742, to produce the bisamidate product
S34.20.
[0606] Using the above procedures, but employing in place of ethyl
leucinate S34.19 or ethyl alaninate S34.16, different aminoesters
S34.9, the corresponding products S34.5 are obtained.
[0607] Alternatively, the phosphonic acid S34.6 is converted into
the bisamidate S34.5 by use of the coupling reactions described
above. The reaction is performed in one step, in which case the
nitrogen-related substituents present in the product S34.5 are the
same, or in two steps, in which case the nitrogen-related
substituents can be different.
[0608] An example of the method is shown in Scheme 34, Example 2.
In this procedure, a phosphonic acid S34.6 is reacted in pyridine
solution with excess ethyl phenylalaninate S34.21 and
dicyclohexylcarbodiimide, for example as described in J. Chem.
Soc., Chem. Comm., 1991, 1063, to give the bisamidate product
S34.22.
[0609] Using the above procedures, but employing, in place of ethyl
phenylalaninate, different aminoesters S34.9, the corresponding
products S34.5 are obtained.
[0610] As a further alternative, the phosphonic acid S34.6 is
converted into the mono or bis-activated derivative S34.7, in which
Lv is a leaving group such as chloro, imidazolyl,
triisopropylbenzenesulfonyloxy etc. The conversion of phosphonic
acids into chlorides S34.7 (Lv=Cl) is effected by reaction with
thionyl chloride or oxalyl chloride and the like, as described in
Organic Phosphorus Compounds, G. M. Kosolapoff, L. Maeir, eds,
Wiley, 1976, p. 17. The conversion of phosphonic acids into
monoimidazolides S34.7 (Lv=imidazolyl) is described in J. Med.
Chem., 2002, 45, 1284 and in J. Chem. Soc. Chem. Comm., 1991, 312.
Alternatively, the phosphonic acid is activated by reaction with
triisopropylbenzenesulfonyl chloride, as described in Nucleosides
and Nucleotides, 2000, 10, 1885. The activated product is then
reacted with the aminoester S34.9, in the presence of a base, to
give the bisamidate S34.5. The reaction is performed in one step,
in which case the nitrogen substituents present in the product
S34.5 are the same, or in two steps, via the intermediate S34.11,
in which case the nitrogen substituents can be different.
[0611] Examples of these methods are shown in Scheme 34, Examples 3
and 5. In the procedure illustrated in Scheme 34, Example 3, a
phosphonic acid S34.6 is reacted with ten molar equivalents of
thionyl chloride, as described in Zh. Obschei Khim., 1958, 28,
1063, to give the dichloro compound S34.23. The product is then
reacted at reflux temperature in a polar aprotic solvent such as
acetonitrile, and in the presence of a base such as triethylamine,
with butyl serinate S34.24 to afford the bisamidate product
S34.25.
[0612] Using the above procedures, but employing, in place of butyl
serinate S34.24, different aminoesters S34.9, the corresponding
products S34.5 are obtained.
[0613] In the procedure illustrated in Scheme 34, Example 5, the
phosphonic acid S34.6 is reacted, as described in J. Chem. Soc.
Chem. Comm., 1991, 312, with carbonyl diimidazole to give the
imidazolide S34.S32. The product is then reacted in acetonitrile
solution at ambient temperature, with one molar equivalent of ethyl
alaninate S34.33 to yield the monodisplacement product S34.S34. The
latter compound is then reacted with carbonyl diimidazole to
produce the activated intermediate S34.35, and the product is then
reacted, under the same conditions, with ethyl N-methylalaninate
S34.33a to give the bisamidate product S34.36.
[0614] Using the above procedures, but employing, in place of ethyl
alaninate S34.33 or ethyl N-methylalaninate S34.33a, different
aminoesters S34.9, the corresponding products S34.5 are
obtained.
[0615] The intermediate monoamidate S34.3 is also prepared from the
monoester S34.2 by first converting the monoester into the
activated derivative S34.8 in which Lv is a leaving group such as
halo, imidazolyl etc, using the procedures described above. The
product S34.8 is then reacted with an aminoester S34.9 in the
presence of a base such as pyridine, to give an intermediate
monoamidate product S34.3. The latter compound is then converted,
by removal of the R.sup.1 group and coupling of the product with
the aminoester S34.9, as described above, into the bisamidate
S34.5.
[0616] An example of this procedure, in which the phosphonic acid
is activated by conversion to the chloro derivative S34.26, is
shown in Scheme 34, Example 4. In this procedure, the phosphonic
monobenzyl ester S34.15 is reacted, in dichloromethane, with
thionyl chloride, as described in Tet. Letters., 1994, 35, 4097, to
afford the phosphoryl chloride S34.26. The product is then reacted
in acetonitrile solution at ambient temperature with one molar
equivalent of ethyl 3-amino-2-methylpropionate S34.27 to yield the
monoamidate product S34.28. The latter compound is hydrogenated in
ethylacetate over a 5% palladium on carbon catalyst to produce the
monoacid product S34.29. The product is subjected to a Mitsunobu
coupling procedure, with equimolar amounts of butyl alaninate
S34.30, triphenyl phosphine, diethylazodicarboxylate and
triethylamine in tetrahydrofuran, to give the bisamidate product
S34.31.
[0617] Using the above procedures, but employing, in place of ethyl
3-amino-2-methylpropionate S34.27 or butyl alaninate S34.30,
different aminoesters S34.9, the corresponding products S34.5 are
obtained.
[0618] The activated phosphonic acid derivative S34.7 is also
converted into the bisamidate S34.5 via the diamino compound
S34.10. The conversion of activated phosphonic acid derivatives
such as phosphoryl chlorides into the corresponding amino analogs
S34.10, by reaction with ammonia, is described in Organic
Phosphorus Compounds, G. M. Kosolapoff, L. Maeir, eds, Wiley, 1976.
The bisamino compound S34.10 is then reacted at elevated
temperature with a haloester S34.12 (Hal=halogen, i.e. F, Cl, Br,
I), in a polar organic solvent such as dimethylformamide, in the
presence of a base such as 4,4-dimethylaminopyridine (DMAP) or
potassium carbonate, to yield the bisamidate S34.5. Alternatively,
S34.6 may be treated with two different amino ester reagents
simulataneously, i.e. S34.12 where R.sup.4b or R.sup.5b are
different. The resulting mixture of bisamidate products S34.5 may
then be separable, e.g. by chromatography.
[0619] An example of this procedure is shown in Scheme 34, Example
6. In this method, a dichlorophosphonate S34.23 is reacted with
ammonia to afford the diamide S34.37. The reaction is performed in
aqueous, aqueous alcoholic or alcoholic solution, at reflux
temperature. The resulting diamino compound is then reacted with
two molar equivalents of ethyl 2-bromo-3-methylbutyrate S34.38, in
a polar organic solvent such as N-methylpyrrolidinone at ca.
150.degree. C., in the presence of a base such as potassium
carbonate, and optionally in the presence of a catalytic amount of
potassium iodide, to afford the bisamidate product S34.39.
[0620] Using the above procedures, but employing, in place of ethyl
2-bromo-3-methylbutyrate S34.38, different haloesters S34.12 the
corresponding products S34.5 are obtained.
[0621] The procedures shown in Scheme 34 are also applicable to the
preparation of bisamidates in which the aminoester moiety
incorporates different functional groups. Scheme 34, Example 7
illustrates the preparation of bisamidates derived from tyrosine.
In this procedure, the monoimidazolide S34.32 is reacted with
propyl tyrosinate S34.40, as described in Example 5, to yield the
monoamidate S34.41. The product is reacted with carbonyl
diimidazole to give the imidazolide S34.42, and this material is
reacted with a further molar equivalent of propyl tyrosinate to
produce the bisamidate product S34.43.
[0622] Using the above procedures, but employing, in place of
propyl tyrosinate S34.40, different aminoesters S34.9, the
corresponding products S34.5 are obtained. The aminoesters employed
in the two stages of the above procedure can be the same or
different, so that bisamidates with the same or different amino
substituents are prepared.
[0623] Scheme 35 illustrates methods for the preparation of
phosphonate monoamidates.
[0624] In one procedure, a phosphonate monoester S34.1 is
converted, as described in Scheme 34, into the activated derivative
S34.8. This compound is then reacted, as described above, with an
aminoester S34.9, in the presence of a base, to afford the
monoamidate product S35.1.
[0625] The procedure is illustrated in Scheme 35, Example 1. In
this method, a monophenyl phosphonate S35.7 is reacted with, for
example, thionyl chloride, as described in J. Gen. Chem. USSR.,
1983, 32, 367, to give the chloro product S35.8. The product is
then reacted, as described in Scheme 34, with ethyl alaninate, S3,
to yield the amidate S35.10.
[0626] Using the above procedures, but employing, in place of ethyl
alaninate S35.9, different aminoesters S34.9, the corresponding
products S35.1 are obtained.
[0627] Alternatively, the phosphonate monoester S34.1 is coupled,
as described in Scheme 34, with an aminoester S34.9 to produce the
amidate, S335.1. If necessary, the R.sup.1 substituent is then
altered, by initial cleavage to afford the phosphonic acid S35.2.
The procedures for this transformation depend on the nature of the
R.sup.1 group, and are described above. The phosphonic acid is then
transformed into the ester amidate product S35.3, by reaction with
the hydroxy compound R.sup.3OH, in which the group R.sup.3 is aryl,
heterocycle, alkyl, cycloalkyl, haloalkyl etc, using the same
coupling procedures (carbodiimide, Aldrithiol-2, PYBOP, Mitsunobu
reaction etc) described in Scheme 34 for the coupling of amines and
phosphonic acids.
##STR00145## ##STR00146## ##STR00147## ##STR00148##
##STR00149##
[0628] Examples of this method are shown in Scheme 35, Examples and
2 and 3. In the sequence shown in Example 2, a monobenzyl
phosphonate S35.11 is transformed by reaction with ethyl alaninate,
using one of the methods described above, into the monoamidate
S35.12. The benzyl group is then removed by catalytic hydrogenation
in ethylacetate solution over a 5% palladium on carbon catalyst, to
afford the phosphonic acid amidate S35.13. The product is then
reacted in dichloromethane solution at ambient temperature with
equimolar amounts of 1-(dimethylaminopropyl)-3-ethylcarbodiimide
and trifluoroethanol S35.14, for example as described in Tet.
Lett., 2001, 42, 8841, to yield the amidate ester S35.15.
[0629] In the sequence shown in Scheme 35, Example 3, the
monoamidate S35.13 is coupled, in tetrahydrofuran solution at
ambient temperature, with equimolar amounts of dicyclohexyl
carbodiimide and 4-hydroxy-N-methylpiperidine S35.16, to produce
the amidate ester product S35.17.
[0630] Using the above procedures, but employing, in place of the
ethyl alaninate product S35.12 different monoacids S35.2, and in
place of trifluoroethanol S35.14 or 4-hydroxy-N-methylpiperidine
S35.16, different hydroxy compounds R.sup.3OH, the corresponding
products S35.3 are obtained.
[0631] Alternatively, the activated phosphonate ester S34.8 is
reacted with ammonia to yield the amidate S35.4. The product is
then reacted, as described in Scheme 34, with a haloester S35.5, in
the presence of a base, to produce the amidate product S35.6. If
appropriate, the nature of the R.sup.1 group is changed, using the
procedures described above, to give the product S35.3. The method
is illustrated in Scheme 35, Example 4. In this sequence, the
monophenyl phosphoryl chloride S35.18 is reacted, as described in
Scheme 34, with ammonia, to yield the amino product S35.19. This
material is then reacted in N-methylpyrrolidinone solution at
170.degree. with butyl 2-bromo-3-phenylpropionate S35.20 and
potassium carbonate, to afford the amidate product S35.21.
[0632] Using these procedures, but employing, in place of butyl
2-bromo-3-phenylpropionate S35.20, different haloesters S35.5, the
corresponding products S35.6 are obtained.
[0633] The monoamidate products S35.3 are also prepared from the
doubly activated phosphonate derivatives S34.7. In this procedure,
examples of which are described in Synlett., 1998, 1, 73, the
intermediate S34.7 is reacted with a limited amount of the
aminoester S34.9 to give the mono-displacement product S34.11. The
latter compound is then reacted with the hydroxy compound R.sup.3OH
in a polar organic solvent such as dimethylformamide, in the
presence of a base such as diisopropylethylamine, to yield the
monoamidate ester S35.3.
[0634] The method is illustrated in Scheme 35, Example 5. In this
method, the phosphoryl dichloride S35.22 is reacted in
dichloromethane solution with one molar equivalent of ethyl
N-methyl tyrosinate S35.23 and dimethylaminopyridine, to generate
the monoamidate S35.24. The product is then reacted with phenol
S35.25 in dimethylformamide containing potassium carbonate, to
yield the ester amidate product S35.26.
[0635] Using these procedures, but employing, in place of ethyl
N-methyl tyrosinate S35.23 or phenol S35.25, the aminoesters 34.9
and/or the hydroxy compounds R.sup.3OH, the corresponding products
S35.3 are obtained.
##STR00150## ##STR00151##
[0636] Scheme 36 illustrates methods for the preparation of
carboalkoxy-substituted phosphonate diesters in which one of the
ester groups incorporates a carboalkoxy substituent.
[0637] In one procedure, a phosphonate monoester S34.1, prepared as
described above, is coupled, using one of the methods described
above, with a hydroxyester S36.1, in which the groups R.sup.4b and
R.sup.5b are as described in Scheme 34. For example, equimolar
amounts of the reactants are coupled in the presence of a
carbodiimide such as dicyclohexyl carbodiimide, as described in
Aust. J. Chem., 1963, 609, optionally in the presence of
dimethylaminopyridine, as described in Tet., 1999, 55, 12997. The
reaction is conducted in an inert solvent at ambient
temperature.
[0638] The procedure is illustrated in Scheme 36, Example 1. In
this method, a monophenyl phosphonate S36.9 is coupled, in
dichloromethane solution in the presence of dicyclohexyl
carbodiimide, with ethyl 3-hydroxy-2-methylpropionate S36.10 to
yield the phosphonate mixed diester S36.11.
[0639] Using this procedure, but employing, in place of ethyl
3-hydroxy-2-methylpropionate S36.10, different hydroxyesters S33.1,
the corresponding products S33.2 are obtained.
[0640] The conversion of a phosphonate monoester S34.1 into a mixed
diester S36.2 is also accomplished by means of a Mitsunobu coupling
reaction with the hydroxyester S36.1, as described in Org. Lett.,
2001, 643. In this method, the reactants 34.1 and S36.1 are
combined in a polar solvent such as tetrahydrofuran, in the
presence of a triarylphosphine and a dialkyl azodicarboxylate, to
give the mixed diester S36.2. The R.sup.1 substituent is varied by
cleavage, using the methods described previously, to afford the
monoacid product S36.3. The product is then coupled, for example
using methods described above, with the hydroxy compound R.sup.3OH,
to give the diester product S36.4.
[0641] The procedure is illustrated in Scheme 36, Example 2. In
this method, a monoallyl phosphonate S36.12 is coupled in
tetrahydrofuran solution, in the presence of triphenylphosphine and
diethylazodicarboxylate, with ethyl lactate S36.13 to give the
mixed diester S36.14. The product is reacted with
tris(triphenylphosphine) rhodium chloride (Wilkinson catalyst) in
acetonitrile, as described previously, to remove the allyl group
and produce the monoacid product S36.15. The latter compound is
then coupled, in pyridine solution at ambient temperature, in the
presence of dicyclohexyl carbodiimide, with one molar equivalent of
3-hydroxypyridine S36.16 to yield the mixed diester S36.17.
[0642] Using the above procedures, but employing, in place of the
ethyl lactate S36.13 or 3-hydroxypyridine, a different hydroxyester
S36.1 and/or a different hydroxy compound R.sup.3OH, the
corresponding products S36.4 are obtained.
[0643] The mixed diesters S36.2 are also obtained from the
monoesters S34.1 via the intermediacy of the activated monoesters
S36.5. In this procedure, the monoester S34.1 is converted into the
activated compound S36.5 by reaction with, for example, phosphorus
pentachloride, as described in J. Org. Chem., 2001, 66, 329, or
with thionyl chloride or oxalyl chloride (Lv=Cl), or with
triisopropylbenzenesulfonyl chloride in pyridine, as described in
Nucleosides and Nucleotides, 2000, 19, 1885, or with carbonyl
diimidazole, as described in J. Med. Chem., 2002, 45, 1284. The
resultant activated monoester is then reacted with the hydroxyester
S36.1, as described above, to yield the mixed diester S36.2.
[0644] The procedure is illustrated in Scheme 36, Example 3. In
this sequence, a monophenyl phosphonate S36.9 is reacted, in
acetonitrile solution at 70.degree. C., with ten equivalents of
thionyl chloride, so as to produce the phosphoryl chloride S36.19.
The product is then reacted with ethyl
4-carbamoyl-2-hydroxybutyrate S36.20 in dichloromethane containing
triethylamine, to give the mixed diester S36.21.
[0645] Using the above procedures, but employing, in place of ethyl
4-carbamoyl-2-hydroxybutyrate S36.20, different hydroxyesters
S36.1, the corresponding products S36.2 are obtained.
[0646] The mixed phosphonate diesters are also obtained by an
alternative route for incorporation of the R.sup.30 group into
intermediates S36.3 in which the hydroxyester moiety is already
incorporated. In this procedure, the monoacid intermediate S36.3 is
converted into the activated derivative S36.6 in which Lv is a
leaving group such as chloro, imidazole, and the like, as
previously described. The activated intermediate is then reacted
with the hydroxy compound R.sup.3OH, in the presence of a base, to
yield the mixed diester product S36.4.
[0647] The method is illustrated in Scheme 36, Example 4. In this
sequence, the phosphonate monoacid S36.22 is reacted with
trichloromethanesulfonyl chloride in tetrahydrofuran containing
collidine, as described in J. Med. Chem., 1995, 38, 4648, to
produce the trichloromethanesulfonyloxy product S36.23. This
compound is reacted with 3-(morpholinomethyl)phenol S36.24 in
dichloromethane containing triethylamine, to yield the mixed
diester product S36.25.
[0648] Using the above procedures, but employing, in place of with
3-(morpholinomethyl)phenol S36.24, different alcohols R.sup.3OH,
the corresponding products S36.4 are obtained.
[0649] The phosphonate esters S36.4 are also obtained by means of
alkylation reactions performed on the monoesters S34.1. The
reaction between the monoacid S34.1 and the haloester S36.7 is
performed in a polar solvent in the presence of a base such as
diisopropylethylamine, as described in Anal. Chem., 1987, 59, 1056,
or triethylamine, as described in J. Med. Chem., 1995, 38, 1372, or
in a non-polar solvent such as benzene, in the presence of
18-crown-6, as described in Syn. Comm., 1995, 25, 3565.
[0650] The method is illustrated in Scheme 36, Example 5. In this
procedure, the monoacid S36.26 is reacted with ethyl
2-bromo-3-phenylpropionate S36.27 and diisopropylethylamine in
dimethylformamide at 80.degree. C. to afford the mixed diester
product S36.28.
[0651] Using the above procedure, but employing, in place of ethyl
2-bromo-3-phenylpropionate S36.27, different haloesters S36.7, the
corresponding products S36.4 are obtained.
##STR00152## ##STR00153##
[0652] Scheme 37 illustrates methods for the preparation of
phosphonate diesters in which both the ester substituents
incorporate carboalkoxy groups.
[0653] The compounds are prepared directly or indirectly from the
phosphonic acids S34.6. In one alternative, the phosphonic acid is
coupled with the hydroxyester S37.2, using the conditions described
previously in Schemes 34-36, such as coupling reactions using
dicyclohexyl carbodiimide or similar reagents, or under the
conditions of the Mitsunobu reaction, to afford the diester product
S37.3 in which the ester substituents are identical.
[0654] This method is illustrated in Scheme 37, Example 1. In this
procedure, the phosphonic acid S34.6 is reacted with three molar
equivalents of butyl lactate S37.5 in the presence of Aldrithiol-2
and triphenyl phosphine in pyridine at ca. 70.degree. C., to afford
the diester S37.6.
[0655] Using the above procedure, but employing, in place of butyl
lactate S37.5, different hydroxyesters S37.2, the corresponding
products S37.3 are obtained.
[0656] Alternatively, the diesters S37.3 are obtained by alkylation
of the phosphonic acid S34.6 with a haloester S37.1. The alkylation
reaction is performed as described in Scheme 36 for the preparation
of the esters S36.4.
[0657] This method is illustrated in Scheme 37, Example 2. In this
procedure, the phosphonic acid S34.6 is reacted with excess ethyl
3-bromo-2-methylpropionate S37.7 and diisopropylethylamine in
dimethylformamide at ca. 80.degree. C., as described in Anal.
Chem., 1987, 59, 1056, to produce the diester S37.8.
[0658] Using the above procedure, but employing, in place of ethyl
3-bromo-2-methylpropionate S37.7, different haloesters S37.1, the
corresponding products S37.3 are obtained.
[0659] The diesters S37.3 are also obtained by displacement
reactions of activated derivatives S34.7 of the phosphonic acid
with the hydroxyesters S37.2. The displacement reaction is
performed in a polar solvent in the presence of a suitable base, as
described in Scheme 36. The displacement reaction is performed in
the presence of an excess of the hydroxyester, to afford the
diester product S37.3 in which the ester substituents are
identical, or sequentially with limited amounts of different
hydroxyesters, to prepare diesters S37.3 in which the ester
substituents are different.
[0660] The methods are illustrated in Scheme 37, Examples 3 and 4.
As shown in Example 3, the phosphoryl dichloride S35.22 is reacted
with three molar equivalents of ethyl
3-hydroxy-2-(hydroxymethyl)propionate S37.9 in tetrahydrofuran
containing potassium carbonate, to obtain the diester product
S37.10.
[0661] Using the above procedure, but employing, in place of ethyl
3-hydroxy-2-(hydroxymethyl)propionate S37.9, different
hydroxyesters S37.2, the corresponding products S37.3 are
obtained.
[0662] Scheme 37, Example 4 depicts the displacement reaction
between equimolar amounts of the phosphoryl dichloride S35.22 and
ethyl 2-methyl-3-hydroxypropionate S37.11, to yield the monoester
product S37.12. The reaction is conducted in acetonitrile at
70.degree. in the presence of diisopropylethylamine. The product
S37.12 is then reacted, under the same conditions, with one molar
equivalent of ethyl lactate S37.13, to give the diester product
S37.14.
[0663] Using the above procedures, but employing, in place of ethyl
2-methyl-3-hydroxypropionate S37.11 and ethyl lactate S37.13,
sequential reactions with different hydroxyesters S37.2, the
corresponding products S37.3 are obtained.
##STR00154## ##STR00155##
[0664] 2,2-Dimethyl-2-aminoethylphosphonic acid intermediates can
be prepared by the route in Scheme 5. Condensation of
2-methyl-2-propanesulfinamide with acetone give sulfinyl imine
S38.11 (J. Org. Chem. 1999, 64, 12). Addition of dimethyl
methylphosphonate lithium to S38.11 afford S38.12. Acidic
methanolysis of S38.12 provide amine S38.13. Protection of amine
with Cbz group and removal of methyl groups yield phosphonic acid
S38.14, which can be converted to desired S38.15 (Scheme 38a) using
methods reported earlier on. An alternative synthesis of compound
S38.14 is also shown in Scheme 38b. Commercially available
2-amino-2-methyl-1-propanol is converted to aziridines S38.16
according to literature methods (J. Org. Chem. 1992, 57, 5813; Syn.
Lett. 1997, 8, 893). Aziridine opening with phosphite give S38.17
(Tetrahedron Lett. 1980, 21, 1623). Reprotection) of S38.17 affords
S38.14.
##STR00156##
[0665] The invention will now be illustrated by the following
non-limiting Examples.
Example 1
##STR00157##
[0667] Rapamycin (compound, 1.1, wherein the remaining portion of
the rapamycin structure is not shown), a synthetic precursor of
everolimus, is O-arylated as shown above using an appropriate aryl
bismuth reagent according to a procedure such as that reported in
Bioorg. Med. Chem. Lett, 1995, 5, 1035.
3-(Dimethyl-t-butylsilyloxy)bromobenzene is treated either with
magnesium in diethyl ether or with butyllithium in tetrahydrofuran,
and the resulting organometallic reagent is reacted with bismuth
trichloride to generate the triarybismuthine. After treating with
1-1.2 equivalents of peracetic acid, the bismuth(V) reagent is
mixed with rapamycin and copper(II) acetate. The reaction is
allowed to proceed for a day at room temperature or, if necessary,
at reflux, affording the desired 3-(dimethyl-t-butylsilyloxy)phenyl
ether, 1.2. After removal of the dimethyl-t-butylsilyl protecting
group, O-alkylation is achieved with diethyl
(bromomethyl)phosphonate in the presence of silver oxide, affording
the desired everolimus analog containing the diethylphosphonate,
1.3. Silver ion-assisted reactions have been used to mediate
O-alkylations on an immunosuppresive macrolide structurally similar
to rapamycin: see J. Med. Chem., 1998, 41, 1764.
Example 2
##STR00158##
[0669] A phosphonate derivative of everolimus indolyl ether is
prepared from rapamycin (formula, 2.1, wherein the remaining
portion of the rapamycin structure is not shown) in a similar
manner to that described in Example 1, with the exception that the
key triindolylbismuthine intermediate is obtained from
5-bromoindole following the procedure described in J. Org. Chem.
1998, 63, 6721.
Example 3
##STR00159##
[0671] Tacrolimus (compound, 3.1, wherein the remaining portion of
the tacrolimus molecule is not shown) is O-arylated as shown above
using an appropriate aryl bismuth reagent according to a procedure
such as that reported in Bioorg. Med. Chem. Lett, 1995, 5, 1035.
3-(Dimethyl-t-butylsilyloxy)-bromobenzene is treated either with
magnesium in diethyl ether or with butyllithium in tetrahydrofuran,
and the resulting organometallic reagent is reacted with bismuth
trichloride to generate the triarybismuthine. After treating with
1-1.2 equivalents of peracetic acid, the bismuth(V) reagent is
mixed with tacrolimus, 3.1, and copper(II) acetate. The reaction is
allowed to proceed for a day at room temperature or, if necessary,
at reflux, affording the desired 3-(dimethyl-t-butylsilyloxy)phenyl
ether. After removal of the dimethyl-t-butylsilyl protecting group
with HF, O-alkylation is achieved with diethyl
(bromomethyl)phosphonate in the presence of silver oxide, affording
the desired tacrolimus analog containing the diethylphosphonate,
3.3. Silver ion-assisted reactions have been used to mediate
O-alkylations on an immunosuppresive macrolide structurally similar
to tacrolimus. (See J. Med. Chem., 1998, 41, 1764.)
Example 4
##STR00160##
[0673] A phosphonate derivative of, 4.3, tacrolimus indolyl ether
is prepared from tacrolimus (compound, 4.1, wherein the remaining
portion of the tacrolimus molecule is not shown) in a similar
manner to that described in Example 3 with the exception that the
key triindolylbismuthine intermediate is obtained from
5-bromoindole following the procedure described in J. Org. Chem.
1998, 63, 6721.
Example 5
[0674] Representative compounds of the invention can be made by
procedures such as those described by Boer, et al, J. Mass
Spectrom. 1995, 30, 497-504 and Hoyte, et al, J. Med. Chem. 2002,
45, 5397-5405; they can also be made according to the following
general routes.
##STR00161##
[0675] Compounds of formulae, 5.1 and 5.2, wherein "Link" have any
of the values defined herein for a linking group or a linker, are
representative compounds of the invention.
Example 6
##STR00162##
[0677] Prednisolone, 6A, is treated in a solvent, such as
chloroform, with formaldehyde in the presence of an acid, such as
concentrated hydrochloric acid. After stirring for several hours
(preferably 7 to 10 hours) at room temperature, the layers are
separated and the organic layer is concentrated to afford the
bis-(methylenedioxy) intermediate, 5.3 (Hirschmann, R. et al, J.
Am. Chem. Soc. 1964, 86, 1520-1527). This intermediate is treated
with diethyl (amino-oxymethyl)phosphonate in a solvent such as
pyridine to afford the oxime, 5.4. The oxime is treated with
aqueous acid to remove the bis-(methylenedioxy) protecting group.
For example, the oxime is treated with 60% aqueous formic acid and
heated at 90.degree. C. for 10 min., cooled and concentrated using
portions of ethanol to assist in removing formic acid.
Chromatographic purification and/or crystallization of the residue
yield the phosphonate oxime analog, 5.5, of prednisolone.
[0678] A key precursor of this synthesis, diethyl
(aminooxymethyl)phosphonate, can be obtained from diethyl
(trifluoromethyl-sulfonyloxymethyl)phosphonate and
N-(t-butoxycarbonyl)-hydroxylamine. Accordingly,
N-(t-butoxycarbonyl)-hydroxylamine is dissolved in a solvent such
as THF and treated with sodium hydride. When bubbling ceases,
diethyl (trifluoromethylsulfonyloxymethyl)-phosphonate (prepared
according to Tetrahedron Lett., 1986, 27, 1477) is added. After
quenching the reaction with aqueous ammonium chloride and
extracting the product with an organic solvent such as ethyl
acetate, the N-Boc protected diethyl (aminooxymethyl)phosphonate is
isolated by chromatography. The N-Boc protecting group is then
removed by treatment of trifluoroacetic acid, affording the desired
diethyl (aminooxymethyl)phosphonate.
Example 7
##STR00163##
[0680] Prednisolone, 6A, is reduced to 1,2-dihydroprednisolone,
7.1, using a rhodium catalysis such as
tris(triphenylphosphine)rhodium(I) chloride under hydrogen
according to a procedure such as that reported by Procopiou, P. et
al, J. Med. Chem., 2001, 44, 602-612. The dihydroxy ketone group on
the D ring of the steroid is then protected using the method
described in Example 6, before formylation at the C-2 position. For
example, the bis-(methylenedioxy) intermediate, 7.2, is treated
with freshly distilled ethyl formate and sodium hydride in a
solvent such as toluene. The reaction is quenched with aqueous
solution of a weak base such as potassium dihydrogen phosphate. The
crude product is purified by a general method such as
crystallization, affording the 2-formyl intermediate, 7.3. This
2-formyl compound is condensed with a phosphonate-substituted
phenylhydrazine to yield, after removal of the bis-(methylenedioxy)
protecting group, the desired phosphonate pyrazole analog, 7.4, of
prednisolone.
[0681] A key precursor,
3-[(diethylphosphono)-methoxy]phenylhydrazine, 7.5, can be made
starting from diethyl
(trifluoromethylsulfonyloxymethyl)-phosphonate and 3-nitrophenol.
3-Nitrophenol is treated with a base such as sodium hydroxide and
then O-alkylated with diethyl
(trifluoromethylsulfonyl-oxymethyl)phosphonate. The nitro group is
reduced with tin(II) chloride and subsequently converted to the
aryl hydrazine by diazotization and reduction with sodium sulfite
(Chem. Ber., 1960, 93, 540) or tin(II) chloride (J. Med. Chem.,
2001, 44, 4031).
Examples 8-13
[0682] Synthetic methodologies and intermediate compounds that can
be used to prepare VX-148 analogs of formulae A, B, or C are
described in Examples 8-13. The below compounds are representative
examples of compounds of Formulae 6, 7, and 8.
##STR00164##
[0683] Link includes 0-8 atoms; 2-6 is preferred.
Example 8
##STR00165##
[0685] A general scheme that is useful for converting a
3,5-difunctionalized nitrobenzene derivative to an aniline that can
be used to prepare a VX-148 analog of the invention is illustrated
above.
Example 9
##STR00166##
[0687] 3-Hydroxy-5-nitro-benzoic acid is heated briefly in thionyl
chloride to generate the acid chloride. The acid chloride is
condensed with O,N-dimethyl-hydroxylamine in the presence of a base
such as triethylamine to produce the Weinreb amide which, upon
reaction with methyl lithium, provides the acetophenone derivative.
The acetophenone derivative is treated with a base such as
potassium carbonate in a dipolar aprotic solvent such as
dimethyl-formamide, in the presence of an excess of
E-1,4-dibromobutene. The monobromide is isolated by chromatography
and then subjected to treatment with triethylphosphite in a solvent
such as toluene (or other Arbuzov reaction conditions: see Engel,
R., "Synthesis of Carbon-phosphorus Bonds," CRC press, 1988) to
generate the desired phosphonate diethyl ester. Thereafter, the
carbonyl of the acetophenone is reduced enantioselectively using an
appropriate homochiral oxazaborolidine such as that described by
Corey (J. Am. Chem. Soc., 1987, 109, 5551), and the resulting
alcohol is displaced by azide using a method such as that described
by Mitsunobu (Bull. Chem. Soc. Japan., 1971, 44, 3427). The azide
is reduced to the amine under Staudinger conditions (Helv. Chim.
Act., 1919, 2, 635) and protected as the t-butyl carbonate.
Finally, the desired aniline intermediate is generated by tin
(II)-mediated reduction of the nitrobenzene. The aniline is
converted to a compound of Formula A (also Formula 6) using
coupling reactions similar to those described in U.S. Pat. No.
6,054,472 and U.S. Pat. No. 6,344,465.
Example 10
##STR00167##
[0689] A general scheme that is useful for converting a
3,4-difunctionalized nitrobenzene derivative, 10.1, to an aniline,
which can be converted to a compound of Formula B (also Formula 7)
using coupling reactions similar to those described in U.S. Pat.
No. 6,054,472 and U.S. Pat. No. 6,344,465, is illustrated
above.
Example 11
##STR00168##
[0691] Manipulation of a 3-substituted nitrobenzene, 11.1, provides
aniline, 11.2, which can be converted to a compound of formula C
(also Formula 8) using coupling reactions similar to those
described in U.S. Pat. No. 6,054,472 and U.S. Pat. No.
6,344,465.
Example 12
##STR00169##
[0693] 3-Nitrobenzaldehyde, 12.1, reacts with a Grignard reagent to
introduce a tether bearing a protected alcohol and simultaneously
to generate a benzylic alcohol, as shown. The alcohol, 12.2, is
displaced by an azide in a manner similar to that described for
Example 9. After deprotection, the liberated alcohol is alkylated
with diethyl phosphonomethyltriflate (prepared according to
Tetrahedron Lett., 1986, 27, 1477) using a base such as magnesium
tert-butoxide in a solvent such as tetrahydrofuran. Subsequent
transformations of the azide and nitro groups proceed in a fashion
similar to that described in Example 9. See Batt et al, Bioorg.
Med. Chem. Lett., 1995, 5, 1549.
Example 13
##STR00170##
[0695] 3-tert-Butoxycarbonylamino-3-(3-nitro-phenyl)-propionic
acid, 13.1, (commercially available) is coupled with
2-aminoethylphosphonic acid diethyl ester (commercially available)
using standard reagents for the formation of a secondary amide such
as dicyclohexylcarbodiimide (DCC) and hydroxy-benztriazole (HOBT),
in a solvent such as dimethylformamide. Subsequent reduction of the
nitro group proceeds in a fashion similar to that described in
Example 9.
Example 14
##STR00171##
[0697] The above scheme illustrates a general route that can be
used to prepare compounds of Formula 9.
Example 15
##STR00172##
[0699] 3-Hydroxy-5-nitro-benzoic acid, 15.1, is heated briefly in
thionyl chloride to generate the acid chloride. This is then
condensed with O,N-dimethyl-hydroxylamine in the presence of a base
such as triethylamine to produce the Weinreb amide which, upon
reaction with methyl lithium, gives the acetophenone derivative.
This is then treated with a base such as potassium carbonate in a
dipolar aprotic solvent such as dimethyl-formamide, in the presence
of an excess of E-1,4-dibromobutene. The monobromide is isolated by
chromatography and then subjected to treatment with
triethylphosphite in a solvent such as toluene (or other Arbuzov
reaction conditions: see Engel, R., "Synthesis of Carbon-phosphorus
Bonds," CRC press, 1988) to generate the desired phosphonate
diethyl ester, 15.2. Thereafter, the carbonyl of the acetophenone
is reduced enantioselectively using an appropriate homochiral
oxazaborolidine such as that described by Corey (J. Am. Chem. Soc.,
1987, 109, 5551), and the resulting alcohol is displaced by azide
using a method such as that described by Mitsunobu (Bull. Chem.
Soc. Japan., 1971, 44, 3427). The azide is reduced to the amine
under Staudinger conditions (Helv. Chim. Act., 1919, 2, 635) and
protected as the t-butyl carbonate. Finally, the desired aniline
intermediate, 15.3, is generated by tin (II)-mediated reduction of
the nitrobenzene.
Example 16
##STR00173##
[0701] Reagents suitable for use in the synthesis of representative
compounds of Formula 10 may be made by routes analogous to that
shown in Example 10, starting from 2-hydroxy-5-nitro-benzoic
acid.
Example 17
##STR00174##
[0703] Representative compounds of Formula 11 can be prepared as
illustrated in Examples 11-13, above. The preparation of anilines
of formula, 17.2, is illustrated in Examples 11-13 above. Anilines
of formula, 17.2, can be converted to compounds of Formula 11 using
procedures similar to those described in U.S. Pat. No. 6,054,472
and U.S. Pat. No. 6,344,465.
Example 18
[0704] The following is a general route that can be used to prepare
compounds of Formula 15.
##STR00175##
Example 19
##STR00176##
[0706] The initial Pfitzinger condensation of compound 19.1 and
compound 19.2 is achieved in a single step using potassium
hydroxide with acidic work-up, as shown. Alternatively, the initial
aldol condensation may be performed using diethylamine in ethanol,
and the quinoline ring may be formed in a second step mediated by
an acid such as hydrochloric acid in a solvent such as 1,4-dioxane.
Following removal of the benzyl protecting group via hydrogenation,
the phenol can be treated in a solvent such as tetrahydrofuran or
dimethylformamide with a base such as sodium hydride. When bubbling
ceases, diethyl phosphonomethyltriflate (prepared according to
Tetrahedron Lett., 1986, 27, 1477) is added, yielding the desired
phosphonate diester. The carboxylate is deprotected by treatment
with lithium hydroxide in ethanol to provide compound 19.4 (which
is a compound of Formula 12).
Example 20
##STR00177##
[0708] The synthesis is similar to that depicted in Example 19
except that, following deprotonation of the phenol,
E-1,4-dibromobutene is added in excess. After quenching the
reaction with aqueous ammonium chloride and extracting the product
with an organic solvent such as ethyl acetate, the mono-alkylated
product is isolated by chromatography. The resulting bromide is
heated with triethylphosphite in a solvent such as toluene to
generate the diethyl ester of the desired phosphonic acid, and the
carboxylic acid is deprotected as before to provide compound 20A
(which is a compound of Formula 12).
Example 21
[0709] The structures of Prednisone, 21A (U.S. Pat. No. 2,897,464),
and representative phosphonate esters are shown below, in which the
substituent R.sup.1 is H, alkyl, alkenyl, aryl or aralkyl. The
phosphonate compounds incorporate a phosphonate moiety
(R.sup.1O).sub.2P(O) connected to the nucleus by means of a
variable linking group, designated as "link."
##STR00178##
[0710] For example, the above scheme depicts a
protection-deprotection sequence in which the steroid side-chain is
protected as a bis-methylenedioxy (BMD) moiety. In this sequence,
Prednisone, 21A, is reacted with paraformaldehyde and an acid
catalyst such as hydrochloric acid, as described in "Protective
Groups in Organic Synthesis," by T. W. Greene and P. G. M. Wuts,
Wiley, Second Edition 1990, p. 223, to yield the BMD derivative,
21.1. The phosphonate moiety is then introduced, using the
procedures described below, to produce the phosphonate ester, 21.2.
The BMD moiety is then hydrolyzed, for example by treatment with
50% aqueous acetic acid, as described in "Protective Groups in
Organic Synthesis," by T. W. Greene and P. G. M. Wuts, Wiley,
Second Edition 1990, p. 223, to afford the triol, 21.3 (which is a
compound of Formula 23).
[0711] Optionally, depending on the nature of the reactions
employed, the 1-ketone group in the BMD compound, 21.1, is
protected before introduction of the phosphonate group. The ketone
is protected, for example, as the cyclic ethylene ketal, by
reaction in toluene solution at reflux temperature with ethylene
glycol and an acid catalyst, as described in J. Am. Chem. Soc.,
1955, 77, 1904. Deprotection is effected by reaction with
pyridinium tosylate in aqueous-acetone, as described in J. Chem.
Soc., Chem. Comm., 1351, 1987.
[0712] Alternatively, the 11-ketone is protected by conversion to
the N,N-dimethylhydrazone. The dimethyl hydrazone is prepared by
the reaction of the ketone, 21.1, with N,N-dimethylhydrazine in
ethanol-acetic acid, as described in Org. Syn., 1970, 50, 102. The
group is removed by treatment with sodium acetate and acetic acid
in aqueous tetrahydrofuran, as described in J. Am. Chem. Soc.,
1979, 101, 5841.
[0713] Alternatively, the 11-ketone is protected as the
diethylamine adduct. In this procedure, the substrate, 21.1, is
reacted with titanium tetrakis-(diethylamide), as described in J.
Chem. Soc., Chem. Comm., 406, 1983, to afford the adduct. The
ketone is deprotected by reaction with water in an aqueous organic
solvent.
[0714] The 11-protected BMD compound, 21.4, is then converted,
using the procedures described below, into the phosphonate, 21.5.
Deprotection then yields the 11-keto diol, 21.3.
Example 22
##STR00179##
[0716] The preparation of phosphonates, 22.3, in which the
phosphonate is attached by means of an imino or iminoxy group and a
variable carbon chain are depicted above. In this procedure, the
doubly-protected derivative, 21.4, is reacted with an amine or
hydroxylamine, 22.1, in which R.sup.2 is an alkyl, alkenyl,
cycloalkyl or cycloalkenyl group, optionally incorporating a
heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent.
[0717] For example, X is dialkylphosphono, bromo, hydroxy, amino,
carboxy and the like. The reaction is conducted between equimolar
amounts of the reactants in an aprotic solvent such as pyridine or
xylene, or in an alcoholic solvent such as ethanol, optionally in
the presence of an acid catalyst, to give the imine or oxime. The
preparation of oximes of steroidal 3-ketones is described in Anal.
Bioch., 1978, 86, 133 and in J. Mass. Spectrom., 1995, 30, 497. The
protecting groups are then removed to afford the ketodiol, 22.3
(which is a compound of Formula 16).
Example 23
##STR00180##
[0719] The preparation of phosphonates, P2.10, in which the
phosphonate is attached by means of an iminoxy group, is
illustrated above. The substrate, 23.1, a compound of Formula 23.1,
in which the 11-ketone is protected as the dimethyl hydrazone, is
reacted with a dialkyl phosphonomethyl hydroxylamine, P2.8,
prepared from a dialkyl trifluoromethyl-sulfonyloxymethyl
phosphonate (Tetrahedron Lett., 1986, 27, 1477) and
BOC-hydroxylamine, to afford the oxime, P2.9, which is deprotected
by reaction with 50% aqueous acetic acid, to afford the diol,
P2.10. The oxime forming reaction is typically performed at ambient
temperature in ethanol-acetic acid solution between equimolar
amounts of the reactants.
[0720] The intermediate dialkyl phosphonomethyl hydroxylamine,
P2.8, (compound, 2.7, wherein R.sup.2 is a bond) can be prepared as
follows.
##STR00181##
[0721] A phosphonate, P2.4, in which Lv is a leaving group such as
bromo or trifluoromethylsulfonyloxy, is reacted with
BOC-hydroxylamine, P2.5, (Aldrich) to produce the ether, P2.6. The
reaction is typically conducted between equimolar amounts of the
reactants in a polar solvent such as dimethyl-formamide or
tetrahydrofuran, in the presence of a base such as potassium
hydroxide or dimethylaminopyridine. Deprotection, for example, by
treatment with trifluoroacetic acid, then gives the hydroxylamine
ether, P2.7.
Example 24
##STR00182##
[0723] The dienone, 23.1, is reacted, as described in Example 23,
with O-(2-bromobenzyl)hydroxylamine, P2.11, prepared from
2-bromobenzyl bromide, to give, after deprotection, the oxime,
P2.12. The product is then reacted, in the presence of a palladium
catalyst, with a dialkyl phosphite, P2.13, to afford the
phosphonate, P2.14. The preparation of arylphosphonates by means of
a coupling reaction between aryl bromides and dialkyl phosphites is
described in J. Med. Chem., 1992, 35, 1371. The reaction is
typically performed in an inert solvent such as toluene, in the
presence of a base such as triethylamine and a catalytic amount of
tetrakis(triphenylphosphine)palladium(0).
[0724] Alternatively, the bromo compound, P2.12, is coupled with a
dialkyl vinylphosphonate, P2.15 (Aldrich), to afford the
phosphonate, P2.16. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in "Advanced
Organic Chemistry," by F. A. Carey and R. J. Sundberg, Plenum,
2001, p. 503ff and in Acc. Chem. Ras., 1979, 12, 146. The aryl
bromide and the olefin are coupled in a polar solvent such as
dimethyl-formamide or dioxan, in the presence of a palladium(0)
catalyst such as tetrakis(triphenylphosphine)palladium(0) or
palladium(II) catalyst such as palladium(II) acetate, and
optionally in the presence of a base such as triethylamine or
potassium carbonate. Optionally, the styrenoid double bond present
in the product, P2.16, is reduced, for example by reaction with
diimide, to produce the saturated analog, P2.17. The reduction of
olefinic bonds is described in "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 6ff. The
transformation is effected by means of catalytic hydrogenation, for
example using a palladium on carbon catalyst and hydrogen or a
hydrogen donor, or by the use of diimide or diborane.
[0725] Using the above procedures, but employing, in place of the
benzyloxy reagent, P2.11, different bromo-substituted aryl or
heteroaryl alkoxy hydroxylamines, and/or different dialkyl alkenyl
phosphonates, the products analogous to the compounds, P2.14, P2.16
and P2.17 are obtained.
Example 25
##STR00183##
[0727] The preparation of phosphonates of Formula 16 wherein the
phosphonate is attached by means of an imino group is illustrated
above. The substrate, 23.1, is reacted with a dialkyl 4-aminophenyl
phosphonate, P2.18 (Epsilon), to give, after deprotection, the
imine product, P2.19. The reaction is typically conducted in a
hydrocarbon solvent such as toluene or xylene, at reflux
temperature, in the presence of a basic catalyst such as sodium
methoxide, or an acid catalyst such as p-toluenesulfonic acid,
under azeotropic conditions.
Example 26
##STR00184##
[0729] The preparation of representative phosphonates of Formula 16
wherein the phosphonate is attached by means of an oximino group
and an ether linkage is illustrated above. In this procedure, the
dienone, 23.1, is reacted with O-(2-hydroxyyethyl)hydroxylamine,
P2.20 (J. Chem. Soc., Chem. Comm., 1986, 903), to yield the oxime,
P2.21. The reaction of steroidal 1,4-dien-3-ones with substituted
hydroxylamines is described in J. Steroid Bioch., 1976, 7, 795. The
reaction is performed between equimolar amounts of the reactants in
a polar organic solvent such as pyridine or methanol, optionally in
the presence of acetic acid or sodium acetate. The oxime is then
reacted in a Mitsonobu reaction with a dialkyl 4-hydroxyphenyl
phosphonate, P2.22 (Epsilon), to yield the ether oxime, P2.23. The
preparation of aromatic ethers by means of the Mitsonobu reaction
is described, for example, in "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 448, and in
"Advanced Organic Chemistry," Part B, by F. A. Carey and R. J.
Sundberg, Plenum, 2001, p. 153-4 and in Org. React., 1992, 42, 335.
The phenol and the alcohol or thiol component are reacted together
in an aprotic solvent such as, for example, tetrahydrofuran, in the
presence of a dialkyl azodicarboxylate and a triarylphosphine, to
afford the ether or thioether products. The procedure is also
described in Org. React., 1992, 42, 335-656. The ether product,
P2.23. is then converted into the ketodiol, P2.24 (which is a
compound of Formula 16).
[0730] Using the above procedures, but employing, in place of the
hydroxylamine, P2.20, different hydroxy-substituted hydroxylamines,
and/or different hydroxy-substituted aryl phosphonates, the
products analogous to P2.24 are obtained.
Example 27
##STR00185## ##STR00186##
[0732] The preparation of the phosphonate esters of Formulae 17 and
18 in which the phosphonate group is attached to the 1' or 2'
position of the pyrazole ring, by means of an aromatic or
heteroaromatic group, a heteroatom and a variable carbon chain. In
this procedure, the BMD-protected dienone, 21.1, is reduced to
afford the 1,2-dihydro product, P3.1. The catalytic hydrogenation
reaction is effected by the use of tris(triphenylphosphine)rhodium
(I) chloride, for example as described in J. Med. Chem., 2001, 44,
602. The product is then reacted with ethyl formate and a base such
as sodium hydride, in an inert solvent such as toluene or
dimethylformamide, as described in J. Am. Chem. Soc., 1964, 86,
1520, to afford the 2-formyl product, P3.2. This compound is then
reacted with an alkyl, aralkyl, aryl or heteroaryl hydrazine, P3.3,
in which the substituent X is either a phosphonate group or a group
which is subsequently transformed into a phosphonate-containing
substituent. For example, X is dialkylphosphono, bromo, hydroxy,
amino, carboxyl and the like. The reaction yields the isomeric 2'-
and 1'-aryl pyrazoles, P3.4 and P3.5. The pyrazole-forming reaction
is performed between equimolar amounts of the reactants in an
acidic solvent such as acetic acid, as described in J. Am. Chem.
Soc., 1964, 86, 1520. The pyrazoles, P3.4 and P3.5, are then
transformed via the BMD-protected intermediates, P3.6 and P3.7,
into the phosphonates, P3.8 and P3.9, which are compounds of
Formulae 17 and 18 respectively.
Example 28
##STR00187##
[0734] The preparation of phosphonates in which the phosphonate is
attached by means of a phenyl ring and an ester or an amide linkage
are illustrated above. The ketoaldehyde, P3.2, is reacted with
3-carboxyphenylhydrazine, P3.10 (Apin), to give the pyrazoles,
P3.11 and P3.12. The 2'-substituted isomer, P3.11, is then reacted
in dichloromethane solution at ambient temperature with one molar
equivalent of a dialkyl 2-hydroxy-2-methylpropyl phosphonate, P3.13
(French Patent No. 2,462,440), and dicyclohexylcarbodiimide, to
yield the ester, P3.14. The protecting groups are then removed to
yield the diol, P3.15, which is a compound of Formula 18.
[0735] Alternatively, the 1'-substituted pyrazole, P3.12, is
coupled with a dialkyl 2-aminoethyl phosphonate, P3.17 (Aurora), to
afford the amide, P3.18. The preparation of amides from carboxylic
acids and derivatives is described, for example, in "Organic
Functional Group Preparations," by S. R. Sandler and W. Karo,
Academic Press, 1968, p. 274, and "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 972ff. The
carboxylic acid is reacted with the amine in the presence of an
activating agent, such as, for example, dicyclohexylcarbodiimide or
diisopropylcarbodiimide, optionally in the presence of, for
example, hydroxybenztriazole, N-hydroxy-succinimide or
N-hydroxypyridone, in a non-protic solvent such as, for example,
pyridine, DMF or dichloromethane, to afford the amide.
[0736] Alternatively, the carboxylic acid may first be converted
into an activated derivative such as the acid chloride, anhydride,
mixed anhydride, imidazolide and the like, and then reacted with
the amine, in the presence of an organic base such as, for example,
pyridine, to afford the amide. The conversion of a carboxylic acid
into the corresponding acid chloride can be effected by treatment
of the carboxylic acid with a reagent such as, for example, thionyl
chloride or oxalyl chloride in an inert organic solvent such as
dichloromethane, optionally in the presence of a catalytic amount
of dimethylformamide. The product, P3.18, is then deprotected to
give the diol, P3.19 (which is a compound of Formula 17).
[0737] Using the above procedures, but employing different amino or
hydroxyl-substituted phosphonates, and/or different
carboxy-substituted hydrazines, the products analogous to P3.15 and
P3.19 are obtained. The functionalization procedures are
interchangeable between the pyrazole substrates, P3.11 and
P3.12.
Example 29
##STR00188##
[0739] The preparation of the phosphonates of Formulae 17 and 18
wherein the phosphonate group is attached by means of a phenyl
group and an alkoxy or alkylthio carbon chain is illustrated above.
In this procedure, the ketoaldehyde, P3.2, is reacted with
4-hydroxyphenyl hydrazine, P3.20 (EP 437 105), to produce the
pyrazoles, P3.21 and P3.22. The 1'-substituted isomer, P3.21, is
reacted, in dimethylformamide solution at 70', with a dialkyl
bromopropyl phosphonate, P3.23 (J. Amer. Chem. Soc., 2000, 122,
1554), and potassium carbonate, to give the phosphonate, P3.24. The
product is then deprotected to afford the diol, P3.25.
[0740] Alternatively, the 2'-substituted pyrazole, P3.22, is
reacted in a Mitsonobu reaction, as described above, with a dialkyl
mercaptoethyl phosphonate, P3.26 (Zh. Obschei. Khim., 1973, 43,
2364), to prepare the thioether phosphonate, P3.27, which is
deprotected to give the diol, P3.28.
[0741] Using the above procedures, but employing, in place of the
hydroxyphenyl reagent, P3.20, different hydroxy-substituted
aralkyl, aryl or heteroaryl alkoxy hydrazines, and/or different
dialkyl bromo or mercapto-substituted phosphonates, the products
analogous to the compounds, P3.25 and P3.28 are obtained.
Example 30
##STR00189## ##STR00190##
[0743] The preparation of phosphonate esters of Formulae 17 and 18
wherein the phosphonate group is attached by means of a variable
carbon linkage is illustrated above. In this procedure, the
ketoaldehyde, P3.2, is reacted with hydrazine to afford the
pyrazole derivative, P4.1. The reaction of steroidal
2-formyl-3-ketones with hydrazine is described in J. Am. Chem. Soc,
1964, 86, 1520. The reaction is performed in acetic acid at ambient
temperature. The pyrazole product is then reacted with a
bromomethyl compound, P4.2, to yield the alkylation products, P4.3
and P4.4. The alkylation of substituted pyrazoles is described, for
example, in "Heterocyclic Chemistry," by T. L. Gilchrist, Longman,
1992, p. 309. The reaction is typically performed between equimolar
amounts of the substrates in a polar solvent such as
dimethylformamide or tetrahydrofuran, in the presence of a base
such as dimethylaminopyridine, lithium hexamethyldisilazide and the
like. The products, P4.3 and P4.4, are, except in cases where X is
dialkylphosphono, converted into the phosphonates, P4.5 and P4.6,
using the procedures described herein. Deprotection affords the
diols, P4.7 and P4.8 (which are compounds of Formulae 18 and 17,
respectively).
Example 31
##STR00191##
[0745] As illustrated above, the pyrazole, P4.1, is reacted with
one molar equivalent of a dialkyl trifluoromethanesulfonyloxy
phosphonate, P4.9, as described above to give the alkylated
pyrazoles, P4.10 and P4.11. Deprotection yields the diols, P4.12
and P4.13 (which are compounds of Formulae 18 and 17
respectively).
Example 32
##STR00192##
[0747] As illustrated above, the pyrazole, P4.1, is reacted, as
described above, with 1,4-bis(bromomethyl)cyclohexane, P4.14
(Salor), to give the pyrazoles, P4.15 and P4.16. The product,
P4.15, is subjected to an Arbuzov reaction, in which the
bromomethyl substituent is converted into the dialkyl
phosphonomethyl substituent, by reaction with a trialkyl phosphite
to prepare, after deprotection of the side chain, the phosphonate,
P4.17, (which is a compound of Formula 18).
[0748] The pyrazole, P4.16, is reacted in dimethylformamide with
potassium carbonate and a dialkyl aminomethyl phosphonate, P4.18,
(Interchim) to give after deprotection the amino phosphonate,
P4.19, which is a compound of Formula 17.
[0749] Using the above procedures, but employing, in place of the
dibromide, P4.14, different dibromides, and/or different
amino-substituted phosphonates, the products analogous to P4.17 and
P4.19 are obtained.
Example 33
[0750] Representative compounds of the invention can be prepared as
generally described by Westwood et al, J. Med. Chem., 1996, 39,
4608-4621, and according to the following general route.
##STR00193##
[0751] Coupling of a suitable aniline, 33.1, wherein X.sup.1 is
hydrogen, halo, trifluoromethyl, (C.sub.1-C.sub.3)alkyl, cyano, or
(C.sub.1-C.sub.3)alkoxy, with acid chloride, 33.2, provides
compound, 33.3 (which is a representative compound of Formula 19 or
20).
[0752] The synthesis of two suitable anilines that can be employed
in the above reaction is outlined below.
##STR00194##
[0753] 3-Nitrophenol is alkylated with E-1,4-dibromobutene and the
resulting monobromide is heated with triethylphosphite in a solvent
such as toluene (or other Arbuzov reaction conditions to generate
the diethyl ester of the desired phosphonic acid, 33.4. (See Engel,
R., "Synthesis of Carbon-phosphorus Bonds," CRC press, 1988).
Finally, the desired aniline is generated by tin (II)-mediated
reduction of the nitrobenzene.
##STR00195##
[0754] The methyl ester of 3-nitro-4-trifluoromethylbenzoic acid is
treated with tin (II) chloride to produce the corresponding
aniline. The 3-iodobenzoic acid is generated by diazotization and
treatment with potassium iodide. A diethylphosphonate ester is
attached via an acetylene linker using palladium catalysis, and
after saponification of the benzoate ester, Curtius rearrangement
of the acyl azide provides an aniline suitable for incorporation
into representative MNA-715 analogs of the invention.
Example 34
[0755] Representative compounds of Formulae 21 and 22 can be
prepared as generally described by Westwood et al, J. Med. Chem.,
1996, 39, 4608-4621, and according to the following general
route.
##STR00196##
[0756] Coupling of a suitable aniline, 34.1, wherein X.sup.2 is
hydrogen, halo, trifluoromethyl, cyano, or methyl with acid
chloride, 34.2, provides a representative compound of Formulae 21
and 22. Anilines prepared as described in Example 33 and elsewhere
herein can be incorporated into this synthesis.
Example 35
##STR00197##
[0758] 5-Nitro-isobenzofuran-1,3-dione, 35.1, (commercially
available), is converted to
5-amino-2-(2,6-dioxo-piperidin-3-yl)-isoindole-1,3-dione, 35.2,
following the procedures reported in Bioorg. Med. Chem. Lett.,
1999, 9, 1625. This amine intermediate is subjected to a reductive
amination with diethyl-phosphonoacetaldehyde (obtained from
ozonolysis of diethyl allyphosphonate) in the presence of a
reducing agent such as sodium triacetoxyborohydride to generate the
desired amine linker analog (J. Org. Chem., 1996, 61, 3849).
Alternatively, the amine is acylated with an activated
diethylphosphonoacetic acid to provide the desired amide linker
compound, according to a procedure such as those reported in J.
Med. Chem., 1982, 25, 960 and J. Med. Chem., 1984, 27, 600. The
activated diethylphosphonoacetic acid can be obtained by treatment
in a solvent such as dimethylformamide with a coupling reagent such
as diethyl cyanophosphonate and a base such as
diisopropylethylamine at room temperature. A specific example where
X is CH.sub.2 is illustrated below.
##STR00198##
[0759] Alternatively,
2-(1,3-dioxo-1,3-dihydro-isoindol-2-yl)-pentanedioic acid, 35.4,
(commercially available) is treated in a solvent such as
acetonitrile with triethylamine, 1-hydroxybenzotriazole,
4-methoxybenzylamine, and 1,3-dicyclohexylcarbodiimide. After the
reaction is complete, the solvent is removed and the residue is
purified by chromatography to generate the desired analog, 35.3,
according to a procedure such as that reported in J. Med. Chem.,
2003, 46, 3793.
Example 36
##STR00199##
[0761] The Boc-protected
(1S)-1-(9-deazaguanin-9-yl)-1,4-dideoxy-1,4-imino-D-ribitol,
compound, 36.3, is prepared by stirring the
(1S)-1-(9-deazaguanin-9-yl)-1,4-dideoxy-1,4-imino-D-ribitol (WO
99/19338 and Evans, G. B. et al., Tetrahedron, 2000, 56, 3053, also
reported in Evans, G. B. et al., J. Med. Chem. 2003, 46, 3412) with
BOC anhydride as described in Greene, T., "Protective groups in
organic synthesis," Wiley-Interscience, 1999. Compound, 36.3, is
then treated in a solvent such as tetrahydrofuran or
dimethylformamide with a base such as sodium hydride. When bubbling
ceases, diethyl phosphonomethyl-triflate (prepared according to
Tetrahedron Lett., 1986, 27, 1477) is added, yielding the desired
phosphonate diester, 36.4, after deprotection of the BOC group
using trifluoroacetic acid (TFA) (which is a compound of Formula
25).
Example 37
##STR00200##
[0763] Protected compound, 37.1,
((1R)-1-(9-deazahypoxanthin-9-yl)-1,2,4-trideoxy-1,4-imino-D-erythro-pent-
itol, as the hydrochloride salt) is prepared as described in Evans,
G. B. et al., Tetrahedron, 2000, 56, 3053, using di-t-butyl
dicarbonate in dichloromethane. Oxidation of the 5'-OH followed by
elimination provides glycal, 37.3 (see the procedure of Zemlicka J.
et al., J. Am. Chem. Soc., 1972, 94, 9, 3213). Selenoetherification
provides the protected phosphonate, 37.4 (Kim, C. et al., J. Org.
Chem., 1991, 56, 2642). Oxidative elimination of the phenylselenide
(as described in Kim, C. et al., J. Org. Chem., 1991, 56, 2642)
followed by stereoselective dihydroxylation provides the desired
diol, 37.6. Finally, the protecting group is removed to provide a
compound, 37.7, compound of Formula 26.
Example 38
##STR00201## ##STR00202##
[0765]
(1R)-1-(9-Deazahypoxanthin-9-yl)-1,2,4-trideoxy-1,4-imino-D-erythro-
-pentitol, prepared as the HCl salt as described in Evans, G. B. et
al., Tetrahedron, 2000, 56, 3053, is first protected and then
oxidized with PtO.sub.2 to provide carboxylic acid, 38.1.
Decarboxylative elimination is achieved using dimethylformamide
dineopentyl acetal in dimethylformamide at high temperature
(Zemlicka J. et al., J. Am. Chem. Soc., 1972, 94, 9, 3213).
Selenoetherification followed by treatment of the protected glycal
with silver perchlorate in the presence of
diethyl(hydroxylmethyl)phosphonate (Phillion, D. et al.,
Tetrahedron Lett., 1986, 27, 1477) provides the phosphonate, 38.3
(Kim, C. et al., J. Org. Chem., 1991, 56, 2642). Oxidative
elimination of the selenide followed by dihydroxylation using
osmium tetraoxide provides diol, 38.5. Removal of the amine
protecting group, according to the procedure of Greene, T.,
"Protective groups in organic synthesis," Wiley-Interscience, 1999,
provides compound 38.6.
Example 39
[0766] Synthetic methodologies and intermediate compounds that can
be used to prepare pro-drugs of analogs of thalidomide are
described below.
##STR00203## [0767] link includes 1 or more atoms; 2 or more is
preferred
##STR00204##
[0768] 2-Methyl-4-nitrobenzoic acid methyl ester (commercially
available) is converted to
3-(5-amino-1-oxo-1,3-dihydro-isoindol-2-yl)-piperidine-2,6-dione,
39.1, following the procedures reported in Bioorg. Med. Chem.
Lett., 1999, 9, 1625. This amine intermediate is subjected to a
reductive amination with diethylphosphonoacetaldehyde (obtained
from ozonolysis of diethyl allyphosphonate) in the presence of a
reducing agent such as sodium triacetoxyborohydride to generate the
desired amine linker analog, 39.2 (J. Org. Chem., 1996, 61, 3849).
Alternatively, the amine is acylated with an activated
diethylphosphonoacetic acid to provide the desired amide linker
compound, 39.3, according to a procedure such as those reported in
J. Med. Chem., 1982, 25, 960 and J. Med. Chem., 1984, 27, 600. The
activated diethylphosphono-acetic acid can be obtained by
treatment, in a solvent such as dimethylformamide, with a coupling
reagent such as diethyl cyanophosphonate and a base such as
diisopropylethylamine at room temperature.
[0769] 2-Methyl-3-nitrobenzoic acid methyl ester (commercially
available) is treated in a solvent such as carbon tetrachloride
with N-bromosuccinimide under light to produce
2-bromomethyl-3-nitrobenzoic acid methyl ester, 39.4. The benzylic
bromide is treated in a solvent such as dimethylformamide with
[2-(3-amino-2,6-dioxo-piperidin-1-yl)-ethyl]-phosphonic acid
diethyl ester (for the preparation of this compound, see Example
40, below) in the presence of a base such as triethylamine. The
coupled product is then reduced by hydrogenation (Bioorg. Med.
Chem. Lett., 1999, 9, 1625) to afford the desired analog.
Example 40
##STR00205##
[0771] 2-Methyl-4-nitrobenzoic acid methyl ester, 39.2
(commercially available), is converted to
3-(5-amino-1-oxo-1,3-dihydro-isoindol-2-yl)-piperidine-2,6-dione,
following the procedures reported in Bioorg. Med. Chem. Lett.,
1999, 9, 1625. This amine intermediate is subjected to a reductive
amination with diethylphosphonoacetaldehyde (obtained from
ozonolysis of diethyl allyphosphonate) in the presence of a
reducing agent such as sodium triacetoxyborohydride to generate the
desired amine linker analog (J. Org. Chem., 1996, 61, 3849).
Alternatively, the amine is acylated with an activated
diethylphosphonoacetic acid to provide the desired amide linker
compound, according to a procedure such as those reported in J.
Med. Chem., 1982, 25, 960 and J. Med. Chem., 1984, 27, 600. The
activated diethylphosphonoacetic acid can be obtained by treatment
in a solvent such as dimethylformamide with a coupling reagent such
as diethyl cyanophosphonate and a base such as
diisopropylethylamine at room temperature.
Example 40A
##STR00206##
[0773] 2-Methyl-3-nitrobenzoic acid methyl ester, 39.2
(commercially available) is treated in a solvent such as carbon
tetrachloride with N-bromosuccinimide under light to produce
2-bromomethyl-3-nitrobenzoic acid methyl ester, 39.4. This benzylic
bromide is treated in a solvent such as dimethylformamide with
[2-(3-amino-2,6-dioxo-piperidin-1-yl)-ethyl]-phosphonic acid
diethyl ester (for the preparation of this compound, see below) in
the presence of a base such as triethylamine. The coupled product
is then reduced by hydrogenation (Bioorg. Med. Chem. Lett., 1999,
9, 1625) to afford the desired analog.
[0774] [2-(3-amino-2,6-dioxo-piperidin-1-yl)-ethyl]-phosphonic acid
diethyl ester, 40.1, is obtained according to a procedure such as
that reported in J. Med. Chem., 2003, 46, 3793. Accordingly,
benzyloxycarbonyl-protected glutaric acid is treated in a solvent
such as acetonitrile with triethylamine, 1-hydroxybenzotriazole,
diethyl 2-aminoethylphosphonate and 1,3-dicyclohexylcarbodiimide.
After the reaction is complete, the solvent is removed and the
residue is purified by chromatography to generate the cyclic
product, which is subjected to hydrogen in the presence of
palladium catalysis to afford the desired intermediate.
[0775] Further manipulations can be performed on the phosphonate
moiety prior to the final deprotection. These types of
transformations are more extensively described herein.
Example 41
##STR00207##
[0777] The structures of Diprolene, 41A (German Patent DE 2905674),
and the esters, 41.1-41.3, are shown below, in which the
substituent R.sup.1 is H, alkyl, alkenyl, aryl or aralkyl. The
compounds, 41.1-41.3, incorporate a phosphonate moiety
(R.sup.1O).sub.2P(O) connected to the nucleus by means of a
variable linking group, designated as "link" in the attached
structures.
Example 42
##STR00208## ##STR00209##
[0779] A protection-deprotection sequence in which the steroid
side-chain is protected as a bis-methylenedioxy (BMD) moiety is
shown above. The propionate ester groups of compound, 42.1, are
hydrolyzed, for example by reaction with two molar equivalents of
lithium hydroxide in aqueous dimethoxyethane solution at ambient
temperature, to give the diol, 42.2. The product is then reacted
with paraformaldehyde and an acid catalyst such as hydrochloric
acid, as described in "Protective Groups in Organic Synthesis," by
T. W. Greene and P. G. M. Wuts, Wiley, Second Edition 1990, p. 223,
to yield the BMD derivative, 42.3. The phosphonate moiety is then
introduced, using the procedures described below, to produce the
phosphonate ester, 42.4. Prior to hydrolysis of the BMD protecting
group, the 11-hydroxyl group is protected. The protecting group is
selected so that it is stable to the conditions required for
removal of the BMD group, and so that it is removable without
affecting the subsequently introduced 17,21-diester moiety.
[0780] For example, the 11-hydroxyl group is protected by
conversion to the 4-azidobutyrate ester, by reaction with
4-azidobutyryl chloride in pyridine. The 11-azidobutyrate group is
then removed from the diester, 42.7, by reaction with
triphenylphosphine, as described in Bull. Soc. Chem. Jpn., 1986,
59, 1296. Alternatively, the 11-hydroxyl group is protected by
conversion to the 2-(tri-methylsilyl)ethyl carbonate, by reaction
with 2-(trimethylsilyl)ethyl carbonyl chloride and pyridine. The
2-(trimethylsilyl) carbonate is removed from the diester, 42.7, by
reaction with tetrabutylammonium fluoride in tetrahydrofuran at
ambient temperature, as described in Tet. Lett., 1981, 22, 969.
[0781] Alternatively, the 11-hydroxyl group is protected by
conversion to the trichloroacetyl ester, by reaction with
trichloroacetyl chloride in dimethylformamide-pyridine. The
trichloroacetyl ester is removed by reaction with ethanolic ammonia
at ambient temperature, as described in Coll. Czech. Chem. Commun.,
1962, 27, 2567.
[0782] The BMD moiety in the protected product, 42.5, is then
hydrolyzed, for example by treatment with 50% aqueous acetic acid,
as described in "Protective Groups in Organic Synthesis," by T. W.
Greene and P. G. M. Wuts, Wiley, Second Edition 1990, p. 223, to
afford the diol, 42.6. The diol compound is then acylated, for
example by reaction with propionic acid and dicyclohexyl
carbodiimide in dimethylformamide at ambient temperature, or by
reaction with propionyl chloride and triethylamine in
dichloromethane, to produce the dipropionate, 42.7. Deprotection of
the 11-hydroxyl group, as described above, then affords the
diester, 42.8.
[0783] Alternatively, the 20-ketone group is protected as the
diethylamine adduct by reaction with titanium
tetrakis(diethylamide), as described in Protective Groups in
Organic Synthesis, by T. W. Greene and P. G. M Wuts, Wiley, Second
Edition 1990, p. 219.
Example 43
##STR00210##
[0785] The preparation of phosphonates in which the phosphonate is
attached by means of an imino or iminoxy group and a variable
carbon chain is illustrated above. In this procedure, the
BMD-protected derivative, 42.3, is reacted with an amine or
hydroxylamine, 43.1, in which R.sup.2 is an alkyl, alkenyl,
cycloalkyl or cycloalkenyl group, optionally incorporating a
heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, to afford the imine or
iminoxy product, 43.2. The reaction is conducted between equimolar
amounts of the reactants in an aprotic solvent such as pyridine or
xylene, or in an alcoholic solvent such as ethanol, optionally in
the presence of an acid catalyst, to give the imine or oxime. The
preparation of oximes of steroidal 3-ketones is described in Anal.
Bioch., 1978, 86, 133 and in J. Mass. Spectrom., 1995, 30, 497. The
BMD-protected compound, 43.2, is then converted, as described
above, into the diester, 43.3.
##STR00211##
[0786] The preparation of hydroxylamine ethers incorporating a
phosphonate group is shown above. In this procedure, a phosphonate,
43.4, in which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxylamine, 43.5
(Aldrich), to produce the ether, 43.6. The reaction is conducted
between equimolar amounts of the reactants in a polar solvent such
as dimethylformamide or tetrahydrofuran, in the presence of a base
such as potassium hydroxide or dimethylaminopyridine, to give the
product, 43.6. Deprotection, for example by treatment with
trifluoroacetic acid, then gives the hydroxylamine ether, 43.7.
Example 44
##STR00212##
[0788] The preparation of phosphonates in which the phosphonate is
attached by means of an iminoxy group is illustrated above. In this
procedure, the substrate, 42.3, is reacted with a dialkyl
phosphonomethyl hydroxylamine, 44.1, prepared as described above
from a dialkyl trifluoromethylsulfonyloxymethyl phosphonate
(Tetrahedron Lett., 1986, 27, 1477) and BOC-hydroxylamine, to
afford, after deprotection and side chain acylation, the oxime
ether, 44.2. The oxime forming reaction is performed at ambient
temperature in pyridine solution between equimolar amounts of the
reactants.
[0789] Using the above procedures, but employing, in place of the
oxime ether, 44.1, different oxime ethers, 43.7, the corresponding
products, 43.3 are obtained.
Example 45
##STR00213##
[0791] The preparation of phosphonates incorporating an iminoxy
group, by means of the reaction between the substrate the
substrate, 42.3, and O-2-(5-bromo-2-thienyl)ethoxyhydroxylamine,
45.1, prepared as described above from 2-(5-bromo-2-thienyl)ethyl
bromide (J. Chem. Soc., Perkin Trans. Phys. Org. Chem., 1975, 821),
is illustrated above. The resultant oxime ether is converted, by
deprotection and side chain acylation, into the compound, 45.2,
which is then reacted, in the presence of a palladium catalyst,
with a dialkyl phosphite, 45.3, to afford the phosphonate, 45.4.
The preparation of arylphosphonates by means of a coupling reaction
between aryl bromides and dialkyl phosphites is described in J.
Med. Chem., 1992, 35, 1371. The reaction is performed in an inert
solvent such as toluene, in the presence of a base such as
triethylamine and a catalytic amount of
tetrakis(triphenylphosphine)palladium(0).
[0792] Alternatively, the bromo-substituted product, 45.2, is
coupled, in a palladium-catalyzed Heck reaction, with a dialkyl
propenyl phosphonate, 45.5, (Acros) to give the unsaturated
phosphonate, 45.6. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in "Advanced
Organic Chemistry," by F. A. Carey and R. J. Sundberg, Plenum,
2001, p. 503ff and in Acc. Chem. Res., 1979, 12, 146. The aryl
bromide and the olefin are coupled in a polar solvent such as
dimethylformamide or dioxan, in the presence of a palladium(0)
catalyst such as tetrakis(triphenylphosphine)-palladium(0) or
palladium(II) catalyst such as palladium(II) acetate, and
optionally in the presence of a base such as triethylamine or
potassium carbonate.
[0793] Optionally, the styrenoid double bond present in the
product, 45.6, is reduced, for example by reaction with diimide, to
produce the saturated analog, 45.7. The reduction of olefinic bonds
is described in "Comprehensive Organic Transformations," by R. C.
Larock, VCH, 1989, p. 6ff. The transformation is effected by means
of catalytic hydrogenation, for example using a palladium on carbon
catalyst and hydrogen, or a hydrogen donor, or by the use of
diimide or diborane.
[0794] Using the above procedures, but employing, in place of the
bromothienyl reagent, 45.1, different bromo-substituted aryl or
heteroaryl alkoxy hydroxylamines, and/or different dialkyl alkenyl
phosphonates, the products analogous to the compounds 45.4, 45.6
and 45.7 are obtained.
Example 46
##STR00214##
[0796] The preparation of phosphonates in which the phosphonate is
attached by means of an imino group is illustrated above. In this
procedure, the substrate, 42.3, which is reacted with a dialkyl
2-aminophenyl phosphonate, 46.1 (Aurora), to give, after
deprotection and side chain acylation, the imine product, 46.2. The
reaction is conducted in a hydrocarbon solvent such as toluene or
xylene, at reflux temperature, in the presence of a basic catalyst
such as sodium methoxide, or an acid catalyst such as
p-toluenesulfonic acid, under azeotropic conditions, to give the
product, 46.2.
[0797] Using the above procedures, but employing, in place of the
2-amino-phenyl phosphonate, 46.1, different amino-substituted aryl
or heteroaryl phosphonates, products analogous to 46.2 are
obtained.
Example 47
##STR00215##
[0799] An alternative method for the preparation of phosphonates in
which the phosphonate is attached by means of an oximino group is
illustrated above. In this procedure, the dienone, 42.3, is reacted
with O-(carboxymethyl)hydroxyl-amine, 47.1 (Interchim), to yield,
after deprotection and side chain acylation, the oxime, 47.2. The
reaction of steroidal 1,4-dien-3-ones with hydroxylamine is
described in J. Steroid Bioch., 1976, 7, 795. The reaction is
performed between equimolar amounts of the reactants in a polar
organic solvent such as pyridine or methanol, optionally in the
presence of acetic acid or sodium acetate. The oxime, 47.2, is then
reacted with a dialkyl 3-hydroxyphenyl phosphonate, 47.3 (Epsilon),
in a Mitsonobu reaction, to yield the substituted oxime, 47.4. The
preparation of aromatic ethers and thioethers by means of the
Mitsonobu reaction is described, for example, in "Comprehensive
Organic Transformations," by R. C. Larock, VCH, 1989, p. 448, and
in "Advanced Organic Chemistry," Part B, by F. A. Carey and R. J.
Sundberg, Plenum, 2001, p. 153-4 and in Org. React., 1992, 42, 335.
The phenol and the hydroxy or mercapto component are reacted
together in an aprotic solvent such as, for example,
tetrahydrofuran, in the presence of a dialkyl azodicarboxylate and
a triarylphosphine, to afford the ether or thioether products. The
procedure is also described in Org. React., 1992, 42, 335-656. The
product, 47.4, is then transformed, by deprotection and acylation,
into the diester, 47.5.
[0800] Using the above procedures, but employing, in place of the
phosphonate, 47.3, different dialkyl hydroxy-substituted aryl or
heteroaryl phosphonates, the products analogous to 47.5 are
obtained.
Example 48
##STR00216##
[0802] The preparation of the phosphonate esters in which the
phosphonate group is attached to the 1' or 2' position of the
pyrazole ring, by means of an aromatic or heteroaromatic group, a
heteroatom and a variable carbon chain is illustrated above. In
this procedure, Diprolene, 41A, is reduced to afford the
1,2-dihydro product, 48.1. The catalytic hydrogenation reaction is
effected by the use of tris(triphenylphosphine)rhodium (I)
chloride, for example as described in J. Med. Chem., 2001, 44, 602.
The product is then reacted with ethyl formate and a base such as
sodium hydride, in an inert solvent such as toluene or
dimethylformamide, as described in Australian Patent Application
275950409, to afford the 2-formyl product, 48.2.
[0803] Optionally, the substrate, 41A, is protected, for example as
described in Example 42, above, prior to the formylation reaction,
as described in J. Am. Chem. Soc., 1964, 86, 1520. The 2-formyl
product is then reacted with an aryl or heteroaryl hydrazine, 48.3,
in which the substituent X is either a phosphonate group or a group
which is subsequently transformed into a phosphonate-containing
substituent. For example, X is dialkylphosphono, bromo, hydroxy,
amino, carboxyl and the like. The reaction yields the isomeric 2'-
and 1'-aryl pyrazoles, 48.4 and 48.5. The ring-forming reaction is
performed between equimolar amounts of the reactants in an acidic
solvent such as acetic acid, as described in J. Am. Chem. Soc.,
1964, 86, 1520. The pyrazoles, 48.4 and 48.5 are then transformed,
for example by the procedures described in Examples 49-50,
respectively into the phosphonates, 48.6 and 48.7.
Example 49
##STR00217##
[0805] The preparation of phosphonates in which the phosphonate is
attached by means of a phenyl group is illustrated above. In this
sequence, the ketoaldehyde, 48.2, is reacted, as described above,
with 2-bromophenylhydrazine, 49.1 (Fluka), to give the isomeric
pyrazole products, 49.2 and 49.3. The products are then reacted, as
described herein, with a dialkyl phosphite HP(O)(OR.sup.1).sub.2
and a palladium catalyst, to afford respectively the phosphonates,
49.4 and 49.5. Using the above procedures, but employing, in place
of 2-bromophenyl hydrazine, different bromoaryl or bromoheteroaryl
hydrazines, 48.3, the products, 48.6 and 48.7 are obtained.
Example 50
##STR00218##
[0807] The preparation of phosphonates in which the phosphonate is
attached by means of an aromatic or heteroaromatic group and a
saturated or unsaturated alkyl chain is illustrated above. In this
procedure, the bromophenyl-substituted pyrazole, 49.2, is coupled
in a Heck reaction, as described above, with, for example a dialkyl
butenyl phosphonate, 50.1, (Org. Lett., 2001, 3, 217) to give the
unsaturated phosphonate product, 50.2. Optionally, the product is
reduced, as described above, to give the saturated analog, 50.3.
Application of the above procedures to the isomeric bromophenyl
pyrazole, 49.3, affords the products isomeric with, 50.2 and 50.3.
Using the above procedures, but employing, in place of the
phosphonate, 50.1, different dialkyl alkenyl phosphonates, and/or
different bromoaryl or heteroaryl pyrazoles, 48.4 or 48.5, the
products analogous to 50.2 and 50.3 are obtained.
Example 51
##STR00219##
[0809] The preparation of phosphonates, 51.5 and 51.6, in which the
phosphonate is attached by means of an aryl or heteroaryl group and
an alkoxy chain is illustrated above. In this procedure,
4-Aminothiophenol, 51.1, is reacted in dimethylformamide solution
at ambient temperature with a dialkyl
trifluoro-methanesulfonyloxymethyl phosphonate, 51.2 (Tetrahedron
Lett., 1986, 27, 1477), and potassium carbonate to give the
thioether, 51.3. The product is then converted into the
corresponding hydrazine, 51.4, by means of a diazotization reaction
in aqueous ethanolic hydrochloric acid, followed by reduction of
the diazonium chloride with tin(II) chloride, as described in J.
Med. Chem., 2001, 44, 4031. The hydrazine is then reacted, as
described above, with the ketoaldehyde, 48.2, to form the isomeric
pyrazoles, 51.5 and 51.6.
[0810] Using the above procedures, but employing, in place of the
triflate, 51.2, different dialkylphosphono alkyl bromides or
triflates, and/or different aromatic or heteroaromatic mercapto or
hydroxyamines, the products analogous to 51.5 and 51.6 are
obtained.
Example 52
##STR00220## ##STR00221##
[0812] The preparation of phosphonates in which the phosphonate is
attached by means of a pyridyl group a heteroatom and a variable
carbon chain is illustrated above. In this procedure,
3-amino-5-hydroxypyridine, 52.1, is converted, by reaction with
acetic anhydride, into the diacetyl analog, 52.2. The product is
then transformed by diazotization and reduction, as described
above, into the hydrazine, 52.3. The hydrazine, 52.3, is then
reacted with the ketoaldehyde, 48.2, to give the isomeric
pyrazoles, 52.4 and 52.5. The 2'-pyridyl product, 52.4, is reacted
in a Mitsonobu reaction, as described above, with a dialkyl
hydroxyethyl phosphonate, 52.6 (Zh. Obschei. Khim., 1973, 43,
2364), to afford the ether, 52.7. Application of this procedure to
the isomeric phenol, 52.5, affords the product isomeric to
compound, 52.7.
[0813] Alternatively, the isomeric phenol, 52.5, is reacted, in
dimethyl-formamide solution at about 800, with one molar equivalent
of a dialkyl bromopropynyl phosphonate, 52.8 (Bioorg. Med. Chem.
Lett., 1994, 4, 273), and cesium carbonate, to prepare the
phosphonate, 52.9. Application of this procedure to the isomeric
phenol, 52.4, affords the product isomeric with compound, 52.4.
Using the above procedures, but employing, in place of the
carbinol, 52.6, or the bromide, 52.8, different thiols, alcohols or
bromides, and/or different phenols, 48.4 or 48.5, in which X is OH,
the corresponding products analogous to 52.7 and 52.9 are
obtained.
Example 53
##STR00222##
[0815] The preparation of the phosphonate esters in which the
phosphonate group is attached by means of a variable carbon linkage
is illustrated above. In this procedure, the ketoaldehyde, 48.2, is
reacted with hydrazine, to afford the pyrazole derivative, 53.1.
The reaction of steroidal 2-formyl-3-ketones with hydrazine is
described in J. Am. Chem. Soc, 1964, 86, 1520. The reaction is
performed in acetic acid at ambient temperature. The resulting
pyrazole is then reacted with a dialkyl bromomethyl phosphonate,
53.2, in which R.sup.2 is as defined above, to produce the isomeric
2' and 1' alkylation products, 53.3 and 53.4, respectively. The
alkylation of substituted pyrazoles is described, for example, in
"Heterocyclic Chemistry," by T. L. Gilchrist, Longman, 1992, p.
309.
Example 54
##STR00223##
##STR00224##
[0817] Pyrazole, 53.1, is reacted, in dimethylformamide solution at
ca. 90.degree., with a dialkyl bromopropyl phosphonate, 54.1
(Aldrich), and a base such as dimethylaminopyridine or lithium
hexamethyldisilazide, to yield the isomeric alkylation products,
54.2 and 54.3.
[0818] As shown in Scheme 54A, the pyrazole, 53.1, is reacted in
dimethyl-formamide solution at ambient temperature with one molar
equivalent of 1,4-dibromobut-2-yne, 54.4 (Narchem), and potassium
carbonate, to afford the alkylation products, 54.5 and 54.6. The
products are then heated at 120.degree. with a trialkyl phosphite
in an Arbuzov reaction, to yield the phosphonates, 54.7 and 54.8.
The Arbuzov reaction is described in Handb. Organophosphorus Chem.,
1992, 115-72. Using the above procedures, but employing, in place
of the dibromide, 54.4, different alkyl, alkenyl or alkynyl
dibromides, the products analogous to 54.7 and 54.8 are
obtained.
Example 55
[0819] The structures of Aclometasone dipropionate, 55/A (J. Med.
Chem., 1980, 23, 430; U.S. Pat. No. 4,124,707), and the esters,
55A-55C, are shown below, in which the substituent R.sup.1 is H,
alkyl, alkenyl, aryl or aralkyl. The compounds, 55A-55C,
incorporate a phosphonate moiety (R.sup.1O).sub.2P(O) connected to
the nucleus by means of a variable linking group, designated as
"link" in the attached structures.
##STR00225##
##STR00226## ##STR00227##
[0820] The steroid side-chain is protected as a bis-methylenedioxy
(BMD) moiety, as illustrated in Scheme 55A. In this sequence, the
propionate esters are hydrolyzed, for example by reaction with two
molar equivalents of lithium hydroxide in aqueous dimethoxyethane
solution at ambient temperature, to give the diol, 55.1. The
product is then reacted with paraformaldehyde and an acid catalyst
such as hydrochloric acid, as described in "Protective Groups in
Organic Synthesis," by T. W. Greene and P. G. M. Wuts, Wiley,
Second Edition 1990, p. 223, to yield the BMD derivative, 55.2. The
phosphonate moiety is then introduced, using the procedures
described below, to produce the phosphonate ester, 55.3. Prior to
hydrolysis of the BMD protecting group, the 11-hydroxyl group is
protected. The protecting group is selected so that it is stable to
the conditions required for removal of the BMD group, and so that
it is removable without affecting the subsequently introduced
17,21-diester moiety. For example, the 11-hydroxyl group is
protected by conversion to the 4-azido-butyrate ester, by reaction
with 4-azidobutyryl chloride in pyridine. The 11-azidobutyrate
group is then removed from the diester, 55.6, by reaction with
triphenylphosphine, as described in Bull. Soc. Chem. Jpn., 1986,
59, 1296. Alternatively, the 11-hydroxyl group is protected by
conversion to the 2-(tri-methylsilyl)ethyl carbonate, by reaction
with 2-(trimethylsilyl)ethyl carbonyl chloride and pyridine. The
2-(trimethylsilyl) carbonate is removed from the diester, 55.6, by
reaction with tetrabutylammonium fluoride in tetrahydrofuran at
ambient temperature, as described in Tet. Lett., 1981, 22, 969.
[0821] Alternatively, the 11-hydroxyl group is protected by
conversion to the trichloroacetyl ester, by reaction with
trichloroacetyl chloride in dimethyl-formamidepyridine. The
trichloroacetyl ester is removed by reaction with ethanolic ammonia
at ambient temperature, as described in Coll. Czech. Chem. Commun.,
1962, 27, 2567. The BMD moiety in the protected product, 55.4, is
then hydrolyzed, for example by treatment with 50% aqueous acetic
acid, as described in "Protective Groups in Organic Synthesis," by
T. W. Greene and P. G. M. Wuts, Wiley, Second Edition 1990, p. 223,
to afford the diol, 55.5. The diol, 55.5, is acylated, for example
by reaction with propionic acid and dicyclohexyl carbodiimide in
dimethylformamide at ambient temperature, or by reaction with
propionyl chloride and triethylamine in dichloromethane, to produce
the dipropionate, 55.6. Deprotection of the 11-hydroxyl group, as
described above, then affords the diester, 55.7.
[0822] Alternatively, the 20-ketone group is protected as the
diethylamine adduct by reaction with titanium
tetrakis(diethylamide), as described in "Protective Groups in
Organic Synthesis," by T. W. Greene and P. G. M Wuts, Wiley, Second
Edition 1990, p. 219.
Example 56
##STR00228##
[0824] The preparation of phosphonates in which the phosphonate is
attached by means of an imino or iminoxy group and a variable
carbon chain is illustrated above. In this procedure, the
BMD-protected derivative, 55.2, is reacted with an amine or
hydroxylamine, 56.1, in which R.sup.2 is an alkyl, alkenyl,
cycloalkyl or cycloalkenyl group, optionally incorporating a
heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, to afford the imine or
iminoxy product, 56.2. The reaction is conducted between equimolar
amounts of the reactants in an aprotic solvent such as pyridine or
xylene, or in an alcoholic solvent such as ethanol, optionally in
the presence of an acid catalyst to give the imine or oxime. The
preparation of oximes of steroidal 3-ketones is described in Anal.
Bioch., 1978, 86, 133 and in J. Mass. Spectrom., 1995, 30, 497. The
BMD-protected side-chain compound, 56.2, is then converted into the
diester, 56.3.
Example 56A
##STR00229##
[0826] Also illustrated is the preparation of hydroxylamine ethers
incorporating a phosphonate group. A phosphonate, 56.4, in which Lv
is a leaving group such as bromo or trifluoromethylsulfonyloxy, is
reacted with BOC-hydroxylamine, 56.5 (Aldrich), to produce the
ether, 56.6. The reaction is conducted between equimolar amounts of
the reactants in a polar solvent such as dimethyl-formamide or
tetrahydrofuran, in the presence of a base such as potassium
hydroxide or dimethylaminopyridine, to give the product, 56.6.
Deprotection, for example by treatment with trifluoroacetic acid,
then gives the hydroxylamine ether, 56.7.
Example 56B
##STR00230##
[0828] The preparation of phosphonates in which the phosphonate is
attached by means of an iminoxy group is illustrated above. In this
procedure, the substrate, 55.2, is reacted with a dialkyl
phosphonomethyl hydroxylamine, 56.1, prepared as described above
from a dialkyl trifluoromethylsulfonyloxymethyl phosphonate
(Tetrahedron Lett., 1986, 27, 1477) and BOC-hydroxylamine, to
afford, after deprotection and side chain acylation, the oxime
ether, 56.2. The oxime forming reaction is performed at ambient
temperature in pyridine solution between equimolar amounts of the
reactants.
[0829] Using the above procedures, but employing, in place of the
oxime ether, 56.1, different oxime ethers, 56.7, the corresponding
products, 56.2 are obtained.
Example 57
##STR00231##
[0831] The preparation of phosphonates incorporating an iminoxy
group, by means of the reaction between the substrate, 55.2, and
O-2-(3-bromophenyl)-ethylhydroxylamine, 57.1, prepared as described
above from compound, 55.1, and 2-(3-bromophenyl)ethyl bromide,
respectively. The resultant oxime ether is converted, by
deprotection and side chain acylation, into the compound, 57.2,
which is then reacted, in the presence of a palladium catalyst,
with a dialkyl phosphite, 57.3, to afford the phosphonate, 57.4.
The preparation of arylphosphonates by means of a coupling reaction
between aryl bromides and dialkyl phosphites is described in J.
Med. Chem., 1992, 35, 1371. The reaction is performed in an inert
solvent such as toluene, in the presence of a base such as
triethylamine and a catalytic amount of
tetrakis(triphenylphosphine)-palladium(0).
##STR00232##
[0832] Alternatively, the bromo-substituted product, 57.2, is
coupled, in a palladium-catalyzed Heck reaction, with a dialkyl
vinyl phosphonate, 57.5 (Aldrich), to give the unsaturated
phosphonate, 57.6. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in "Advanced
Organic Chemistry," by F. A. Carey and R. J. Sundberg, Plenum,
2001, p. 503ff and in Acc. Chem. Res., 1979, 12, 146. The aryl
bromide and the olefin are coupled in a polar solvent such as
dimethylformiamide or dioxan, in the presence of a palladium(0)
catalyst such as tetrakis(triphenylphosphine)-palladium(0) or a
palladium(II) catalyst such as palladium(II) acetate, and
optionally in the presence of a base such as triethylamine or
potassium carbonate. Optionally, the styrenoid double bond present
in the product, 57.6, is reduced, for example by reaction with
diimide, to produce the saturated analog, 57.7. The reduction of
olefinic bonds is described in "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 6ff. The
transformation is effected by means of catalytic hydrogenation, for
example using a palladium on carbon catalyst and hydrogen or a
hydrogen donor, or by the use of diimide or diborane.
[0833] Using the above procedures, but employing, in place of the
bromophenyl reagent, 57.1, different bromo-substituted aryl or
heteroaryl alkoxy hydroxylamines, and/or different dialkyl alkenyl
phosphonates, the products analogous to the compounds, 57.4, 57.6
and 57.7 are obtained.
Example 58
##STR00233##
[0835] The preparation of phosphonates in which the phosphonate is
attached by means of an imino group is illustrated above. In this
procedure, the substrate, 55.2, is reacted with a dialkyl
3-aminophenyl phosphonate, 58.1 (J. Med. Chem., 1984, 27, 654), to
give, after deprotection and side chain acylation, the imine
product, 58.2. The reaction is conducted in a hydrocarbon solvent
such as toluene or xylene, at reflux temperature, in the presence
of a basic catalyst such as sodium methoxide, or an acid catalyst
such as p-toluenesulfonic acid, under azeotropic conditions, to
give the product, 58.2.
[0836] Using the above procedures, but employing, in place of the
3-aminophenyl phosphonate, 58.1, different amino-substituted aryl
or heteroaryl phosphonates, products analogous to 58.2 are
obtained.
[0837] An alternative method for the preparation of phosphonates,
58.3, where the phosphonate is attached by means of an oximino
group starts with the dienone, 55.2, is illustrated above. The
dienone is reacted with hydroxylamine to yield, after deprotection
and side chain acylation, the oxime, 58.3. The reaction of
steroidal 1,4-dien-3-ones with hydroxylamine is described in J.
Steroid Bioch., 1976, 7, 795; the reaction is performed between
equimolar amounts of the reactants in a polar organic solvent such
as pyridine or methanol, optionally in the presence of acetic acid
or sodium acetate. The oxime is then reacted with a dialkyl
3-hydroxyphenyl phosphonate, 58.4 (Epsilon), in a Mitsonobu
reaction, to yield the substituted oxime, 58.5. The preparation of
aromatic ethers and thioethers by means of the Mitsonobu reaction
is described, for example, in "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 448, and in
"Advanced Organic Chemistry," Part B, by F. A. Carey and R. J.
Sundberg, Plenum, 2001, p. 153-4 and in Org. React., 1992, 42, 335.
The phenol and the hydroxy or mercapto component are reacted
together in an aprotic solvent such as, for example,
tetrahydrofuran, in the presence of a dialkyl azodicarboxylate and
a triarylphosphine, to afford the ether or thioether products. The
procedure is also described in Org. React., 1992, 42, 335-656.
[0838] Using the above procedures, but employing, in place of the
phosphonate, 58.4, different dialkyl hydroxy-substituted aryl or
heteroaryl phosphonates, the products analogous to 58.5 are
obtained.
Example 59
##STR00234##
[0840] The preparation of the phosphonate esters in which the
phosphonate group is attached to the 1' or 2' position of the
pyrazole ring, by means of an aromatic or heteroaromatic group, a
heteroatom and a variable carbon chain is shown above. In this
procedure, Aclometasone dipropionate, 59A, is reduced to afford the
1,2-dihydro product, 59.1. The catalytic hydrogenation reaction is
effected by the use of tris(triphenylphosphine)rhodium (I)
chloride, for example as described in J. Med. Chem., 2001, 44, 602.
The product is then reacted with ethyl formate and a base such as
sodium hydride, in an inert solvent such as toluene or
dimethylformamide, as described in Australian Patent Application
275950409, to afford the 2-formyl product, 59.2. Optionally, the
substrate, 59A, is protected, for example, as described above in
Example 55, prior to the formylation reaction, as described in J.
Am. Chem. Soc., 1964, 86, 1520. The 2-formyl product is then
reacted with an aryl or heteroaryl hydrazine, 59.3, in which the
substituent X is either a phosphonate group or a group which is
subsequently transformed into a phosphonate-containing substituent.
For example, X is dialkylphosphono, bromo, hydroxy, amino, carboxyl
and the like. The reaction yields the isomeric 2'- and 1'-aryl
pyrazoles, 59.4 and 59.5. The ring-forming reaction is performed
between equimolar amounts of the reactants in an acidic solvent
such as acetic acid, as described in J. Am. Chem. Soc., 1964, 86,
1520. The pyrazoles, 59.4 and 59.5, are then transformed, for
example by the procedures described in Examples 60-65, respectively
into the phosphonates, 59.6 and 59.7.
Example 60
##STR00235##
[0842] The preparation of phosphonates in which the phosphonate is
attached by means of a phenyl group is illustrated above. In this
sequence, the ketoaldehyde, 59.2, is reacted, as described above,
with 3-bromophenylhydrazine, 60.1 (Fluka), to give the isomeric
pyrazole products, 60.2 and 60.3. The products are then reacted, as
described above, with a dialkyl phosphite HP(O)(OR.sup.1).sub.2 and
a palladium catalyst, to afford respectively the phosphonates, 60.4
and 60.5. Using the above procedures, but employing, in place of
3-bromophenyl hydrazine, different bromoaryl or bromoheteroaryl
hydrazines, 59.3, the corresponding products, 59.6 and 59.7 are
obtained.
Example 60A
##STR00236##
[0844] The preparation of phosphonates in which the phosphonate is
attached by means of an aromatic or heteroaromatic group and a
saturated or unsaturated alkyl chain is illustrated above. In this
procedure, the bromophenyl-substituted pyrazole, 60.2, is coupled
in a Heck reaction, as described above, with, for example a dialkyl
vinyl phosphonate, 60.6 (Aldrich), to give the unsaturated
phosphonate product, 60.7. Optionally, the product is reduced, as
described above, to give the saturated analog, 60.8. Application of
the above procedures to the isomeric bromophenyl pyrazole, 60.3,
affords the products isomeric with, 60.7 and 60.8.
[0845] Using the above procedures, but employing, in place of the
phosphonate, 60.6, different dialkyl alkenyl phosphonates, and/or
different bromoaryl or heteroaryl pyrazoles, 59.4 or 59.5
(X.dbd.Br), the products analogous to 60.7 and 60.8 are
obtained.
Example 61
##STR00237##
[0847] The preparation of phosphonates in which the phosphonate is
attached by means of an aryl or heteroaryl group and an alkoxy
chain is illustrated above. In this procedure, 4-aminophenol, 61.1,
is reacted in dimethylformamide solution at ambient temperature
with a dialkyl trifluoromethanesulfonyloxymethyl phosphonate, 61.2
(Tetrahedron Lett., 1986, 27, 1477), and potassium carbonate to
give the ether, 61.3. The product is then converted into the
corresponding hydrazine, 61.4, by means of a diazotization reaction
in aqueous ethanolic hydrochloric acid, followed by reduction of
the diazonium chloride with tin(II) chloride, as described in J.
Med. Chem., 2001, 44, 4031. The hydrazine is then reacted, as
described above, with the ketoaldehyde, 59.2, to form the isomeric
pyrazoles, 61.5 and 61.6.
[0848] Using the above procedures, but employing, in place of the
triflate, 61.2, different dialkylphosphono alkyl bromides or
triflates, and/or different aromatic or heteroaromatic
hydroxyamines, the products analogous to 61.5 and 61.6 are
obtained.
Example 62
##STR00238##
[0850] The preparation of phosphonates in which the phosphonate is
attached by means of a pyridyl group, a heteroatom, and a variable
carbon chain is shown herein. In this procedure,
3-amino-5-hydroxypyridine, 62.1, is converted, by reaction with
acetic anhydride, into the diacetyl analog, 62.2. The product is
then transformed by diazotization and reduction, as described
above, into the hydrazine, 62.3.
##STR00239##
[0851] The hydrazine, 62.3, is then reacted with the ketoaldehyde,
59.2, to give the isomeric pyrazoles, 62.4 and 62.5. The 2'-pyridyl
product, 62.4, is reacted in a Mitsonobu reaction, as described
above, with a dialkyl mercaptoethyl phosphonate, 62.6 (Zh. Obschei.
Khim., 1973, 43, 2364), to afford the thioether, 62.7. Application
of this procedure to the isomeric phenol, 62.5, affords the product
isomeric to, 62.7.
[0852] Alternatively, the isomeric phenol, 62.5, is reacted, in
dimethyl-formamide solution at ca. 80.degree., with one molar
equivalent of a dialkyl bromo-butenyl phosphonate, 62.8 (J. Med.
Chem., 1992, 35, 1371), and cesium carbonate, to prepare the
phosphonate, 62.9. Application of this procedure to the isomeric
phenol, 62.4, affords the product isomeric with, 62.9.
[0853] Using the above procedures, but employing, in place of the
thiol, 62.6, or the bromide, 62.8, different thiols, alcohols or
bromides, and/or different phenols, 59.4 or 59.5, in which X is OH,
the corresponding products analogous to 62.7 and 62.9 are
obtained.
Example 63
##STR00240##
[0855] The preparation of the phosphonate esters in which the
phosphonate group is attached by means of a variable carbon linkage
is illustrated above. In this procedure, the ketoaldehyde, 59.2, is
reacted with hydrazine, to afford the pyrazole derivative, 63.1.
The reaction of steroidal 2-formyl-3-ketones with hydrazine is
described in J. Am. Chem. Soc, 1964, 86, 1520. The reaction is
performed in acetic acid at ambient temperature. The resulting
pyrazole is then reacted with a dialkyl bromomethyl phosphonate,
63.2, in which R.sup.2 is as defined above, to produce the isomeric
2' and 1' alkylation products, 63.3 and 63.4, respectively. The
alkylation of substituted pyrazoles is described, for example, in
"Heterocyclic Chemistry," by T. L. Gilchrist, Longman, 1992, p.
309.
Example 64
##STR00241##
[0857] The pyrazole, 63.1, is reacted, in dimethylformamide
solution at ca. 90.degree., with a dialkyl bromopropyl phosphonate,
64.1 (Aldrich), and a base such as dimethylaminopyridine or lithium
hexamethyldisilazide, to yield the isomeric alkylation products,
64.2 and 64.3.
Example 65
[0858] Pyrazole, 63.1, is reacted, as described above, with a
dialkyl 4-bromomethyl benzyl phosphonate, 65.1 (Tet., 1998, 54,
9341), to give the products, 65.2 and 65.3.
##STR00242##
Example 66
[0859] The structures of Hydrocortisone, 66A (U.S. Pat. No.
2,602,769) and the phosphonate esters are shown below, in which the
substituent R.sup.1 is H, alkyl, alkenyl, aryl or aralkyl. These
compounds incorporate a phosphonate moiety (R.sup.1O).sub.2P(O)
connected to the nucleus by means of a variable linking group,
designated as "link" in the attached structures. A general
protection-deprotection sequence in which the steroid side-chain is
protected as a bis-methylenedioxy (BMD) moiety is shown below.
##STR00243##
[0860] Hydrocortisone, 66A, is reacted with paraformaldehyde and an
acid catalyst such as hydrochloric acid, as described "Protective
Groups in Organic Synthesis," by T. W. Greene and P. G. M. Wuts,
Wiley, Second Edition 1990, p. 223, to yield the BMD derivative,
66.1. The phosphonate moiety is then introduced, using the
procedures described below, to produce the phosphonate ester, 66.2.
The BMD moiety is then hydrolyzed, for example by treatment with
50% aqueous acetic acid, as described in "Protective Groups in
Organic Synthesis," by T. W. Greene and P. G. M. Wuts, Wiley,
Second Edition 1990, p. 223, to afford the triol, 66.3
Example 66A
##STR00244##
[0862] The BMD-protected derivative, 66.1, is reacted with an amine
or hydroxylamine, 66.4, in which R.sup.2 is an alkyl, alkenyl,
cycloalkyl or cycloalkenyl group, optionally incorporating a
heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the imine or oxime, 66.5. The preparation of
oximes of steroidal 3-ketones is described in Anal. Bioch., 1978,
86, 133 and in J. Mass. Spectrom., 1995, 30, 497. In cases in which
X is not dialkylphosphono, the substituent X is converted, using
the methods described below; into a phosphonate-containing
substituent; the BMD-protected side-chain is then removed to afford
the triol, 66.6.
Example 66B
##STR00245##
[0864] The preparation of hydroxylamine ethers incorporating a
phosphonate group is illustrated above. In this procedure, a
phosphonate, 66.7, in which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxylamine, 66.8
(Aldrich), to produce the ether, 66.9. The reaction is conducted
between equimolar amounts of the reactants in a polar solvent such
as dimethylformamide or tetrahydrofuran, in the presence of a base
such as potassium hydroxide or dimethylaminopyridine. Deprotection,
for example by treatment with trifluoroacetic acid, then gives the
hydroxylamine ether, 66.10.
Example 67
##STR00246##
[0866] The substrate, 66.1, is reacted with a dialkyl
phosphonomethyl hydroxyl-amine, 67.1, prepared as described above
from a dialkyl trifluoromethylsulfonyl-oxymethyl phosphonate
(Tetrahedron Lett., 1986, 27, 1477) and BOC-hydroxylamine, to
afford the oxime, 67.2, which is deprotected to afford the triol,
67.3. The oxime forming reaction is performed at ambient
temperature in ethanol-acetic acid solution between equimolar
amounts of the reactants. Using the above procedures, but
employing, in place of the hydroxylamine ether, 67.1, different
oxime ethers, 66.10, the corresponding products, 66.6 are
obtained.
Example 68
##STR00247##
[0868] The preparation of compounds in which the phosphonate group
is attached by means of a phenyl ethoxy group is illustrated above.
In this procedure, the enone, 66.1, is reacted, as described above,
with O-(3-bromo-phenyl)ethyl hydroxylamine, 68.1, prepared as
described above from 2-(3-bromophenyl)ethyl bromide (French Patent
FR 1,481,052), to give, after deprotection of the side-chain, the
oxime, 68.2. The product is then reacted, in the presence of a
palladium catalyst, with a dialkyl phosphite, 68.3, to afford the
phosphonate, 68.4. The preparation of arylphosphonates by means of
a coupling reaction between aryl bromides and dialkyl phosphites is
described in J. Med. Chem., 1992, 35, 1371. The reaction is
performed in an inert solvent such as toluene, in the presence of a
base, such as triethylamine, and a catalytic amount of
tetrakis(triphenylphosphine)palladium(0).
Example 68A
##STR00248##
[0870] Alternatively, the bromo compound, 68.2, is coupled with a
dialkyl vinylphosphonate, 68.5 (Aldrich), to afford the
phosphonate, 68.6. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in "Advanced
Organic Chemistry," by F. A. Carey and R. J. Sundberg, Plenum,
2001, p. 503ff and in Acc. Chem. Res., 1979, 12, 146. The aryl
bromide and the olefin are coupled in a polar solvent such as
dimethylformamide or dioxan, in the presence of a palladium(0)
catalyst such as tetrakis(triphenylphosphine)palladium(0) or
palladium(II) catalyst such as palladium(II) acetate, and
optionally in the presence of a base such as triethylamine or
potassium carbonate. Optionally, the styrenoid double bond present
in the product 68.6 is reduced, for example by reaction with
diimide, to produce the saturated analog, 68.7. The reduction of
olefinic bonds is described in "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 6ff. The
transformation is effected by means of catalytic hydrogenation, for
example using a palladium on carbon catalyst and hydrogen or a
hydrogen donor, or by the use of diimide or diborane.
[0871] Using the above procedures, but employing, in place of the
bromophenyl ethoxy reagent, 68.1, different bromo-substituted aryl
or heteroaryl alkoxy hydroxylamines, and/or different dialkyl
alkenyl phosphonates, the products analogous to the compounds,
68.4, 68.6 and 68.7 are obtained.
Example 69
##STR00249##
[0873] The enone, 66.1, is reacted with
O-(2-aminoethyl)hydroxylamine, 69.1, (Pol. J. Chem., 1981, 55,
1163) to yield the oxime, 69.2. The reaction of steroidal
1,4-dien-3-ones with substituted hydroxylamines is described in J.
Steroid Bioch., 1976, 7, 795. The reaction is performed between
equimolar amounts of the reactants in a polar organic solvent such
as pyridine or methanol, optionally in the presence of acetic acid
or sodium acetate. The oxime is then coupled with a dialkyl
4-carboxyphenyl phosphonate, 69.3 (Epsilon), to yield the amide
oxime, 69.4. The preparation of amides from carboxylic acids and
derivatives is described, for example, in Organic Functional Group
Preparations, by S. R. Sandler and W. Karo, Academic Press, 1968,
p. 274, and Comprehensive Organic Transformations, by R. C. Larock,
VCH, 1989, p. 972ff. The carboxylic acid is reacted with the amine
in the presence of an activating agent, such as, for example,
dicyclohexylcarbodiimide or diisopropylcarbodiimide, optionally in
the presence of, for example, hydroxybenztriazole,
N-hydroxysuccinimide or N-hydroxypyridone, in a non-protic solvent
such as, for example, pyridine, DMF or dichloromethane, to afford
the amide.
[0874] Alternatively, the carboxylic acid (e.g., dialkyl
4-carboxyphenyl phosphonate, 69.3) is first converted into an
activated derivative such as the acid chloride, anhydride, mixed
anhydride, imidazolide and the like, and then reacted with the
amine, in the presence of an organic base such as, for example,
pyridine, to afford the amide. The conversion of a carboxylic acid
into the corresponding acid chloride is effected by treatment of
the carboxylic acid with a reagent such as, for example, thionyl
chloride or oxalyl chloride in an inert organic solvent such as
dichloromethane, optionally in the presence of a catalytic amount
of dimethylformamide. The amide product, 69.4, is then converted,
as described herein, into the triol, 69.5.
[0875] Using the above procedures, but employing, in place of the
hydroxylamine, 69.1, different amino-substituted hydroxylamines,
and/or different carboxy-substituted phosphonates, the products
analogous to 69.5 are obtained.
Example 70
##STR00250##
[0877] The preparation of the phosphonate esters in which the
phosphonate group is attached to the 1' or 2' position of the
pyrazole ring, by means of a variable carbon chain is illustrated
above. In this procedure, the BMD-protected enone, 66.1, is reacted
with ethyl formate and a base such as sodium hydride, in an inert
solvent such as toluene or dimethylformamide, as described in J.
Am. Chem. Soc., 1964, 86, 1520, to afford the 2-formyl product,
70.1. This compound is then reacted with an alkyl, aralkyl, aryl or
heteroaryl hydrazine, 70.2, wherein R.sup.2 is alkyl, aralkyl,
aryl, or heteroaryl, and in which the substituent X is either a
phosphonate group or a group which is subsequently transformed into
a phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxyl and the like. The
reaction yields the isomeric 2'- and 1'-aryl pyrazoles, 70.3 and
70.4. The pyrazole-forming reaction is performed between equimolar
amounts of the reactants in an acidic solvent such as acetic acid,
as described in J. Am. Chem. Soc., 1964, 86, 1520. The pyrazoles,
70.3 and 70.4, are then transformed, for example, using procedures
described herein, via the BMD-protected intermediates, 70.5 and
70.6, into the phosphonates, 70.7 and 70.8.
Example 71
##STR00251## ##STR00252##
[0879] The preparation of phosphonates in which the phosphonate
moiety is attached by means of a phenyl ring and an amide linkage
is illustrated above. In this procedure, the ketoaldehyde, 70.1, is
reacted, with 3-carbomethoxyphenyl-hydrazine, 71.1 (Apin), to give
the pyrazoles, 71.2 and 71.3. The 2'-substituted isomer, 71.2, is
then reacted with one molar equivalent of lithium hydroxide in
aqueous dimethoxyethane, to produce the carboxylic acid, 71.4. The
acid is then coupled, as described above, with a dialkyl
aminomethyl phosphonate, 71.5, (Interchim) to give the amide, 71.6,
deprotection then affords the triol, 71.7. Alternatively, the
1'-substituted pyrazole, 71.3, is hydrolyzed, as described above,
to the carboxylic acid, 71.8. The product is then coupled with a
dialkyl 3-aminophenyl phosphonate, 71.9 (J. Med. Chem., 1984, 27,
654), to yield after deprotection the triol amide, 71.10.
[0880] Using the above procedures, but employing, in place of the
carbomethoxyphenyl hydrazine, 71.1, different
carbomethoxy-substituted aralkyl, aryl or heteroaryl alkoxy
hydrazines, and/or different dialkyl amino-substituted
phosphonates, the products analogous to the compounds, 71.7 and
71.10 are obtained.
Example 72
##STR00253## ##STR00254##
[0882] The preparation of the phosphonate esters in which the
phosphonate group is attached by means of a variable carbon linkage
is illustrated above. In this procedure, the ketoaldehyde, 70.1, is
reacted, as described above, with 4-bromophenyl hydrazine, 72.1 (J.
Organomet. Chem., 1999, 62, 581), to produce the pyrazoles, 72.2
and 73.3. The 1'-substituted isomer, 72.2, is coupled, as described
herein, in the presence of a palladium catalyst, with a dialkyl
butenyl phosphonate, 72.4 (Org. Lett., 2001, 3, 217), to give the
phosphonate, 72.5. The product is then deprotected to afford the
triol, 72.6. Optionally, the styrenoid double bond present in the
product, 72.6, is reduced, as described above, to produce the
saturated analog, 72.7.
[0883] Alternatively, the 2'-substituted pyrazole, 72.3, is
coupled, in the presence of a palladium catalyst, with a dialkyl
phosphite to prepare the phosphonate, 72.8, which is deprotected to
give the triol, 72.9. The preparation of arylphosphonates by means
of a coupling reaction between aryl bromides and dialkyl phosphites
is described in J. Med. Chem., 1992, 35, 1371. This reaction is
performed in an inert solvent such as toluene, in the presence of a
base such as triethylamine and
tetrakis(triphenylphosphine)-palladium(0).
[0884] Using the above procedures, but employing, in place of the
bromophenyl hydrazine, 72.1, different bromo-substituted aralkyl,
aryl or heteroaryl alkoxy hydrazines, and/or different dialkyl
alkenyl phosphonates, the products analogous to the compounds,
72.6, 72.7 and 72.9 are obtained.
Example 73
##STR00255##
[0886] The preparation of the phosphonate esters in which the
phosphonate group is attached by means of a variable carbon linkage
is illustrated above. In this procedure, the ketoaldehyde, 70.1, is
reacted with hydrazine, to afford the pyrazole derivative, 73.1.
The reaction of steroidal 2-formyl-3-ketones with hydrazine is
described in J. Am. Chem. Soc, 1964, 86, 1520. The reaction is
performed in ethanol at reflux temperature. The pyrazole product is
then reacted with a bromomethyl compound, 73.2, in which R.sup.2
and X are as defined above, to yield the alkylation products, 73.3
and 73.4. The alkylation of substituted pyrazoles is described, for
example, in "Heterocyclic Chemistry," by T. L. Gilchrist, Longman,
1992, p. 309.
[0887] The reaction is performed between equimolar amounts of the
substrates in a polar solvent such as dimethylformamide or
tetrahydrofuran, in the presence of a base such as
dimethylaminopyridine, lithium hexamethyldisilazide and the like.
The products, 73.3 and 73.4, are converted into the phosphonates,
73.5 and 73.6, except in cases where X is dialkylphosphono, using
the procedures described herein. Deprotection affords the triols,
73.7 and 73.8.
Example 74
##STR00256##
[0889] The pyrazole, 73.1, is reacted, as described above, with one
molar equivalent of a dialkyl 4-(bromomethyl)phenyl phosphonate,
74.1 (WO 2003/042150), to give the alkylated pyrazoles, 74.2 and
74.3. Deprotection then yields the triols, 74.4 and 74.5.
Example 75
##STR00257##
[0891] The pyrazole, 73.1, is reacted, as described above, with
2,5-bis(bromo-methyl)thiophene, 75.1 (Tet., 1999, 55, 4709), to
give the pyrazoles, 75.2 and 75.3. The products are subjected to an
Arbuzov reaction, in which the bromomethyl substituent is converted
into the dialkyl phosphonomethyl substituent, by reaction with a
trialkyl phosphite at 120.degree., to prepare, after deprotection
of the side chain, the phosphonates, 75.4 and 75.5. The Arbuzov
reaction is described in Handb. Organophosphorus Chem., 1992,
115-72. In the procedure, the substrate is heated at from
60.degree. to about 160.degree. with a five to fifty-fold molar
excess of the trialkyl phosphite.
[0892] Using the above procedures, but employing, in place of the
dibromide, 75.1, different dibromides, the products analogous to
75.4 and 75.5 are obtained.
Example 76
[0893] Dexamethasone, 76A, (U.S. Pat. No. 3,007,923) analogs where
the substituent R.sup.1 is H, alkyl, alkenyl, aryl or aralkyl are
prepared by the procedures below. The compounds 76.1-76.3
incorporate a phosphonate moiety (R.sup.1O).sub.2P(O) connected to
the nucleus by means of a variable linking group, designated as
"link" in the attached structures.
##STR00258##
[0894] Dexamethasone, 76A, is reacted with paraformaldehyde and an
acid catalyst such as hydrochloric acid, as described in
"Protective Groups in Organic Synthesis," by T. W. Greene and P. G.
M. Wuts, Wiley, Second Edition 1990, p. 223, to yield the BMD
derivative, 76.1. The phosphonate moiety is then introduced, using
the procedures described below, to produce the phosphonate ester,
76.2. The BMD moiety is then hydrolyzed, for example by treatment
with 50% aqueous acetic acid, as described in "Protective Groups in
Organic Synthesis," by T. W. Greene and P. G. M. Wuts, Wiley,
Second Edition 1990, p. 223, to afford the triol, 76.3.
Example 77
##STR00259##
[0896] The preparation of phosphonates in which the phosphonate is
attached by means of an imino or iminoxy group and a variable
carbon chain is illustrated above. In this procedure, the
BMD-protected derivative, 76.1, is reacted with an amine or
hydroxylamine, 77.1, in which R.sup.2 is an alkyl, alkenyl,
cycloalkyl or cycloalkenyl group, optionally incorporating a
heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the imine or oxime. The preparation of oximes of
steroidal 3-ketones is described in Anal. Bioch., 1978, 86, 133 and
in J. Mass. Spectrom., 1995, 30, 497. The BMD-protected side-chain
compound, 77.2, is then converted, as described in Scheme M1 in
Example 76, into the triol, 77.3.
Example 77A
##STR00260##
[0898] The preparation of hydroxylamine ethers incorporating a
phosphonate group is illustrated above. In this procedure, a
phosphonate, 77.4, in which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxylamine, 77.5
(Aldrich), to produce the ether, 77.6. The reaction is conducted
between equimolar amounts of the reactants in a polar solvent such
as dimethylformamide or tetrahydrofuran, in the presence of a base
such as potassium hydroxide or dimethylaminopyridine. Deprotection,
for example by treatment with trifluoroacetic acid, then gives the
hydroxylamine ether, 77.7.
Example 78
##STR00261##
[0900] The preparation of phosphonates in which the phosphonate is
attached by means of an iminoxy group. In this procedure, the
substrate, 76.1, is reacted with a dialkyl phosphonomethyl
hydroxylamine, 78.1, prepared as described above from a dialkyl
trifluoromethylsulfonyloxymethyl phosphonate (Tetrahedron Lett.,
1986, 27, 1477) and BOC-hydroxylamine, to afford the oxime, 78.2,
which is deprotected to afford the triol, 78.3. The oxime forming
reaction is performed at ambient temperature in ethanol-acetic acid
solution between equimolar amounts of the reactants.
[0901] Using the above procedures, but employing, in place of the
hydroxylamine ether, 78.1, different oxime ethers, 77.1, the
corresponding products, 77.3 are obtained.
Example 79
##STR00262##
[0903] The preparation of compounds in which the phosphonate group
is attached by means of a pyridyl methoxy group is illustrated
above. In this procedure, the dienone, 76.1, is reacted, as
described above, with O-(3-bromo-5-pyridylmethyl)hydroxylamine,
79.1, prepared as described above from
3-bromo-5-bromomethylpyridine (WO 95/28400), to give, after
deprotection of the side-chain, the oxime, 79.2. The product is
then reacted, in the presence of a palladium catalyst, with a
dialkyl phosphite, 79.3, to afford the phosphonate, 79.4. The
preparation of arylphosphonates by means of a coupling reaction
between aryl bromides and dialkyl phosphites is described in J.
Med. Chem., 1992, 35, 1371. The reaction is performed in an inert
solvent such as toluene, in the presence of a base such as
triethylamine and a catalytic amount of
tetrakis-(triphenylphosphine)palladium(0).
[0904] Alternatively, the bromo compound, 79.2, is coupled with a
dialkyl vinylphosphonate, 79.5 (Aldrich), to afford the
phosphonate, 79.6. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in "Advanced
Organic Chemistry," by F. A. Carey and R. J. Sundberg, Plenum,
2001, p. 503ff and in Acc. Chem. Res., 1979, 12, 146. The aryl
bromide and the olefin are coupled in a polar solvent such as
dimethylformamide or dioxan, in the presence of a palladium(0)
catalyst such as tetrakis(triphenyl-phosphine)palladium(0) or
palladium(II) catalyst such as palladium(II) acetate, and
optionally in the presence of a base such as triethylamine or
potassium carbonate. Optionally, the styrenoid double bond present
in the product, 79.6, is reduced, for example by reaction with
diimide, to produce the saturated analog, 79.7. The reduction of
olefinic bonds is described in "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 6ff. The
transformation is effected by means of catalytic hydrogenation, for
example using a palladium on carbon catalyst and hydrogen or a
hydrogen donor, or by the use of diimide or diborane.
[0905] Using the above procedures, but employing, in place of the
bromopyridyloxy reagent, 79.1, different bromo-substituted aryl or
heteroaryl alkoxy hydroxylamines, and/or different dialkyl alkenyl
phosphonates, the products analogous to the compounds, 79.4, 79.6
and 79.7 are obtained.
Example 80
##STR00263##
[0907] The preparation of phosphonates in which the phosphonate is
attached by means of an imino group is illustrated above. In this
procedure, the substrate, 76.1, is reacted with a dialkyl
2-aminophenyl phosphonate, 80.1, (Syn., 1999, 1368) to give, after
deprotection, the imine product, 80.2. The reaction is conducted in
a hydrocarbon solvent such as toluene or xylene, at reflux
temperature, in the presence of a basic catalyst such as sodium
methoxide, or an acid catalyst such as p-toluenesulfonic acid,
under azeotropic conditions. Using the above procedures, but
employing, in place of the 2-aminophenyl phosphonate, 80.1,
different amino-substituted aryl or heteroaryl phosphonates,
products analogous to 80.2 are obtained.
Example 81
##STR00264##
[0909] The preparation of phosphonates in which the phosphonate is
attached by means of an oximino group and an amide linkage is
illustrated above. In this procedure, the dienone, 76.2, is reacted
with O-(2-carboxyethyl)hydroxylamine, 81.1, (J. Med. Chem., 1990,
33, 1423) to yield the oxime, 81.2. The reaction of steroidal
1,4-dien-3-ones with substituted hydroxylamines is described in J.
Steroid Bioch., 1976, 7, 795; the reaction is performed between
equimolar amounts of the reactants in a polar organic solvent such
as pyridine or methanol, optionally in the presence of acetic acid
or sodium acetate. The oxime is then reacted with a dialkyl
methylaminomethyl phosphonate, 81.3, to yield the amide oxime,
81.4. The preparation of amides from carboxylic acids and
derivatives is described, for example, in "Organic Functional Group
Preparations," by S. R. Sandler and W. Karo, Academic Press, 1968,
p. 274, and "Comprehensive Organic Transformations," by R. C.
Larock, VCH, 1989, p. 972ff. The carboxylic acid is reacted with
the amine in the presence of an activating agent, such as, for
example, dicyclohexylcarbodiimide or diisopropylcarbodiimide,
optionally in the presence of, for example, hydroxybenztriazole,
N-hydroxysuccinimide or N-hydroxypyridone, in a non-protic solvent
such as, for example, pyridine, DMF or dichloromethane, to afford
the amide.
[0910] Alternatively, the carboxylic acid is first converted into
an activated derivative such as the acid chloride, anhydride, mixed
anhydride, imidazolide and the like, and then reacted with the
amine, in the presence of an organic base such as, for example,
pyridine, to afford the amide. The conversion of a carboxylic acid
into the corresponding acid chloride is effected by treatment of
the carboxylic acid with a reagent such as, for example, thionyl
chloride or oxalyl chloride in an inert organic solvent such as
dichloromethane, optionally in the presence of a catalytic amount
of dimethylformamide.
[0911] The amide product, 81.4, is then converted, as described
herein, into the triol, 81.5.
[0912] Using the above procedures, but employing, in place of the
hydroxylamine, 81.3, different carboxy-substituted hydroxylamines,
and/or different amino-substituted phosphonates, the products
analogous to 81.5 are obtained.
Example 82
##STR00265## ##STR00266##
[0914] The preparation of the phosphonate esters in which the
phosphonate group is attached to the 1' or 2' position of the
pyrazole ring, by means of an aromatic or heteroaromatic group, a
heteroatom and a variable carbon chain is illustrated above. In
this procedure, the BMD-protected dienone, 76.1, is reduced to
afford the 1,2-dihydro product, 82.1. The catalytic hydrogenation
reaction is effected by the use of tris(triphenylphosphine)rhodium
(I) chloride, for example as described in J. Med. Chem., 2001, 44,
602. The product is then reacted with ethyl formate and a base such
as sodium hydride, in an inert solvent such as toluene or
dimethylformamide, as described in J. Am. Chem. Soc., 1964, 86,
1520, to afford the 2-formyl product, 82.2. This compound is then
reacted with an alkyl, aralkyl, aryl or heteroaryl hydrazine, 82.3,
wherein R.sup.2 is alkyl, aralkyl, aryl or heteroaryl and in which
the substituent X is either a phosphonate group or a group which is
subsequently transformed into a phosphonate-containing substituent.
For example, X is dialkylphosphono, bromo, hydroxy, amino, carboxyl
and the like. The reaction yields the isomeric 2'- and 1'-aryl
pyrazoles, 82.4 and 82.5. The pyrazole-forming reaction is
performed between equimolar amounts of the reactants in an acidic
solvent such as acetic acid, as described in J. Am. Chem. Soc.,
1964, 86, 1520. The pyrazoles, 82.4 and 82.5, are then transformed,
for example by the procedures described herein, via the
BMD-protected intermediates, 82.6 and 82.7, into the phosphonates,
82.8 and 82.9.
Example 83
##STR00267## ##STR00268##
[0916] The preparation of phosphonates in which the phosphonate is
attached by means of a phenyl ring and an alkoxy or an acetylenic
linkage is illustrated above. In this procedure, the ketoaldehyde,
82.2, is reacted, as described above, with
3-hydroxyphenylhydrazine, 83.1 (Japanese Patent No. JP 03011081),
to give the pyrazoles, 83.2 and 83.3. The 2'-substituted isomer,
83.2, is then reacted in dichloromethane solution at ambient
temperature with one molar equivalent of trifluoromethylsulfonyl
chloride and dimethylaminopyridine, to yield the triflate, 83.4.
The product is then reacted in toluene solution with a dialkyl
propynyl phosphonate, 83.5 (Syn., 1999, 2027), triethylamine and a
catalytic amount of tetrakis(triphenylphosphine)palladium (0), to
give the acetylenic product, 83.6. The palladium-catalyzed coupling
reaction of aryl triflates with terminal acetylenes is described in
WO 02/30930. The BMD protecting group is then removed to yield the
triol, 83.7.
[0917] Alternatively, the 1'-substituted pyrazole, 83.3, is
reacted, in a Mitsonobu reaction, with a dialkyl 2-hydroxyethyl
phosphonate, 83.8 (Epsilon), to afford the ether, 83.9. The
preparation of aromatic ethers by means of the Mitsonobu reaction
is described, for example, in "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 448, and in
"Advanced Organic Chemistry," Part B, by F. A. Carey and R. J.
Sundberg, Plenum, 2001, p. 153-4 and in Org. React., 1992, 42, 335.
The phenol and the alcohol component are reacted together in an
aprotic solvent such as, for example, tetrahydrofuran, in the
presence of a dialkyl azodicarboxylate and a triarylphosphine, to
afford the ether or thioether products. The procedure is also
described in Org. React., 1992, 42, 335-656. The product, 83.9, is
then deprotected to give the triol, 83.10.
[0918] Using the above procedures, but employing different
acetylenic or hydroxyl-substituted phosphonates, the products
analogous to 83.7 and 83.10 are obtained. The functionalization
procedures are interchangeable between the pyrazole substrates,
83.2 and 83.3.
Example 84
##STR00269##
[0920] The preparation of the phosphonates in which the phosphonate
group is attached by means of a benzyl group and a saturated or
unsaturated carbon chain is illustrated above. In this procedure,
the ketoaldehyde, 82.2, is reacted, as described above, with
3-bromobenzyl hydrazine, 84.1 (U.S. Pat. No. 4,370,339), to produce
the pyrazoles, 84.2 and 84.3. The 1'-substituted isomer 84.2 is
coupled, in the presence of a palladium catalyst, with a dialkyl
vinylphosphonate, 84.4 (Aldrich), to give the phosphonate, 84.5.
The product is then deprotected to afford the triol, 84.6.
Optionally, the styrenoid double bond present in the product, 84.6,
is reduced, as described above, to produce the saturated analog,
84.7.
[0921] Alternatively, the 2'-substituted pyrazole, 84.3, is
coupled, in the presence of a palladium catalyst, with a dialkyl
phosphite to prepare the phosphonate, 84.8, which is deprotected to
give the triol, 84.9. The preparation of arylphosphonates by means
of a coupling reaction between aryl bromides and dialkyl phosphites
is described in J. Med. Chem., 1992, 35, 1371. This reaction is
performed in an inert solvent such as toluene, in the presence of a
base such as triethylamine and
tetrakis(triphenylphosphine)palladium(0).
[0922] Using the above procedures, but employing, in place of the
bromobenzyl reagent, 84.1, different bromo-substituted aralkyl,
aryl or heteroaryl alkoxy hydrazines, and/or different dialkyl
alkenyl phosphonates, the products analogous to the compounds,
84.6, 84.7 and 84.9 are obtained.
Example 85
##STR00270##
[0924] The preparation of the phosphonate esters, 85.7 and 85.8, in
which the phosphonate group is attached by means of a variable
carbon linkage is illustrated above. In this procedure, the
ketoaldehyde, 82.2, is reacted with hydrazine, to afford the
pyrazole derivative, 85.1. The reaction of steroidal
2-formyl-3-ketones with hydrazine is described in J. Am. Chem. Soc,
1964, 86, 1520. The reaction is performed in acetic acid at ambient
temperature. The pyrazole product is then reacted with a
bromomethyl compound, 85.2, in which R.sup.2 and X are as defined
above, to yield the alkylation products, 85.3 and 85.4. The
alkylation of substituted pyrazoles is described, for example, in
"Heterocyclic Chemistry," by T. L. Gilchrist, Longman, 1992, p.
309. The reaction is performed between equimolar amounts of the
substrates in a polar solvent such as dimethylformamide or
tetrahydrofuran, in the presence of a base such as
dimethylaminopyridine, lithium hexamethyldisilazide and the like.
The products, 85.3 and 85.4, are, except in cases where X is
dialkylphosphono, converted into the phosphonates, 85.5 and 85.6,
using the procedures described herein, and deprotection then
affords the triols, 85.7 and 85.8.
Example 86
##STR00271##
[0926] The pyrazole, 85.1, is reacted, as described above, with one
molar equivalent of a dialkyl bromoacetonyl phosphonate, 86.1
(Tet., 1978, 34, 649), to give the alkylated pyrazoles, 86.2 and
86.3. Deprotection then yields the triols, 86.4 and 86.5.
Example 87
##STR00272##
[0928] The pyrazole, 85.1, is reacted, as described above, with
1,4-bis(bromo-methyl)benzene, 87.1, to give the pyrazoles, 87.2 and
87.3. The products are subjected to an Arbuzov reaction, in which
the bromomethyl substituent is converted into the dialkyl
phosphonomethyl substituent, by reaction with a trialkyl phosphite
at 120.degree., to prepare, after deprotection of the side chain,
the phosphonates, 87.4 and 87.5. The Arbuzov reaction is described
in Handb. Organophosphorus Chem., 1992, 115-72. In the procedure,
the substrate is heated at from 60.degree. to about 160.degree.
with a five to fifty-fold molar excess of the trialkyl
phosphite.
[0929] Using the above procedures, but employing, in place of the
dibromide, 87.1, different dibromides, the products analogous to
87.4 and 87.5 are obtained.
Example 88
[0930] A synthetic methodology towards the preparation of
phosphonate compounds of Formulae 88.1 and 88.2 is described by
Westwood et al, J. Med. Chem., 1996, 39, 4608-4621, according to
the general routes outlined below.
##STR00273##
Example 89
[0931] The preparation of compounds of the invention having
phosphonate groups and intermediate compounds useful for their
synthesis are illustrated below.
##STR00274##
Example 90
[0932] The preparation of compounds of the invention having
phosphonate groups and intermediate compounds useful for their
synthesis are illustrated below.
##STR00275##
Example 91
##STR00276## ##STR00277##
[0934] The structures of Methylprednisolone suleptanate, 91A (WO
89/00558), and the phosphonate esters, 91.1-91.3, are shown above
in Example 91, in which the substituent R.sup.1 is H, alkyl,
alkenyl, aryl or aralkyl. The compounds, 91.1-91.3, incorporate a
phosphonate moiety (R.sup.1O).sub.2P(O) connected to the nucleus by
means of a variable linking group, designated as "link" in the
attached structures. The syntheses of the phosphonate compounds of
this invention, 91.1-91.3, and of the intermediate compounds
necessary for their synthesis are set forth below.
[0935] Methylprednisolone, 91.4, is reacted with paraformaldehyde
and an acid catalyst such as hydrochloric acid, as described in
"Protective Groups in Organic Synthesis," by T. W. Greene and P. G.
M. Wuts, Wiley, Second Edition 1990, p. 223, to yield the BMD
derivative, 91.5. The phosphonate moiety is then introduced, using
the procedures described herein, to produce the phosphonate ester,
91.6. The BMD moiety is then hydrolyzed, for example by treatment
with 50% aqueous acetic acid, as described in "Protective Groups in
Organic Synthesis," by T. W. Greene and P. G. M. Wuts, Wiley,
Second Edition 1990, p. 223, to afford the triol, 91.7. The triol
is then converted into the 21-suleptanate ester as described in WO
89/00558. In this procedure, a mixed anhydride prepared by reacting
suleptanic acid with pivaloyl chloride, in the presence of a base
such as triethylamine, is reacted with the 21-hydroxy steroid,
91.7, to prepare the 21-suleptanate ester, 91.8.
Example 92
##STR00278##
[0937] The preparation of phosphonates in which the phosphonate is
attached by means of an imino or iminoxy group and a variable
carbon chain is illustrated above. In this procedure, the
BMD-protected derivative, 91.5, is reacted with an amine or
hydroxylamine, 92.1, in which R.sup.2 is an alkyl, alkenyl,
cycloalkyl or cycloalkenyl group, optionally incorporating a
heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the imine or oxime. The preparation of oximes of
steroidal 3-ketones is described in Anal. Bioch., 1978, 86, 133 and
in J. Mass. Spectrom., 1995, 30, 497. The BMD-protected side-chain
compound, 92.2, is then converted into the triol, 92.3, and then to
the suleptanate, 92.4, as described above in Example 91.
Example 92A
##STR00279##
[0939] The preparation of hydroxylamine ethers incorporating a
phosphonate group is illustrated above. In this procedure, a
phosphonate, 92.5, in which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy. The phosphonate is reacted with
BOC-hydroxylamine, 92.6 (Aldrich), to produce the ether, 92.7. The
reaction is conducted between equimolar amounts of the reactants in
a polar solvent such as dimethylformamide or tetrahydrofuran, in
the presence of a base such as potassium hydroxide or
dimethylaminopyridine. Deprotection, for example by treatment with
trifluoroacetic acid, then gives the hydroxylamine ether, 92.8.
Example 93
##STR00280##
[0941] The preparation of phosphonates in which the phosphonate is
attached by means of an iminoxy group is illustrated above. In this
procedure, the substrate, 91.5, is reacted with a dialkyl
phosphonomethyl hydroxylamine, 93.1, prepared as described above
from a dialkyl trifluoromethylsulfonyloxymethyl phosphonate
(Tetrahedron Lett., 1986, 27, 1477) and BOC-hydroxylamine, to
afford the oxime, 93.4, which is deprotected to afford the triol,
93.5, from which the suleptanate ester, 93.6, is prepared. The
oxime forming reaction is performed at ambient temperature in
ethanol-acetic acid solution between equimolar amounts of the
reactants.
[0942] Using the above procedures, but employing, in place of the
hydroxylamine ether, 93.1, different oxime ethers, 92.1, the
corresponding products, 92.4 are obtained.
Example 94
##STR00281##
[0944] The preparation of compounds in which the phosphonate group
is attached by means of a phenoxyethoxy oxime group is illustrated
above. In this procedure, the dienone, 91.5, is reacted, as
described above, with O-(3-bromo-phenoxyethyl)hydroxylamine, 94.1,
prepared as described above from 3-bromophenoxyethyl bromide (FR
1,481,052) and BOC-protected hydroxyl-amine, to give, after
deprotection of the side-chain, the oxime, 94.2. The product is
then reacted, in the presence of a palladium catalyst, with a
dialkyl phosphite, 94.3, to afford the phosphonate, 94.4. The
preparation of arylphosphonates by means of a coupling reaction
between aryl bromides and dialkyl phosphites is described in J.
Med. Chem., 1992, 35, 1371. The reaction is performed in an inert
solvent such as toluene, in the presence of a base such as
triethylamine and a catalytic amount of
tetrakis(triphenylphosphine)palladium(0). The 21-hydroxy group is
then converted into the 21-suleptanate product, 94.5.
[0945] Alternatively, the bromo compound, 94.2, is coupled with a
dialkyl propenylphosphonate, 94.6 (Aldrich), to afford the
phosphonate, 94.7. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in "Advanced
Organic Chemistry," by F. A. Carey and R. J. Sundberg, Plenum,
2001, p. 503ff and in Acc. Chem. Res., 1979, 12, 146. The aryl
bromide and the olefin are coupled in a polar solvent such as
dimethylformamide or dioxan, in the presence of a palladium(0)
catalyst such as tetrakis(triphenylphosphine)palladium(0) or
palladium(II) catalyst such as palladium(II) acetate, and
optionally in the presence of a base such as triethylamine or
potassium carbonate. Optionally, the styrenoid double bond present
in the product, 94.7, is reduced, for example by reaction with
diimide, to produce the saturated analog, 94.9. The reduction of
olefinic bonds is described in "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 6ff. The
transformation is effected by means of catalytic hydrogenation, for
example using a palladium on carbon catalyst and hydrogen or a
hydrogen donor, or by the use of diimide or diborane. The products,
94.7 and 94.9, are then converted into the suleptanate esters, 94.8
and 94.10.
[0946] Using the above procedures, but employing, in place of the
bromo-phenoxyethoxy reagent, 94.1, different bromo-substituted aryl
or heteroaryl alkoxy hydroxylamines, and/or different dialkyl
alkenyl phosphonates, the products analogous to the compounds,
94.5, 94.8 and 94.10 are obtained.
Example 95
##STR00282##
[0948] The preparation of phosphonates in which the phosphonate is
attached by means of an imino group is illustrated above. In this
procedure, compound, 91.5, is reacted with a dialkyl 4-aminophenyl
phosphonate, 95.1 (Epsilon), to give, after deprotection, the imine
product, 95.2. The reaction is conducted in a hydrocarbon solvent
such as toluene or xylene, at reflux temperature, in the presence
of a basic catalyst such as sodium methoxide, or an acid catalyst
such as p-toluenesulfonic acid, under azeotropic conditions. The
product is then converted into the suleptanate ester, 95.3.
[0949] Using the above procedures, but employing, in place of the
4-aminophenyl phosphonate, 95.1, different amino-substituted aryl
or heteroaryl phosphonates, products analogous to 95.3 are
obtained.
Example 96
##STR00283##
[0951] The preparation of phosphonates in which the phosphonate is
attached by means of an oximino group and an amide linkage is
illustrated above. In this procedure, the dienone, 91.5, is reacted
with O-(4-aminobutyl)hydroxylamine, 96.1 (Pol. J. Chem., 1981, 55,
1163), to yield the oxime, 96.2. The reaction of steroidal
1,4-dien-3-ones with substituted hydroxylamines is described in J.
Steroid Bioch., 1976, 7, 795. The reaction is performed between
equimolar amounts of the reactants in a polar organic solvent such
as pyridine or methanol, optionally in the presence of acetic acid
or sodium acetate. The oxime is then coupled with a dialkyl
phosphonoacetic acid, 96.3 (Aldrich), to yield the amide oxime,
96.4. The preparation of amides from carboxylic acids and
derivatives is described, for example, in "Organic Functional Group
Preparations," by S. R. Sandler and W. Karo, Academic Press, 1968,
p. 274, and "Comprehensive Organic Transformations," by R. C.
Larock, VCH, 1989, p. 972ff. The carboxylic acid is reacted with
the amine in the presence of an activating agent, such as, for
example, dicyclohexylcarbodiimide or diisopropylcarbodiimide,
optionally in the presence of, for example, hydroxybenztriazole,
N-hydroxysuccinimide or N-hydroxypyridone, in a non-protic solvent
such as, for example, pyridine, DMF or dichloromethane, to afford
the amide.
[0952] Alternatively, the carboxylic acid is first converted into
an activated derivative such as the acid chloride, anhydride, mixed
anhydride, imidazolide and the like, and then reacted with the
amine, in the presence of an organic base such as, for example,
pyridine, to afford the amide. The conversion of a carboxylic acid
into the corresponding acid chloride is effected by treatment of
the carboxylic acid with a reagent such as, for example, thionyl
chloride or oxalyl chloride in an inert organic solvent such as
dichloromethane, optionally in the presence of a catalytic amount
of dimethylformamide.
[0953] The amide product, 96.4, is then converted, as described
herein, into the suleptanate, 96.6.
[0954] Using the above procedures, but employing, in place of the
hydroxylamine, 96.1, different amino-substituted hydroxylamines,
and/or different carboxy-substituted phosphonates, the products
analogous to 96.6 are obtained.
Example 97
##STR00284##
[0956] The preparation of the phosphonate esters in which the
phosphonate group is attached to the 1' or 2' position of the
pyrazole ring, by means of an aromatic or heteroaromatic group, a
heteroatom and a variable carbon chain is illustrated above. In
this procedure, the BMD-protected dienone, 91.5, is reduced to
afford the 1,2-dihydro product, 97.1. The catalytic hydrogenation
reaction is effected by the use of tris(triphenylphosphine)rhodium
(I) chloride, for example as described in J. Med. Chem., 2001, 44,
602. The product is then reacted with ethyl formate and a base such
as sodium hydride, in an inert solvent such as toluene or
dimethylformamide, as described in J. Am. Chem. Soc., 1964, 86,
1520, to afford the 2-formyl product, 97.2. This compound is then
reacted with an alkyl, aralkyl, aryl or heteroaryl hydrazine, 97.3,
wherein R.sup.2 is alkyl, aralkyl, aryl or heteroaryl and in which
the substituent X is either a phosphonate group or a group which is
subsequently transformed into a phosphonate-containing substituent.
For example, X is dialkylphosphono, bromo, hydroxy, amino, carboxyl
and the like. The reaction yields the isomeric 2'- and 1'-aryl
pyrazoles, 97.4 and 97.5. The pyrazole-forming reaction is
performed between equimolar amounts of the reactants in an acidic
solvent such as acetic acid, as described in J. Am. Chem. Soc.,
1964, 86, 1520. The pyrazoles, 97.4 and 97.5, are then transformed,
for example by the procedures described in Examples 98 and 99, via
the BMD-protected intermediates, 97.6 and 97.7, into the
phosphonate suleptanates, 97.9 and 97.11.
Example 98
##STR00285## ##STR00286##
[0958] The preparation of phosphonates in which the phosphonate is
attached by means of a phenyl ring and an alkoxy or an alkenyl
linkage is illustrated above. In this procedure, the ketoaldehyde,
97.2, is reacted, as described above, with
4-hydroxyphenylhydrazine, 98.1 (Epsilon), to give the pyrazoles,
98.2 and 98.3. The 2'-substituted isomer, 98.2, is then reacted in
dimethylformamide solution at ambient temperature with one molar
equivalent of 1,4-dibromobut-2-ene and dimethylaminopyridine, to
yield the bromoether, 98.4. The product is then reacted at
120.degree. in an Arbuzov reaction with a trialkyl phosphite, 98.5,
to give the phosphonate product, 98.6. The Arbuzov reaction, in
which an alkyl bromide is transformed into the corresponding
phosphonate, by heating at from 60.degree. to about 150.degree.
with a trialkyl phosphite, is described in Handb. Organophosphorus
Chem., 1992, 115-72. The BMD protecting group is then removed and
the product is acylated to yield the suleptanate ester triol,
98.8.
[0959] Alternatively, the 1'-substituted pyrazole, 98.3, is
reacted, in a Mitsonobu reaction, with a dialkyl 2-hydroxymethyl
phosphonate, 98.9 (Aldrich), to afford the ether, 98.10. The
preparation of aromatic ethers by means of the Mitsonobu reaction
is described, for example, in "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 448, and in
"Advanced Organic Chemistry," Part B, by F. A. Carey and R. J.
Sundberg, Plenum, 2001, p. 153-4 and in Org. React., 1992, 42, 335.
The phenol and the alcohol or thiol component are reacted together
in an aprotic solvent such as, for example, tetrahydrofuran, in the
presence of a dialkyl azodicarboxylate and a triaryl-phosphine, to
afford the ether or thioether products. The procedure is also
described in Org. React., 1992, 42, 335. The product, 98.10, is
then deprotected to give the triol, 98.11, and the latter compound
is acylated to afford the suleptanate, 98.12.
[0960] Using the above procedures, but employing different
dibromides or hydroxyl-substituted phosphonates, the products
analogous to 98.8 and 98.12 are obtained. The functionalization
procedures are interchangeable between the pyrazole substrates,
98.2 and 98.3.
Example 991
##STR00287##
[0962] The preparation of the phosphonates in which the phosphonate
group is attached by means of a phenyl ring or a phenyl ring and a
saturated or unsaturated carbon chain is illustrated above. In this
procedure, the keto-aldehyde, 97.2, is reacted, as described above,
with 4-bromophenyl hydrazine, 99.1 (J. Organomet. Chem., 1999, 62,
581), to produce the pyrazoles, 99.2 and 99.3. The 1'-substituted
isomer, 99.2, is coupled, in the presence of a palladium catalyst,
with a dialkyl vinylphosphonate, 99.4 (Aldrich), to give the
phosphonate, 99.4a. The product is then deprotected to afford the
triol, 99.5, which is converted into the suleptanate, 99.6.
Optionally, the styrenoid double bond present in the product, 99.6,
is reduced, as described above, to produce the saturated analog,
99.8.
[0963] Alternatively, the 2'-substituted pyrazole, 99.3, is
coupled, in the presence of a palladium catalyst, with a dialkyl
phosphite to prepare the phosphonate, 99.9, which is deprotected,
and the product is acylated to give the suleptanate ester, 99.11.
The preparation of arylphosphonates by means of a coupling reaction
between aryl bromides and dialkyl phosphites is described in J.
Med. Chem., 1992, 35, 1371. This reaction is performed in an inert
solvent such as toluene, in the presence of a base such as
triethylamine and tetrakis-(triphenylphosphine)palladium(0).
[0964] Using the above procedures, but employing, in place of the
bromophenyl hydrazine, 99.1, different bromo-substituted aralkyl,
aryl or heteroaryl alkoxy hydrazines, and/or different dialkyl
alkenyl phosphonates, the products analogous to the compounds,
99.6, 99.8 and 99.11 are obtained.
Example 100
##STR00288##
[0966] The preparation of the phosphonate esters in which the
phosphonate group is attached by means of a variable carbon linkage
is illustrated above. In this procedure, the ketoaldehyde, 97.2, is
reacted with hydrazine, to afford the pyrazole derivative, 100.1.
The reaction of steroidal 2-formyl-3-ketones with hydrazine is
described in J. Am. Chem. Soc, 1964, 86, 1520. The reaction is
performed in acetic acid at ambient temperature. The pyrazole
product is then reacted with a bromomethyl compound, 100.2, in
which R.sup.2 and X are as defined above, to yield the alkylation
products, 100.3 and 100.4. The alkylation of substituted pyrazoles
is described, for example, in "Heterocyclic Chemistry," by T. L.
Gilchrist, Longman, 1992, p. 309. The reaction is performed between
equimolar amounts of the substrates in a polar solvent such as
dimethylformamide or tetrahydrofuran, in the presence of a base
such as dimethylaminopyridine, lithium hexamethyldisilazide and the
like. The products, 100.3 and 100.4 are, except in cases where X is
dialkylphosphono, converted into the phosphonates, 100.1 and 100.6,
using the procedures described herein, and deprotection/acylation
then affords the suleptanate esters, 100.8 and 100.10.
Example 101
##STR00289##
[0968] The pyrazole, 100.1, is reacted in tetrahydrofuran solution,
as described above, with one molar equivalent of a dialkyl
bromobutyl phosphonate, 101.1, (Synthesis, 1994, 9, 909) and
lithium hexamethyldisilazide to give the alkylated pyrazoles, 101.2
and 101.3. Deprotection/acylation then yields the suleptanates,
101.5 and 101.7.
Example 102
##STR00290##
[0970] The pyrazole, 100.1, is reacted in tetrahydrofuran solution,
as described above, with 1,2-bis(bromomethyl)cyclopropane, 102.1
(Tet., 1997, 53, 10459), to give the pyrazoles, 102.2 and 102.3.
The products are subjected to an Arbuzov reaction, in which the
bromomethyl substituent is converted into the dialkyl
phosphonomethyl substituent, by reaction with a trialkyl phosphite
at 120.degree., to prepare, after deprotection of the side chain
and acylation, the suleptanate phosphonates, 102.5 and 102.7. The
Arbuzov reaction is described in Handb. Organophosphorus Chem.,
1992, 115-72. In the procedure, the substrate is heated at from
60.degree. to about 160.degree. with a five to fifty-fold molar
excess of the trialkyl phosphite.
[0971] Using the above procedures, but employing, in place of the
dibromide, 102.1, different dibromides, the products analogous to
102.5 and 102.7 are obtained.
Example 103
##STR00291##
[0973] The structures of Clobetasol, 103A (U.S. Pat. No.
3,721,687), and the phosphonate esters, 103.1-103.3, are shown
above. The compounds, 103.1-103.3, incorporate a phosphonate moiety
(R.sup.1O).sub.2P(O) connected to the nucleus by means of a
variable linking group, designated as "link" in the attached
structures.
##STR00292## ##STR00293##
[0974] A protection-deprotection sequence in which the steroid
side-chain is protected as a bis-methylenedioxy (BMD) moiety is
illustrated above. In this sequence,
9.alpha.-fluoro-16.beta.-methyl-11.beta.,17.alpha.,21-trihydroxypregn-1,4-
-dien-3,21-dione, 103.4 (U.S. Pat. No. 3,721,687), is reacted with
paraformaldehyde and an acid catalyst such as hydrochloric acid, as
described in "Protective Groups in Organic Synthesis," by T. W.
Greene and P. G. M. Wuts, Wiley, Second Edition 1990, p. 223, to
yield the BMD derivative, 103.5. The phosphonate moiety is then
introduced, using the procedures described below, to produce the
phosphonate ester, 103.6. The BMD moiety is then hydrolyzed, for
example by treatment with 50% aqueous acetic acid, as described in
"Protective Groups in Organic Synthesis," by T. W. Greene and P. G.
M. Wuts, Wiley, Second Edition 1990, p. 223, to afford the triol,
103.7. The 21-hydroxy group is then converted into the 21-chloro
group as described in U.S. Pat. No. 3,721,687, Chimia, 1992, 46,
338, or J. Med. Chem., 1987, 30, 1581. In this procedure, the
21-hydroxy substrate is reacted at about 0.degree. with one molar
equivalent of methanesulfonyl chloride in a basic solvent such as
pyridine, to afford the 21-mesylate, 103.8. The product is then
reacted, in dimethylformamide solution at about 70.degree., with
ca. five molar equivalents of lithium chloride, to yield the
21-chloro product, 103.9.
Example 104
##STR00294##
[0976] The preparation of phosphonates in which the phosphonate is
attached by means of an imino or iminoxy group and a variable
carbon chain is described herein. In this procedure, the
BMD-protected derivative, 103.1, is reacted with an amine or
hydroxylamine, 104.1, in which R.sup.2 is an alkyl, alkenyl,
cycloalkyl or cycloalkenyl group, optionally incorporating a
heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the imine or oxime. The preparation of oximes of
steroidal 3-ketones is described in Anal. Bioch., 1978, 86, 133 and
in J. Mass. Spectrom., 1995, 30, 497. The BMD-protected side-chain
compound, 104.2, is then converted into the triol, 104.3, and then
to the 21-chloro product, 104.4, as described herein.
Example 104A
##STR00295##
[0978] The preparation of hydroxylamine ethers incorporating a
phosphonate group is illustrated above. In this procedure, a
phosphonate, 104.5, in which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxylamine,
104.6 (Aldrich), to produce the ether, 104.7. The reaction is
conducted between equimolar amounts of the reactants in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as potassium hydroxide or
dimethylaminopyridine. Deprotection, for example by treatment with
trifluoroacetic acid, then gives the hydroxylamine ether,
104.8.
Example 105
##STR00296##
[0980] The preparation of phosphonates in which the phosphonate is
attached by means of an iminoxy group. In this procedure, the
substrate, 103.1, is reacted with a dialkyl phosphonomethyl
hydroxylamine, 105.1, prepared as described above from a dialkyl
trifluoromethylsulfonyloxymethyl phosphonate (Tetrahedron Lett.,
1986, 27, 1477) and BOC-hydroxylamine, to afford the oxime, 105.2.
Deprotection then affords the triol, 105.3, from which the
21-chloro compound, 105.4, is prepared. The oxime forming reaction
is performed at ambient temperature in ethanol-acetic acid solution
between equimolar amounts of the reactants. Using the above
procedures, but employing, in place of the hydroxylamine ether,
105.1, different oxime ethers, 104.1, the corresponding products,
105.4 are obtained.
Example 106
##STR00297##
[0982] The preparation of compounds in which the phosphonate group
is attached by means of a 3-pyridylmethoxy oxime group described
herein. In this procedure, the dienone, 103.1, is reacted, as
described above, with O-(5-bromo-3-pyridylmethoxy)hydroxylamine,
106.1, prepared as described above from
5-bromo-3-bromomethylpyridine (WO 95/28400) and BOC-protected
hydroxyl-amine, to give, after deprotection of the side-chain, the
oxime, 106.2. The product is then reacted, in the presence of a
palladium catalyst, with a dialkyl phosphite, 106.3, to afford the
phosphonate, 106.4. The preparation of arylphosphonates by means of
a coupling reaction between aryl bromides and dialkyl phosphites is
described in J. Med. Chem., 1992, 35, 1371. The reaction is
performed in an inert solvent such as toluene, in the presence of a
base such as triethylamine and a catalytic amount of
tetrakis(triphenylphosphine)-palladium(0). The 21-hydroxy group is
then converted into the 21-chloro derivative, 106.5.
[0983] Alternatively, the bromo compound, 106.2, is coupled with a
dialkyl 4-vinylphenyl phosphonate, 106.6 (Macromolecules, 1998, 31,
2918), to afford the phosphonate, 106.7. The coupling of aryl
halides with olefins by means of the Heck reaction is described,
for example, in "Advanced Organic Chemistry," by F. A. Carey and R.
J. Sundberg, Plenum, 2001, p. 503ff and in Acc. Chem. Res., 1979,
12, 146. The aryl bromide and the olefin are coupled in a polar
solvent such as dimethylformamide or dioxan, in the presence of a
palladium(0) catalyst such as
tetrakis(triphenylphosphine)palladium(0) or palladium(II) catalyst
such as palladium(II) acetate, and optionally in the presence of a
base such as triethylamine or potassium carbonate. Optionally, the
styrenoid double bond present in the product, 106.7, is reduced,
for example by reaction with diimide, to produce the saturated
analog, 106.9. The reduction of olefinic bonds is described in
"Comprehensive Organic Transformations," by R. C. Larock, VCH,
1989, p. 6ff. The transformation is effected by means of catalytic
hydrogenation, for example using a palladium on carbon catalyst and
hydrogen or a hydrogen donor, or by the use of diimide or diborane.
The products, 106.7 and 106.9, are then converted into the
21-chloro analogs, 106.8 and 106.10. Using the above procedures,
but employing, in place of the bromopyridyl-methoxy reagent, 106.1,
different bromo-substituted aryl or heteroaryl alkoxy
hydroxylamines, and/or different dialkyl alkenyl phosphonates, the
products analogous to the compounds, 106.5, 106.8 and 106.10 are
obtained.
Example 107
##STR00298##
[0985] The preparation of phosphonates in which the phosphonate is
attached by means of an imino group is illustrated above. In this
procedure, the substrate, 103.1, is reacted with a dialkyl
4-aminobenzyl phosphonate, 107.1, (Fluka) to give, after
deprotection, the imine product, 107.2. The reaction is conducted
in a hydrocarbon solvent such as toluene or xylene, at reflux
temperature, in the presence of a basic catalyst such as sodium
methoxide, or an acid catalyst such as p-toluenesulfonic acid,
under azeotropic conditions. The product is then converted into the
21-chloro compound, 107.3.
[0986] Using the above procedures, but employing, in place of the
4-aminobenzyl phosphonate, 107.1, different amino-substituted aryl
or heteroaryl phosphonates, products analogous to 107.3 are
obtained.
Example 108
##STR00299##
[0988] The preparation of phosphonates in which the phosphonate is
attached by means of an oximino group and a thioether linkage is
illustrated above. In this procedure, the dienone, 103.1, is
reacted with O-(2-mercaptoethyl)hydroxyl-amine, 108.1
(Bioorganicheskaya Khim., 1986, 12, 1662), to yield the oxime,
108.2. The reaction of steroidal 1,4-dien-3-ones with substituted
hydroxyl-amines is described in J. Steroid Bioch., 1976, 7, 795;
the reaction is performed between equimolar amounts of the
reactants in a polar organic solvent such as pyridine or methanol,
optionally in the presence of acetic acid or sodium acetate. The
product is then coupled, in a Mitsonobu reaction, with a dialkyl
3-hydroxy-phenyl phosphonate, 108.3 (Aurora), to yield the
thioether oxime, 108.4. The preparation of aromatic ethers by means
of the Mitsonobu reaction is described, for example, in
"Comprehensive Organic Transformations", by R. C. Larock, VCH,
1989, p. 448, and in "Advanced Organic Chemistry," Part B, by F. A.
Carey and R. J. Sundberg, Plenum, 2001, p. 153-4 and in Org.
React., 1992, 42, 335. The phenol and the alcohol or thiol
component are reacted together in an aprotic solvent such as, for
example, tetrahydrofuran, in the presence of a dialkyl
azodicarboxylate and a triarylphosphine, to afford the ether or
thioether products. The procedure is also described in Org. React.,
1992, 42, 335-656. The thioether product, 108.4, is then hydrolyzed
and converted into the 21-chloro product, 108.6, as described in
Example 103.
[0989] Using the above procedures, but employing, in place of the
hydroxyl-amine, 108.3, different hydroxy or mercapto-substituted
hydroxylamines, and/or different hydroxyaryl-substituted
phosphonates, the products analogous to 108.6 are obtained.
Example 109
##STR00300##
[0991] The preparation of the phosphonate esters in which the
phosphonate group is attached to the 1' or 2' position of the
pyrazole ring, by means of an aromatic or heteroaromatic group, a
heteroatom and a variable carbon chain is illustrated above. In
this procedure, the BMD-protected dienone, 103.5, is reduced to
afford the 1,2-dihydro product, 109.1. The catalytic hydrogenation
reaction is effected by the use of tris(triphenylphosphine)rhodium
(I) chloride, for example as described in J. Med. Chem., 2001, 44,
602. The product is then reacted with ethyl formate and a base such
as sodium hydride, in an inert solvent such as toluene or
dimethylformamide, as described in J. Am. Chem. Soc., 1964, 86,
1520, to afford the 2-formyl product, 109.2. This compound is then
reacted with an alkyl, aralkyl, aryl or heteroaryl hydrazine,
109.3, wherein R2 is alkyl, aralkyl, aryl or heteroaryl and in
which the substituent X is either a phosphonate group or a group
which is subsequently transformed into a phosphonate-containing
substituent. For example, X is dialkylphosphono, bromo, hydroxy,
amino, carboxyl and the like. The reaction yields the isomeric 2'-
and 1'-aryl pyrazoles, 109.4 and 109.5. The pyrazole-forming
reaction is performed between equimolar amounts of the reactants in
an acidic solvent such as acetic acid, as described in J. Am. Chem.
Soc., 1964, 86, 1520. The pyrazoles, 109.4 and 109.5, are then
transformed, for example by the procedures described in Examples
110 and 111, via the BMD-protected intermediates, 109.6 and 109.7,
into the 21-chloro phosphonates, 109.9 and 109.11.
Example 110
##STR00301##
[0993] The preparation of the phosphonate esters in which the
phosphonate group is attached to the 1' or 2' position of the
pyrazole ring, by means of a carbamate or an amino linkage is
illustrated above. In this procedure, the ketoaldehyde, 109.2, is
reacted, as described above, with 3-aminophenyl-hydrazine 110.1 (EP
437105) to give the pyrazoles 110.2 and 110.3. The 2'-substituted
isomer 110.2 is then reacted in dimethylformamide solution at
ambient temperature with one molar equivalent of a dialkyl
2-hydroxyethyl phosphonate, 110.4 (Epsilon), and carbonyl
diimidazole, to yield the carbamate, 110.5. The preparation of
carbamates is described in "Comprehensive Organic Functional Group
Transformations," A. R. Katritzky, ed., Pergamon, 1995, Vol. 6, p
416ff, and in "Organic Functional Group Preparations," by S. R.
Sandler and W. Karo, Academic Press, 1986, p. 260ff. In the
procedure, the amine is reacted in an inert aprotic solvent such as
dichloromethane or tetrahydrofuran, with phosgene or a functional
equivalent thereof, such as carbonyl diimidazole, triphosgene,
pentafluorophenyl carbonate and the like, to afford the
corresponding activated acylamine. The latter compound is then
reacted with an alcohol to yield the carbamate. The BMD protecting
group is then removed and the product is converted into the
21-chloro product, 110.7.
[0994] Alternatively, the 1'-substituted pyrazole, 110.3, is
reacted, in a reductive amination reaction, with a dialkyl
formylmethyl phosphonate, 110.8 (Zh. Obschei. Khim., 1987, 57,
2793), and sodium triacetoxyborohydride, to afford the amine,
110.9. The preparation of amines by means of reductive amination
procedures is described, for example, in "Comprehensive Organic
Transformations," by R. C. Larock, VCH, p 421, and in "Advanced
Organic Chemistry," Part B, by F. A. Carey and R. J. Sundberg,
Plenum, 2001, p 269. In this procedure, the amine component and the
aldehyde or ketone component are reacted together in the presence
of a reducing agent such as, for example, borane, sodium
cyanoborohydride, sodium triacetoxyborohydride or
diisobutylaluminum hydride, optionally in the presence of a Lewis
acid, such as titanium tetraisopropoxide, as described in J. Org.
Chem., 1990, 55, 2552. The product, 110.9, is then deprotected to
give the triol, 110.10, and the latter compound is transformed into
the 21-chloro analog, 110.11.
[0995] Using the above procedures, but employing different formyl
or hydroxyl-substituted phosphonates, and/or different
amino-substituted hydrazines, the products analogous to 110.7 and
110.11 are obtained. The functionalization procedures are
interchangeable between the pyrazole substrates, 110.2 and
110.3.
Example 111
##STR00302##
[0997] The preparation of the phosphonates in which the phosphonate
group is attached by means of a phenyl ring and an amide linkage is
illustrated above. In this procedure, the ketoaldehyde, 109.2, is
reacted, as described above, with 3-carboxyphenyl hydrazine, 111.1
(Apin), to produce the pyrazoles, 111.2 and 111.3. The
1'-substituted isomer, 111.1, is coupled, in the presence of
dicyclohexylcarbodiimide, with a dialkyl 3-aminophenyl phosphonate,
111.4 (Aurora), to give the amide, 111.5. The preparation of amides
from carboxylic acids and derivatives is described, for example, in
"Organic Functional Group Preparations," by S. R. Sandler and W.
Karo, Academic Press, 1968, p. 274, and "Comprehensive Organic
Transformations," by R. C. Larock, VCH, 1989, p. 972ff. The
carboxylic acid is reacted with the amine in the presence of an
activating agent, such as, for example, dicyclohexylcarbodiimide or
diisopropylcarbodiimide, optionally in the presence of, for
example, hydroxybenztriazole, N-hydroxysuccinimide or
N-hydroxypyridone, in a non-protic solvent such as, for example,
pyridine, DMF or dichloromethane, to afford the amide.
[0998] Alternatively, the carboxylic acid may first be converted
into an activated derivative such as the acid chloride, anhydride,
mixed anhydride, imidazolide and the like, and then reacted with
the amine, in the presence of an organic base such as, for example,
pyridine, to afford the amide.
[0999] The conversion of a carboxylic acid into the corresponding
acid chloride can be effected by treatment of the carboxylic acid
with a reagent such as, for example, thionyl chloride or oxalyl
chloride in an inert organic solvent such as dichloromethane,
optionally in the presence of a catalytic amount of
dimethylformamide.
[1000] The product is then deprotected to afford the triol, 111.6,
which is converted into the 21-chloro compound, 111.7.
[1001] Alternatively, the 2'-substituted pyrazole, 111.3, is
coupled, as described above, with a dialkyl methylaminomethyl
phosphonate, 111.8, to prepare the amide phosphonate 111.9 which is
deprotected, and the product is converted into the 21-chloro
analog, 111.11.
[1002] Using the above procedures, but employing, in place of the
carboxyphenyl hydrazine, 111.1, different carboxy-substituted
aralkyl, aryl or heteroaryl alkoxy hydrazines, and/or different
dialkyl amino-substituted phosphonates, the products analogous to
the compounds, 111.7 and 111.11 are obtained.
Example 112
##STR00303##
[1004] The preparation of the phosphonate esters in which the
phosphonate group is attached by means of a variable carbon linkage
is illustrated above. In this procedure, the ketoaldehyde, 109.2,
is reacted with hydrazine, to afford the pyrazole derivative,
112.1. The reaction of steroidal 2-formyl-3-ketones with hydrazine
is described in J. Am. Chem. Soc, 1964, 86, 1520. The reaction is
performed in acetic acid at ambient temperature. The pyrazole
product is then reacted with a bromomethyl compound, 112.2, in
which R.sup.2 and X are as defined above, to yield the alkylation
products, 112.3 and 112.4. The alkylation of substituted pyrazoles
is described, for example, in "Heterocyclic Chemistry," by T. L.
Gilchrist, Longman, 1992, p. 309. The reaction is performed between
equimolar amounts of the substrates in a polar solvent such as
dimethylformamide or tetrahydrofuran, in the presence of a base
such as dimethylaminopyridine, lithium hexamethyldisilazide and the
like. The products, 112.3 and 112.4, are, except in cases where X
is dialkylphosphono, converted into the phosphonates, 112.5 and
112.6, using the procedures described herein, and
deprotection/acylation then affords the 21-chloro compounds, 112.8
and 112.10.
Example 113
##STR00304##
[1006] The pyrazole, 112.1, is reacted in tetrahydrofuran solution,
as described above, with one molar equivalent of a dialkyl
bromobutenyl phosphonate, 113.1 (J. Med. Chem., 1992, 35, 1371),
and lithium hexamethyldisilazide to give the alkylated pyrazoles,
113.2 and 113.3. Deprotection followed by chlorination yields the
21-chloro products, 113.5 and 113.7.
Example 114
##STR00305##
[1008] The pyrazole, 112.1, is reacted in tetrahydrofuran solution,
as described above, with 1,4-dibromobut-2-yne, 114.1 (Aldrich), to
give the pyrazoles, 114.2 and 114.3. The products are subjected to
an Arbuzov reaction, in which the bromomethyl substituent is
converted into the dialkyl phosphonomethyl substituent, by reaction
with a trialkyl phosphite at 120.degree., to prepare, after
deprotection of the side chain and chlorination, the 21-chloro
phosphonates, 114.5 and 114.7. The Arbuzov reaction is described in
Handb. Organophosphorus Chem., 1992, 115-72. In the procedure, the
substrate is heated at from 60.degree. to about 160.degree. with a
five to fifty-fold molar excess of the trialkyl phosphite. Using
the above procedures, but employing, in place of the dibromide,
114.1, different dibromides, the products analogous to 114.5 and
114.7 are obtained.
Example 115
##STR00306##
[1010] The preparation of compounds of the invention having
phosphonate groups and intermediate compounds useful for their
synthesis are illustrated herein. A .beta.-ketonitrile, 115.2, is
generated from a phenylacetic acid, 115.1, by condensation with a
malononitrile ester under Claisen conditions. Reaction with
hydroxylamine provides the 5-amino-1,2-oxazole which, upon
condensation with cyanomorpholine provides the desired SMP-114
analogs.
Example 116
##STR00307##
[1012] The anisole derivative, 116.1, is demethylated by treatment
with a Lewis acid such as boron tribromide. The resulting phenol is
alkylated with E-1,4-dibromobutene and the resulting monobromide is
heated with triethylphosphite in a solvent such as toluene (or
other Arbuzov reaction conditions: see Engel, R., "Synthesis of
Carbon-phosphorus Bonds," CRC press, 1988) to generate the diethyl
ester of the desired phosphonic acid, 116.2. Saponification of the
carboxylate ester gives the phenylacetic acid ready for
incorporation into the synthesis of SMP-114 analogs.
Example 117
##STR00308##
[1014] The preparation of compounds of the invention having
phosphonate groups can be prepared the procedure of Example 116 and
substituting 1,3-dibromopropane in place of the
1,4-dibromobutene.
Example 118
##STR00309##
[1016] The free phenol in ethyl homovanillate, 118.1, is converted
to the aryl triflate, and the biphenyl motif is generated by Suzuki
coupling with phenyl-boronic acid (see Chem. Rev., 1995, 95, 2457).
The remaining steps are analogous to those described in Example
116.
Example 119
##STR00310##
[1018] Ethyl 4-bromophenylacetate, 119.1, is coupled with
4-methoxyphenyl-boronic acid using the Suzuki method (see above).
The remaining steps are analogous to those described in Example
116.
Example 120
##STR00311## ##STR00312##
[1020]
6.alpha.,9.alpha.-Difluoro-16.beta.-methyl-11.beta.,17.alpha.,21-tr-
ihydroxypregn-1,4-dien-3,21-dione, 120A, (U.S. Pat. No. 4,619,921)
is reacted with paraformaldehyde and an acid catalyst such as
hydrochloric acid, as described in "Protective Groups in Organic
Synthesis," by T. W. Greene and P. G. M. Wuts, Wiley, Second
Edition 1990, p. 223, to yield the BMD derivative, 120.1. The
phosphonate moiety is then introduced, using the procedures
described below, to produce the phosphonate ester 120.2. The BMD
moiety is then hydrolyzed, for example by treatment with 50%
aqueous acetic acid, as described in "Protective Groups in Organic
Synthesis," by T. W. Greene and P. G. M. Wuts, Wiley, Second
Edition 1990, p. 223, to afford the triol, 120.3. The latter
compound is then converted into the 17,21-cyclic orthoester, 120.4,
using the procedure described in Chem. Pharm. Bull., 1986, 34,
1613. The substrate is reacted in dimethylformamide at 70.degree.
C. with two molar equivalents of triethyl orthopropionate and a
catalytic amount of p-toluenesulfonic acid. The product is then
reacted with an excess of trimethylsilyl chloride in
dimethylformamide at ambient temperature to produce the 21-chloro
17-propionate product, 120.5.
[1021] Alternatively, the substrate, 120.3, is converted into the
product, 120.5, by means of the method described in J. Med. Chem.,
1987, 30: 1581. In this procedure, the 21-hydroxy group is
activated by conversion to the 21-mesylate, by reaction with mesyl
chloride in pyridine; the mesylate group is then displaced to yield
the 21-chloro intermediate, by reaction with lithium chloride in
dimethylformamide, and the 17-hydroxyl group is esterified to give
the 21-chloro-17-propionate derivative, 120.5. The selective
acylation of the 17.alpha. hydroxyl group in the presence of an
11.beta. hydroxyl group is described in J. Med. Chem., 1987, 30:
1581.
Example 121
##STR00313##
[1023] The BMD-protected derivative, 120.1, is reacted with an
amine or hydroxylamine, 121.1, in which R.sup.2 is an alkyl,
alkenyl, cycloalkyl or cycloalkenyl group, optionally incorporating
a heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the imine or oxime. The preparation of oximes of
steroidal 3-ketones is described in Anal. Bioch., 1978, 86, 133 and
in J. Mass. Spectrom., 1995, 30, 497. The BMD-protected side-chain
compound, 121.2, is then converted into the triol, 121.3, and then
to the 21-chloro 17 propionate product, 121.4, as described
above.
##STR00314##
[1024] The preparation of hydroxylamine ethers incorporating a
phosphonate group is illustrated above. A phosphonate, 121.5, in
which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxylamine,
121.6, (Aldrich) to produce the ether, 121.7. The reaction is
conducted between equimolar amounts of the reactants in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as potassium hydroxide or
dimethylaminopyridine. Deprotection, for example by treatment with
trifluoroacetic acid, then gives the hydroxylamine ether,
121.8.
Example 122
##STR00315##
[1026] The substrate, 120.1, is reacted with a dialkyl
phosphonomethyl hydroxylamine, 122.1, prepared as described above
from a dialkyl trifluoro-ethylsulfonyloxymethyl phosphonate (Tet.
Lett., 1986, 27:1477) and BOC-hydroxylamine, to afford the oxime,
122.2. Deprotection then affords the triol, 122.3, from which the
21-chloro 17-propionate compound, 122.4, is prepared. The oxime
forming reaction is performed at ambient temperature in
ethanol-acetic acid solution between equimolar amounts of the
reactants.
[1027] Using the above procedures, but employing, in place of the
hydroxylamine ether, 122.1, different oxime ethers, 121.1, the
corresponding products, 121.4 are obtained.
Example 123
##STR00316##
[1029] The dienone, 121.1, is reacted, as described above, with
O-(4-bromo-2-thienylmethoxy)hydroxylamine, 123.1, prepared as
described above from 4-bromo-2-bromomethylthiophene (WO 94/20456)
and BOC-protected hydroxylamine, to give, after deprotection of the
side-chain, the oxime, 123.2. The product is then reacted, in the
presence of a palladium catalyst, with a dialkyl phosphate, 123.3,
to afford the phosphonate, 123.4. The preparation of
arylphosphonates by means of a coupling reaction between aryl
bromides and dialkyl phosphites is described in J. Med. Chem. 1992,
35, 1371. The reaction is performed in an inert solvent such as
toluene, in the presence of a base such as triethylamine and a
catalytic amount of tetrakis(triphenylphosphine)-palladium(0). The
21-hydroxy compound, 123.4, is then converted, as described herein,
into the 21-chloro 17-propionate derivative, 123.5.
[1030] Alternatively, the bromo compound, 123.2, is coupled with a
dialkyl butenyl phosphonate, 123.6, (Org. Lett., 2001, 3, 217) to
afford the phosphonate, 123.7. The coupling of aryl halides with
olefins by means of the Heck reaction is described, for example, in
F. A. Carey and R. J. Sundberg, Advanced Organic Chemistry, 503ff
(Plenum, 2001) and in Acc. Chem. Res., 1979, 12, 146. The aryl
bromide and the olefin are coupled in a polar solvent such as
dimethylformamide or dioxan, in the presence of a palladium(0)
catalyst such as tetrakis(triphenylphosphine)palladium(0) or
palladium(II) catalyst such as palladium(II) acetate, and
optionally in the presence of a base such as triethylamine or
potassium carbonate. Optionally, the double bond present in the
product, 123.7, is reduced, for example by reaction with diimide,
to produce the saturated analog, 123.9. The reduction of olefinic
bonds is described in R. C. Larock, Comprehensive Organic
Transformations, 6ff (VCH 1989). The transformation is effected by
means of catalytic hydrogenation, for example using a palladium on
carbon catalyst and hydrogen or a hydrogen donor, or by the use of
diimide or diborane. The products, 123.7 and 123.9, are then
converted into the 21-chloro 17-propionate analogs, 123.8 and
123.10.
[1031] Using the above procedures, but employing, in place of the
bromothienylmethoxy reagent, 123.1, different bromo-substituted
aryl or heteroaryl alkoxy hydroxylamines, and/or different dialkyl
alkenyl phosphonates, the products analogous to the compounds,
123.5, 123.8 and 123.10 are obtained.
Example 124
##STR00317##
[1033] The substrate, 121.1, is reacted with a dialkyl
4-amino-2-thienyl phosphonate, 124.1, prepared by the
palladium-catalyzed coupling, as described above, between
4-amino-2-bromothiophene (Tet., 1987, 43, 3295) and a dialkyl
phosphite, to give, after deprotection, the imine product, 124.2.
The imine forming reaction is conducted in a hydrocarbon solvent
such as toluene or xylene, at reflux temperature, in the presence
of a basic catalyst such as sodium methoxide, or an acid catalyst
such as p-toluenesulfonic acid, under azeotropic conditions. The
product is then converted into the 21-chloro 17-propionate
compound, 124.3.
[1034] Using the above procedures, but employing, in place of the
4-aminothienyl phosphonate, 124.1 different amino-substituted aryl
or heteroaryl phosphonates, products analogous to 124.3 are
obtained.
Example 125
##STR00318##
[1036] The dienone, 121.1, is reacted with
O-(4-aminobutyl)hydroxylamine, 125.1, (Pol. J. Chem., 1981, 55,
1163) to yield the oxime, 125.2. The reaction of steroidal
1,4-dien-3-ones with substituted hydroxylamines is described in J.
Steroid Bioch., 1976, 7, 795; the reaction is performed between
equimolar amounts of the reactants in a polar organic solvent such
as pyridine or methanol, optionally in the presence of acetic acid
or sodium acetate. The product is then coupled with a dialkyl
2-hydroxyethyl phosphonate, 125.3, (Epsilon) and carbonyl
diimidazole, to yield the carbamate oxime, 125.4. The preparation
of carbamates is described in A. R. Katritzky, Comprehensive
Organic Functional Group Transformations, 6, 416ff (Pergamon,
1995), and in S. R. Sandler and W. Karo, Organic Functional Group
Preparations, 260ff (Academic Press, 1986). In the procedure, the
amine is reacted in an inert aprotic solvent such as
dichloromethane or tetrahydrofuran, with phosgene or a functional
equivalent thereof, such as carbonyl diimidazole, triphosgene,
pentafluorophenyl carbonate and the like, to afford the
corresponding activated acylamine. The latter compound is then
reacted with an alcohol to yield the carbamate. The carbamate
product, 125.4, is then converted, as described herein, into the
21-chloro 17-propionate product, 125.6.
[1037] Using the above procedures, but employing, in place of the
hydroxylamine, 125.3, different amino-substituted hydroxylamines,
and/or different hydroxy-substituted phosphonates, the products
analogous to 125.6 are obtained.
Example 126
##STR00319##
[1039] The BMD-protected dienone, 121.1, is reduced to afford the
1,2-dihydro product, 126.1. The catalytic hydrogenation reaction is
effected by the use of tris(triphenylphosphine)rhodium (I)
chloride, for example as described in J. Med. Chem., 2001, 44, 602.
The product is then reacted with ethyl formate and a base such as
sodium hydride, in an inert solvent such as toluene or
dimethylformamide, as described in J. Am. Chem. Soc., 1964, 86,
1520, to afford the 2-formyl product, 126.2. This compound is then
reacted with an alkyl, aralkyl, aryl or heteroaryl hydrazine,
126.3, in which the substituent X is either a phosphonate group or
a group which is subsequently transformed into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxyl and the like. The
reaction yields the isomeric 2'- and 1'-aryl pyrazoles, 126.4 and
126.5. The pyrazole-forming reaction is performed between equimolar
amounts of the reactants in an acidic solvent such as acetic acid,
as described in J. Am. Chem. Soc., 1964, 86, 1520. The pyrazoles,
126.4 and 126.5, are then transformed, for example by the
procedures described in Examples 122 and 123, via the BMD-protected
intermediates, 126.6 and 126.7, into the 21-chloro 17-propionate
phosphonates, 126.9 and 126.11.
Example 127
##STR00320##
[1041] The ketoaldehyde, 126.2, is reacted, as described above,
with 3-carboxypropyl hydrazine, 127.1, (Ind. J. Exp. Biol., 1994,
32, 218) to give the pyrazoles, 127.2 and 127.3. The 2'-substituted
isomer, 127.2, is then reacted in dimethylformamide solution at
ambient temperature with one molar equivalent of a dialkyl
4-aminophenyl phosphonate, 127.4, (Epsilon) and dicyclohexyl
carbodiimide, to yield the amide, 127.5. The preparation of amides
from carboxylic acids and derivatives is described, for example, in
S. R. Sandler and W. Karo, Organic Functional Group Preparations,
274 (Academic Press, 1968), and R. C. Larock, Comprehensive Organic
Transformations, 972ff (VCH, 1989). The carboxylic acid is reacted
with the amine in the presence of an activating agent, such as, for
example, dicyclohexylcarbodiimide or diisopropylcarbodiimide,
optionally in the presence of, for example, hydroxybenztriazole,
N-hydroxysuccinimide or N-hydroxypyridone, in a non-protic solvent
such as, for example, pyridine, DMF or dichloromethane, to afford
the amide.
[1042] Alternatively, the carboxylic acid may first be converted
into an activated derivative such as the acid chloride, anhydride,
mixed anhydride, imidazolide and the like, and then reacted with
the amine, in the presence of an organic base such as, for example,
pyridine, to afford the amide.
[1043] The conversion of a carboxylic acid into the corresponding
acid chloride can be effected by treatment of the carboxylic acid
with a reagent such as, for example, thionyl chloride or oxalyl
chloride in an inert organic solvent such as dichloromethane,
optionally in the presence of a catalytic amount of
dimethylformamide. The BMD protecting group is then removed and the
product is converted into the 21-chloro 17-propionate product,
127.7.
[1044] The 1'-substituted pyrazole, 127.3, is coupled, as described
above, with a dialkyl aminomethyl phosphonate, 127.8 (Interchim),
to afford the amide, 127.9. The product, 127.9, is then deprotected
to give the triol, 127.10, and the latter compound is transformed
into the 21-chloro 17-propionate, 127.11.
[1045] Using the above procedures, but employing different
amino-substituted phosphonates, and/or different
carboxy-substituted hydrazines, the products analogous to 127.7 and
127.11 are obtained. The functionalization procedures are
interchangeable between the pyrazole substrates, 127.2 and
127.3.
Example 128
##STR00321##
[1047] The ketoaldehyde, 126.2, is reacted, as described above,
with allyl hydrazine, 128.1, (Zh. Org. Khim., 1967, 3, 983) to
produce the pyrazoles, 128.2 and 128.3. The 1'-substituted isomer,
128.2, is coupled, as described herein, with a dialkyl
3-bromophenyl phosphonate, 128.4, (Epsilon) to give the
phosphonate, 128.5. The product is then deprotected to afford the
triol, 128.6, which is converted into the 21-chloro 17-propionate
compound, 128.7.
[1048] The 2'-substituted pyrazole, 128.3, is coupled, as described
above, with a dialkyl 5-bromo-2-thienyl phosphonate, 128.8, (Syn.,
2003, 455) to prepare the phosphonate, 128.9, which is deprotected,
and the product is converted into the 21-chloro 17-propionate
analog, 128.11.
[1049] Using the above procedures, but employing, in place of the
propenyl hydrazine, 128.1, different alkenyl hydrazines, and/or
different dialkyl bromo-substituted phosphonates, the products
analogous to the compounds, 128.7 and 128.11 are obtained.
Example 129
##STR00322##
[1051] The ketoaldehyde, 126.2, is reacted with hydrazine, to
afford the pyrazole derivative, 129.1. The reaction of steroidal
2-formyl-3-ketones with hydrazine is described in J. Am. Chem. Soc,
1964, 86, 1520. The reaction is performed in acetic acid at ambient
temperature. The pyrazole product is then reacted with a
bromomethyl compound, 129.2, in which R.sup.2 and X are as defined
above, to yield the alkylation products, 129.3 and 129.4. The
alkylation of substituted pyrazoles is described, for example, in
T. L. Gilchrist, Heterocyclic Chemistry, 309 (Longman, 1992). The
reaction is performed between equimolar amounts of the substrates
in a polar solvent such as dimethylformamide or tetrahydrofuran, in
the presence of a base such as dimethylaminopyridine, lithium
hexamethyldisilazide and the like. The products, 129.3 and 129.4,
are, except in cases where X is dialkylphosphono, converted into
the phosphonates, 129.5 and 129.6, using the procedures described
herein, and deprotection/chlorination/acylation then affords the
21-chloro 17-propionate compounds, 129.8 and 129.10.
Example 130
##STR00323##
[1053] Following the procedure described in Example 129, the
pyrazole, 129.1, is reacted with 2-bromobenzyl bromide, 130.1, to
give the pyrazoles, 130.2 and 130.3. The products are then coupled,
as described above, with a dialkyl phosphite, to afford, after
side-chain deprotection and modification, as described herein, the
21-chloro 17 propionates, 130.5 and 130.7.
Example 131
##STR00324##
[1055] Following the procedure described in Example 129, the
pyrazole, 129.1, is reacted in tetrahydrofuran solution with
4-bromomethyl cyclohexanone, 131.1, (WO 97/37959) to give the
alkylation products, 131.2 and 131.3. The 1'-substituted isomer,
131.2, is then reacted, in a reductive amination reaction, with a
dialkyl aminomethyl phosphonate, 131.8, (Interchim) and sodium
cyanoborohydride, to yield, after deprotection and side-chain
modification, the 21-chloro 17-propionate, 131.5.
[1056] The preparation of amines by means of reductive amination
procedures is described, for example, in R. C. Larock,
Comprehensive Organic Transformations, 421 (VCH, 1989), and in F.
A. Carey and R. J. Sundberg, Advanced Organic Chemistry, Part B,
269 (Plenum, 2001). In this procedure, the amine component and the
aldehyde or ketone component are reacted together in the presence
of a reducing agent such as, for example, borane, sodium
cyanoborohydride, sodium triacetoxyborohydride or
diisobutylaluminum hydride, optionally in the presence of a Lewis
acid, such as titanium tetraisopropoxide, as described in J. Org.
Chem., 1990, 55, 2552.
[1057] The 2'-substituted pyrazole, 131.3, is subjected to the same
series of reaction to give the amine phosphonate, 131.7.
[1058] Using the above procedures, but employing different
bromomethyl-substituted aldehydes or ketones, and/or different
amino-substituted phosphonates, the products analogous to 131.5 and
131.7 are obtained.
Example 132
##STR00325##
[1060] A protection-deprotection sequence in which the 20-ketone
group of Cliclesonide, 132A, (U.S. Pat. No. 5,482,934) is protected
to afford the derivative, 132.1. The ketone is protected, for
example, by conversion to the cyclic ethylene ketal, by reaction in
toluene solution at reflux temperature with ethylene glycol and an
acid catalyst, as described in J. Am. Chem. Soc., 1955, 77, 1904.
Deprotection is effected by reaction with pyridinium tosylate in
aqueous acetone, as described in J. Chem. Soc. Chem. Comm., 1987,
1351.
[1061] Alternatively, the 20-ketone is protected by conversion to
the N,N-dimethylhydrazone. The dimethyl hydrazone is prepared by
the reaction of the ketone, 132A, with N,N-dimethylhydrazine in
ethanol-acetic acid, as described in Org. Syn., 1970, 50, 102. The
group is removed by treatment with sodium acetate and acetic acid
in aqueous tetrahydrofuran, as described in J. Am. Chem. Soc.,
1979, 101, 5841.
[1062] Alternatively, the 20-ketone is protected as the
diethylamine adduct. In this procedure, the substrate, 132A, is
reacted with titanium tetrakis(diethylamide), as described in J.
Chem. Soc. Chem. Comm., 1983, 406, to afford the adduct. The ketone
is deprotected by reaction with water in an aqueous organic
solvent.
[1063] The protected compound, 132.1, is then converted into the
phosphonate-containing analog, 132.2, using the procedures
described below, and the protecting group is then removed, as
described above, to give the phosphonate, 132.3.
Example 133
##STR00326##
[1065] The protected derivative, 133.1, is reacted with an amine or
hydroxylamine, 133.2, in which R.sup.2 is an alkyl, alkenyl,
cycloalkyl or cycloalkenyl group, optionally incorporating a
heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the imine or oxime, 133.3. The preparation of
oximes of steroidal 3-ketones is described in Anal. Bioch., 1978,
86, 133 and in J. Mass. Spectrom., 1995, 30, 497. The protecting
group is then removed, as described herein, to afford the 20-keto
phosphonate product, 133.4.
Example 133A
##STR00327##
[1067] The preparation of hydroxylamine ethers incorporating a
phosphonate group is illustrated herein. In this procedure, a
phosphonate, 133.5, in which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxylamine,
133.6, (Aldrich) to produce the ether, 133.7. The reaction is
conducted between equimolar amounts of the reactants in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as potassium hydroxide or
dimethylaminopyridine. Deprotection, for example by treatment with
trifluoroacetic acid, then gives the hydroxylamine ether, 133.8.
The above procedure is also employed for the preparation of
substituted hydroxylamines which are precursors to
phosphonates.
Example 134
##STR00328##
[1069] The substrate, 133.1, in which the 20-ketone is protected as
the dimethyl hydrazone derivative, is reacted with a dialkyl
phosphonomethyl hydroxylamine, 133.8, prepared as described above
from a dialkyl trifluoromethylsulfonyl-oxymethyl phosphonate
(Tetrahedron Lett., 1986, 27, 1477) and BOC-hydroxylamine, to
afford the oxime, 134.2. Deprotection, as described in Example 132,
then affords the 20-keto phosphonate, 134.3. The oxime forming
reaction is performed at ambient temperature in ethanol-acetic acid
solution between equimolar amounts of the reactants.
[1070] Using the above procedures, but employing, in place of the
hydroxylamine ether, 133.8, different oxime ethers, 133.2, the
corresponding products, 133.4 are obtained.
Example 135
##STR00329##
[1072] The dienone, 133.1, in which the 20-ketone is protected as
the dimethyl hydrazone, is reacted, as described above, with
O-(4-bromobenzyloxy)-hydroxylamine, 135.1, prepared as described
above from 4-bromobenzyl bromide and BOC-protected hydroxylamine,
133.6, to give the oxime, 135.2. The protecting group is then
removed to yield the 20-keto product, 135.3. The latter product is
then reacted, in the presence of a palladium catalyst, with a
dialkyl phosphate, 135.4, to afford the phosphonate, 135.5. The
preparation of arylphosphonates by means of a coupling reaction
between aryl bromides and dialkyl phosphites is described in J.
Med. Chem., 1992, 35, 1371. The reaction is performed at ca.
100.degree. C. in an inert solvent such as toluene, in the presence
of a base such as triethylamine and a catalytic amount of
tetrakis(triphenyl-phosphine)palladium(0).
[1073] Alternatively, the bromo compound, 135.3, is coupled with a
dialkyl vinyl phosphonate, 135.6, (Aldrich) to afford the
phosphonate, 135.7. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in F. A.
Carey and R. J. Sundberg, Advanced Organic Chemistry 503ff (Plenum,
2001) and in Acc. Chem. Res., 1979, 12, 146. The aryl bromide and
the olefin are coupled in a polar solvent such as dimethylformamide
or dioxan, in the presence of a palladium(0) catalyst such as
tetrakis(triphenyl-phosphine)palladium(0) or palladium(II) catalyst
such as palladium(II) acetate, and optionally in the presence of a
base such as triethylamine or potassium carbonate. Optionally, the
styrenoid double bond present in the product, 135.7, is reduced,
for example by reaction with diimide, to produce the saturated
analog, 135.8. The reduction of olefinic bonds is described in R.
C. Larock, Comprehensive Organic Transformations 6ff (VCH 1989).
The transformation is effected by means of catalytic hydrogenation,
for example using a palladium on carbon catalyst and hydrogen or a
hydrogen donor, or by the use of diimide or diborane.
[1074] Using the above procedures, but employing, in place of the
bromobenzyl-oxy reagent, 135.1, different bromo-substituted aryl or
heteroaryl alkoxy hydroxylamines, and/or different dialkyl alkenyl
phosphonates, products analogous to the compounds, 135.5, 135.7 and
135.8 are obtained.
Example 136
##STR00330##
[1076] The substrate, 133.1, in which the 20-ketone is protected as
the dimethylhydrazone, is reacted with a dialkyl 4-amino-2-furyl
phosphonate, 136.1, prepared by the palladium catalyzed coupling
reaction, as described above, between 4-amino-2-bromofuran
(Tetrahedron Lett., 1987, 43, 3295) and a dialkyl phosphite, to
give, after deprotection, the imine product, 136.2. The imine
forming reaction is conducted in a hydrocarbon solvent such as
toluene or xylene, at reflux temperature, in the presence of a
basic catalyst such as sodium methoxide, or an acid catalyst such
as p-toluenesulfonic acid, under azeotropic conditions.
[1077] Using the above procedures, but employing, in place of the
4-amino-2-furyl phosphonate, 136.1, different amino-substituted
aryl or heteroaryl phosphonates, products analogous to 136.2 are
obtained.
Example 137
##STR00331##
[1079] The dienone, 133.1, in which the 20-ketone is protected as
the dimethyl-hydrazone, is reacted with
O-(2-carboxyethyl)hydroxylamine, 137.1, (J. Med. Chem., 1990, 33,
1423) to yield the oxime, 137.2. The reaction of steroidal
1,4-dien-3-ones with substituted hydroxylamines is described in J.
Steroid Bioch., 1976, 7, 795; the reaction is performed between
equimolar amounts of the reactants in a polar organic solvent such
as pyridine or methanol, optionally in the presence of acetic acid
or sodium acetate. The product, 137.2, is then coupled with a
dialkyl 4-aminophenyl phosphonate, 137.3, (Epsilon) and
dicyclohexylcarbodiimide, to yield, after deprotection the amide
oxime, 137.4. The preparation of amides from carboxylic acids and
derivatives is described, for example, in S. R. Sandler and W.
Karo, Organic Functional Group Preparations 274 (Academic Press,
1968) and R. C. Larock, Comprehensive Organic Transformations 972ff
(VCH, 1989). The carboxylic acid is reacted with the amine in the
presence of an activating agent, such as, for example,
dicyclohexyl-carbodiimide or diisopropylcarbodiimide, optionally in
the presence of, for example, hydroxybenztriazole,
N-hydroxysuccinimide or N-hydroxypyridone, in a non-protic solvent
such as, for example, pyridine, DMF or dichloromethane, to afford
the amide.
[1080] Alternatively, the carboxylic acid may first be converted
into an activated derivative such as the acid chloride, anhydride,
mixed anhydride, imidazolide and the like, and then reacted with
the amine, in the presence of an organic base such as, for example,
pyridine, to afford the amide.
[1081] The conversion of a carboxylic acid into the corresponding
acid chloride can be effected by treatment of the carboxylic acid
with a reagent such as, for example, thionyl chloride or oxalyl
chloride in an inert organic solvent such as dichloromethane,
optionally in the presence of a catalytic amount of
dimethylformamide.
[1082] Using the above procedures, but employing, in place of the
carboxy-substituted hydroxylamine, 137.1, different
carboxy-substituted hydroxylamines, and/or different
amino-substituted phosphonates, products analogous to 137.4 are
obtained.
Example 138
##STR00332##
[1084] The dienone, 132A, is reduced to afford the 1,2-dihydro
product, 138.1. The catalytic hydrogenation reaction is effected by
the use of tris(triphenyl-phosphine)rhodium (I) chloride, for
example as described in J. Med. Chem., 2001, 44, 602. The product
is then reacted with ethyl formate and a base such as sodium
hydride, in an inert solvent such as toluene or dimethylformamide,
as described in J. Am. Chem. Soc., 1964, 86, 1520, to afford the
2-formyl product, 138.2. This compound is then reacted with an
alkyl, aralkyl, aryl or heteroaryl hydrazine, 138.3, in which the
substituent X is either a phosphonate group or a group which is
subsequently transformed into a phosphonate-containing substituent.
For example, X is dialkylphosphono, bromo, hydroxy, amino, carboxyl
and the like. The reaction yields the isomeric 2'- and 1'-aryl
pyrazoles, 138.4 and 138.5. The pyrazole-forming reaction is
performed between equimolar amounts of the reactants in an acidic
solvent such as acetic acid, as described in J. Am. Chem. Soc.,
1964, 86, 1520. The pyrazoles, 138.4 and 13.5, are then
transformed, for example by the procedures described in Examples
139 and 140, into the phosphonates, 138.6 and 138.7.
Example 139
##STR00333##
[1086] The ketoaldehyde, 138.2, is reacted, as described above,
with 4-hydroxy-phenyl hydrazine, 139.1, (EP 437105) to give the
pyrazoles, 139.2 and 139.3. The 2'-substituted isomer, 139.2, is
then reacted in dimethylformamide solution at ca. 70.degree. C.
with a dialkyl bromobutenyl phosphonate, 139.4, (J. Med. Chem.,
1992, 35, 1371) and potassium carbonate, to yield the ether
phosphonate, 139.5.
[1087] The isomeric pyrazole, 139.3, is reacted, in a Mitsonobu
reaction, with a dialkyl mercaptomethyl phosphonate, 139.6, (J.
Med. Chem., 1985, 26, 1688) to yield the thioether phosphonate,
139.7. The preparation of aromatic ethers and thioethers by means
of the Mitsonobu reaction is described, for example, in R. C.
Larock, Comprehensive Organic Transformations 448 (VCH, 1989), in
F. A. Carey and R. J. Sundberg, Advanced Organic Chemistry, Part B
153-4 (Plenum, 2001), and in Org. React., 1992, 42, 335. The phenol
and the alcohol or thiol component are reacted together in an
aprotic solvent such as, for example, tetrahydrofuran, in the
presence of a dialkyl azodicarboxylate and a triarylphosphine, to
afford the ether or thioether products. The procedure is also
described in Org. React., 1992, 42, 335-656.
[1088] Using the above procedures, but employing different
hydroxy-substituted hydrazines, and/or different bromo- or
mercapto-substituted phosphonates, products analogous to 139.5 and
139.7 are obtained.
Example 140
##STR00334##
[1090] The ketoaldehyde, 138.2, is reacted, as described above,
with 4-aminophenyl hydrazine, 140.1, (Epsilon) to produce the
pyrazoles, 140.2 and 140.3. The 2'-substituted isomer, 140.2, is
coupled, as described above, with a dialkyl phosphonoacetic acid,
140.4, (Aldrich) and dicyclohexyl carbodiimide, to give the amide
phosphonate, 140.5.
[1091] Alternatively, the 1'-substituted pyrazole, 140.3, is
reacted with a dialkyl 3-hydroxypropyl phosphonate, 140.6, (Zh.
Obschei. Khim., 1973, 43, 2364), and carbonyl diimidazole to
prepare the carbamate phosphonate, 140.7. The preparation of
carbamates is described in Comprehensive Organic Functional Group
Transformations, Vol. 6, 416ff (A. R. Katritzky, ed., Pergamon,
1995) and in S. R. Sandler and W. Karo, Organic Functional Group
Preparations 260ff (Academic Press, 1986). In the procedure, the
amine is reacted in an inert aprotic solvent such as
dichloromethane or tetrahydrofuran, with phosgene or a functional
equivalent thereof, such as carbonyl diimidazole, triphosgene,
pentafluorophenyl carbonate and the like, to afford the
corresponding activated acylamine. The latter compound is then
reacted with an alcohol to yield the carbamate.
[1092] Using the above procedures, but employing, in place of the
4-amino-1-phenyl hydrazine, 140.1, different amino-substituted
hydrazines, and/or different dialkyl carboxy or hydroxy-substituted
phosphonates, products analogous to the compounds, 140.5 and 140.7
are obtained.
Example 141
##STR00335##
[1094] The ketoaldehyde, 138.2, is reacted with hydrazine, to
afford the pyrazole derivative, 141.1. The reaction of steroidal
2-formyl-3-ketones with hydrazine is described in J. Am. Chem.
Soc., 1964, 86, 1520. The reaction is performed in acetic acid at
ambient temperature. The pyrazole product is then reacted with a
bromomethyl compound, 141.2, in which R.sup.2 and X are as defined
above, or a reactive bromoheteroaromatic reagent, to yield the
alkylation products, 141.3 and 141.4. The alkylation of substituted
pyrazoles is described, for example, in T. L. Gilchrist,
Heterocyclic Chemistry 309 (Longman, 1992). The reaction is
performed between equimolar amounts of the substrates in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as dimethylaminopyridine, lithium
hexamethyldisilazide and the like. The products, 141.3 and 141.4,
are, except in cases where X is dialkyl-phosphono, converted into
the phosphonates, 141.5 and 141.6, using the procedures described
herein.
Example 142
##STR00336##
[1096] The pyrazole, 141.1, is reacted, as described above, with a
dialkyl acetonyl phosphonate, 142.1, (Tetrahedron Lett., 1978, 34,
649) to give the pyrazoles, 141.2 and 141.3.
Example 143
##STR00337##
[1098] The pyrazole, 141.1, is reacted in tetrahydrofuran solution,
with 2,5-bis(bromomethyl)thiophene, 143.1, (Tetrahedron Lett.,
1999, 55, 4709) and potassium hexamethyl disilazide, to give the
alkylation products, 143.2 and 143.3. The 2'-substituted isomer,
143.2, is then reacted, in a Arbuzov reaction, with a trialkyl
phosphite to yield the phosphonate, 143.4. The Arbuzov reaction is
described in Handb. Organophosphorus Chem., 1992, 115. In this
procedure, in which a bromo substituent is converted into the
corresponding phosphonate, the substrate is heated at from about
60.degree. C. to about 160.degree. C. with a five to fifty-fold
molar excess of a trialkyl phosphite, to effect the
transformation.
[1099] The 2'-substituted pyrazole, 143.3, is reacted at 70.degree.
C. in dimethylformamide solution with one molar equivalent of a
dialkyl 3-aminophenyl phosphonate, 143.5, and cesium carbonate, to
give the amine phosphonate, 143.6.
[1100] Using the above procedures, but employing different
dibromides, and/or different amino-substituted phosphonates,
products analogous to 143.4 and 143.6 are obtained.
Example 144
##STR00338##
[1102] A protection-deprotection sequence in which the 20-ketone
group of Deflazacort, 144A, (U.S. Pat. No. 3,436,389) is protected
to afford the derivative, 144.1, as shown. The ketone is protected,
for example, by conversion to the cyclic ethylene ketal, by
reaction in toluene solution at reflux temperature with ethylene
glycol and an acid catalyst, as described in J. Am. Chem. Soc.,
1955, 77, 1904. Deprotection is effected by reaction with
pyridinium tosylate in aqueous acetone, as described in J. Chem.
Soc. Chem. Comm., 1987, 1351.
[1103] Alternatively, the 20-ketone is protected by conversion to
the N,N-dimethylhydrazone. The dimethyl hydrazone is prepared by
the reaction of the ketone, 144A, with N,N-dimethylhydrazine in
ethanol-acetic acid, as described in Org. Syn., 1970, 50, 102. The
group is removed by treatment with sodium acetate and acetic acid
in aqueous tetrahydrofuran, as described in J. Am. Chem. Soc.,
1979, 101, 5841.
[1104] Alternatively, the 20-ketone is protected as the
diethylamine adduct. In this procedure, the substrate, 144A, is
reacted with titanium tetrakis(diethylamide), as described in J.
Chem. Soc. Chem. Comm., 1983, 406, to afford the adduct. The ketone
is deprotected by reaction with water in an aqueous organic
solvent.
[1105] The protected compound, 144.1, is then converted into the
phosphonate-containing analog, 144.2, using the procedures
described below, and the protecting group is then removed, as
described above, to give the phosphonate, 144.3.
Example 145
##STR00339##
[1107] The protected derivative, 145.1, is reacted with an amine or
hydroxylamine, 145.2, in which R.sup.2 is an alkyl, alkenyl,
cycloalkyl or cycloalkenyl group, optionally incorporating a
heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the imine or oxime, 145.3. The preparation of
oximes of steroidal 3-ketones is described in Anal. Bioch., 1978,
86, 133 and in J. Mass. Spectrom., 1995, 30, 497. The protecting
group is then removed, as described herein, to afford the 20-keto
phosphonate product, 145.4.
Example 145A
##STR00340##
[1109] The preparation of hydroxylamine ethers incorporating a
phosphonate group is illustrated herein. In this procedure, a
phosphonate, 145.5, in which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxylamine,
145.6, (Aldrich) to produce the ether, 145.7. The reaction is
conducted between equimolar amounts of the reactants in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as potassium hydroxide or
dimethylaminopyridine. Deprotection, for example by treatment with
trifluoroacetic acid, then gives the hydroxylamine ether, 145.8.
The above procedure is also employed for the preparation of
substituted hydroxylamines which are precursors to
phosphonates.
Example 146
##STR00341##
[1111] The substrate, 145.1, in which the 20-ketone is protected as
the dimethyl hydrazone derivative, is reacted with a dialkyl
phosphonomethyl hydroxylamine, 146.1, prepared as described above
from a dialkyl trifluoromethylsulfonyl-oxymethyl phosphonate
(Tetrahedron Lett., 1986, 27, 1477) and BOC-hydroxylamine, to
afford the oxime, 146.2. Deprotection, as described in Example 144,
then affords the 20-keto phosphonate, 146.3. The oxime forming
reaction is performed at ambient temperature in ethanol-acetic acid
solution between equimolar amounts of the reactants.
[1112] Using the above procedures, but employing, in place of the
hydroxylamine ether, 146.1, different oxime ethers, 145.2, the
corresponding products, 145.4 are obtained.
Example 147
##STR00342##
[1114] The dienone, 145.1, in which the 20-ketone is protected as
the dimethyl hydrazone, is reacted, as described above, with
O-(3-bromophenylethoxy)-hydroxylamine, 147.1, prepared as described
above from 3-bromophenylethyl bromide (French Patent FR 1481052),
and BOC-protected hydroxylamine, 145.6, to give the oxime, 147.2.
The protecting group is then removed to yield the 20-keto product,
147.3. The latter product is then reacted, in the presence of a
palladium catalyst, with a dialkyl phosphate, 147.4, to afford the
phosphonate, 147.5. The preparation of arylphosphonates by means of
a coupling reaction between aryl bromides and dialkyl phosphites is
described in J. Med. Chem., 1992, 35, 1371. The reaction is
performed at ca. 100.degree. C. in an inert solvent such as
toluene, in the presence of a base such as triethylamine and a
catalytic amount of tetrakis(triphenylphosphine)palladium(0).
[1115] Alternatively, the bromo compound, 147.3, is coupled with a
dialkyl propenyl phosphonate, 147.6, (Aldrich) to afford the
phosphonate, 147.7. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in F. A.
Carey and R. J. Sundberg, Advanced Organic Chemistry 503ff (Plenum,
2001) and in Acc. Chem. Res., 1979, 12, 146. The aryl bromide and
the olefin are coupled in a polar solvent such as dimethylformamide
or dioxan, in the presence of a palladium(0) catalyst such as
tetrakis(triphenyl-phosphine)palladium(0) or palladium(II) catalyst
such as palladium(II) acetate, and optionally in the presence of a
base such as triethylamine or potassium carbonate. Optionally, the
styrenoid double bond present in the product, 147.7, is reduced,
for example by reaction with diimide, to produce the saturated
analog, 147.8. The reduction of olefinic bonds is described in R.
C. Larock, Comprehensive Organic Transformations 6ff (VCH 1989).
The transformation is effected by means of catalytic hydrogenation,
for example using a palladium on carbon catalyst and hydrogen or a
hydrogen donor, or by the use of diimide or diborane.
[1116] Using the above procedures, but employing, in place of the
bromophenylethyl reagent, 147.1, different bromo-substituted aryl
or heteroaryl alkoxy hydroxylamines, and/or different dialkyl
alkenyl phosphonates, products analogous to the compounds, 147.5,
147.7 and 147.8 are obtained.
Example 148
##STR00343##
[1118] The substrate, 145.1, in which the 20-ketone is protected as
the dimethylhydrazone, is reacted with a dialkyl 3-aminophenyl
phosphonate, 148.1, (J. Med. Chem., 1984, 27, 654), to give, after
deprotection, the imine product, 148.2. The imine forming reaction
is conducted in a hydrocarbon solvent such as toluene or xylene, at
reflux temperature, in the presence of a basic catalyst such as
sodium methoxide, or an acid catalyst such as p-toluenesulfonic
acid, under azeotropic conditions.
[1119] Using the above procedures, but employing, in place of the
3-aminophenyl phosphonate, 148.1, different amino-substituted aryl
or heteroaryl phosphonates, products analogous to 148.2 are
obtained.
Example 149
##STR00344##
[1121] The dienone, 145.1, in which the 20-ketone is protected as
the dimethylhydrazone, is reacted with
O-(2-hydroxyethyl)hydroxylamine, 149.1, (J. Chem. Soc. Chem. Comm.,
1986, 903) to yield the oxime, 149.2. The reaction of steroidal
1,4-dien-3-ones with substituted hydroxylamines is described in J.
Steroid Bioch., 1976, 7, 795; the reaction is performed between
equimolar amounts of the reactants in a polar organic solvent such
as pyridine or methanol, optionally in the presence of acetic acid
or sodium acetate. The product, 149.2, is then coupled with a
dialkyl 4-aminophenyl phosphonate, 149.3, (Epsilon) and carbonyl
diimidazole, to yield, after deprotection, the carbamate oxime,
149.4. The preparation of carbamates is described in Comprehensive
Organic Functional Group Transformations, Vol. 6, 416ff (A. R.
Katritzky, ed., Pergamon, 1995) and in S. R. Sandler and W. Karo,
Organic Functional Group Preparations 260ff (Academic Press, 1986).
In the procedure, the amine is reacted in an inert aprotic solvent
such as dichloromethane or tetrahydrofuran, with phosgene or a
functional equivalent thereof, such as carbonyl diimidazole,
triphosgene, pentafluorophenyl carbonate and the like, to afford
the corresponding activated acylamine. The latter compound is then
reacted with an alcohol to yield the carbamate.
[1122] Using the above procedures, but employing, in place of the
hydroxy-substituted hydroxylamine, 149.1, different
hydroxy-substituted hydroxylamines, and/or different
amino-substituted phosphonates, the products analogous to 149.4 are
obtained.
Example 150
##STR00345##
[1124] The dienone, 144A, is reduced to afford the 1,2-dihydro
product, 150.1. The catalytic hydrogenation reaction is effected by
the use of tris(triphenyl-phosphine)rhodium (I) chloride, for
example, as described in J. Med. Chem., 2001, 44, 602. The product
is then reacted with ethyl formate and a base such as sodium
hydride, in an inert solvent such as toluene or dimethylformamide,
as described in J. Am. Chem. Soc., 1964, 86, 1520, to afford the
2-formyl product, 150.2. This compound is then reacted with an
alkyl, aralkyl, aryl or heteroaryl hydrazine, 150.3, in which the
substituent X is either a phosphonate group or a group which is
subsequently transformed into a phosphonate-containing substituent.
For example, X is dialkylphosphono, bromo, hydroxy, amino, carboxyl
and the like. The reaction yields the isomeric 2'- and 1'-aryl
pyrazoles, 150.4 and 150.5. The pyrazole-forming reaction is
performed between equimolar amounts of the reactants in an acidic
solvent such as acetic acid, as described in J. Am. Chem. Soc.,
1964, 86, 1520. The pyrazoles, 150.4 and 150.5, are then
transformed, for example by the procedures described herein, into
the phosphonates, 150.6 and 150.7.
Example 151
##STR00346##
[1126] The ketoaldehyde, 150.2, is reacted, as described above,
with 3-carboxyphenyl hydrazine, 151.1, (Apin) to give the
pyrazoles, 151.2 and 151.3. The 2'-substituted isomer, 151.2, is
then coupled in dimethylformamide solution at ambient temperature
with a dialkyl 3-aminopropyl phosphonate, 151.4, (Acros) and
dicyclohexyl carbodiimide, to yield the amide phosphonate, 151.5.
The preparation of amides from carboxylic acids and derivatives is
described, for example, in S. R. Sandler and W. Karo, Organic
Functional Group Preparations 274 (Academic Press, 1986), and R. C.
Larock, Comprehensive Organic Transformations 972ff (VCH, 1989).
The carboxylic acid is reacted with the amine in the presence of an
activating agent, such as, for example, dicyclohexyl-carbodiimide
or diisopropylcarbodiimide, optionally in the presence of, for
example, hydroxybenztriazole, N-hydroxysuccinimide or
N-hydroxypyridone, in a non-protic solvent such as, for example,
pyridine, DMF or dichloromethane, to afford the amide.
[1127] Alternatively, the carboxylic acid may first be converted
into an activated derivative such as the acid chloride, anhydride,
mixed anhydride, imidazolide and the like, and then reacted with
the amine, in the presence of an organic base such as, for example,
pyridine, to afford the amide.
[1128] The conversion of a carboxylic acid into the corresponding
acid chloride can be effected by treatment of the carboxylic acid
with a reagent such as, for example, thionyl chloride or oxalyl
chloride in an inert organic solvent such as dichloromethane,
optionally in the presence of a catalytic amount of
dimethylformamide.
[1129] The isomeric pyrazole, 151.3, is reacted, as described
above, with a dialkyl 2-aminophenyl phosphonate, 151.6, (Acros) to
yield the amide phosphonate, 151.7.
[1130] Using the above procedures, but employing different
carboxy-substituted hydrazines, and/or different amino-substituted
phosphonates, the products analogous to 151.5 and 151.7 are
obtained.
Example 152
##STR00347##
[1132] The ketoaldehyde, 150.2, is reacted, as described above,
with 1,3-bis(hydrazino)benzene, 152.1, (Bull. Soc. Chim. Fr., 1975,
1371) to produce the pyrazoles, 152.2 and 152.3. The 2'-substituted
isomer, 152.2, is reacted in tetrahydrofuran solution at ambient
temperature with one molar equivalent of a dialkylphosphono
acetaldehyde (Aurora), to give the hydrazone phosphonate,
152.5.
[1133] Alternatively, the 1'-substituted pyrazole, 152.3, is
coupled, as described above, with a dialkylphosphono butyric acid,
152.6, (Epsilon) and dicyclohexyl carbodiimide to prepare the
phosphonate, 152.7.
[1134] Using the above procedures, but employing, in place of the
1,3-bis(hydrazino)phenyl hydrazine, 152.1, different bis
hydrazines, and/or different dialkyl formyl or carboxy-substituted
phosphonates, the products analogous to the compounds, 152.5 and
152.7 are obtained.
Example 153
##STR00348##
[1136] The ketoaldehyde, 150.2, is reacted with hydrazine to afford
the pyrazole derivative, 153.1. The reaction of steroidal
2-formyl-3-ketones with hydrazine is described in J. Am. Chem.
Soc., 1964, 86, 1520. The reaction is performed in acetic acid at
ambient temperature. The pyrazole product is then reacted with a
bromomethyl compound 153.2, in which R.sup.2 and X are as defined
above, or a reactive bromoheteroaromatic reagent, to yield the
alkylation products, 153.3 and 153.4. The alkylation of substituted
pyrazoles is described, for example, in T. L. Gilchrist,
Heterocyclic Chemistry 309 (Longman, 1992). The reaction is
performed between equimolar amounts of the substrates in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as dimethylaminopyridine, lithium
hexamethyldisilazide and the like. The products, 153.3 and 153.4,
are, except in cases where X is dialkylphosphono, converted into
the phosphonates, 153.5 and 153.6, using the procedures described
herein.
Example 154
##STR00349##
[1138] The pyrazole, 153.1, is reacted in dimethylformamide
solution at 70.degree. C. with one molar equivalent of a dialkyl
bromopropyl phosphonate, 154.1, (Synthelec) and cesium carbonate,
to give the pyrazoles, 154.2 and 154.3.
Example 155
##STR00350##
[1140] The pyrazole, 153.1, is reacted in tetrahydrofuran solution
with 1,4-bis(bromomethyl)benzene, 155.1, and potassium hexamethyl
disilazide, to give the alkylation products, 155.2 and 155.3. The
2'-substituted isomer, 155.2, is then reacted, in an Arbuzov
reaction, with a trialkyl phosphite to yield the phosphonate,
155.4. The Arbuzov reaction is described in Handb. Organophosphorus
Chem., 1992, 115. In this procedure, in which a bromo substituent
is converted into the corresponding phosphonate, the substrate is
heated at from about 60.degree. C. to about 160.degree. C. with a
five to fifty-fold molar excess of a trialkyl phosphite, to effect
the transformation.
[1141] The 2'-substituted-pyrazole, 155.3, is reacted at 70.degree.
C. in dimethyl-formamide solution with one molar equivalent of a
dialkyl mercaptoethyl phosphonate, 155.5, (Zh. Obschei. Khim.,
1973, 43, 2364) and cesium carbonate, to give the thioether
phosphonate, 155.6.
[1142] Using the above procedures, but employing different
dibromides, and/or different mercapto-substituted phosphonates,
products analogous to 155.4 and 155.6 are obtained.
Example 156
##STR00351##
[1144] Medroxyprogesterone, 156A, (U.S. Pat. Nos. 3,043,832,
3,061,616, and 3,377,364) is protected to afford the derivative,
156.1. The ketone is protected, for example, by conversion to the
cyclic ethylene ketal, by reaction in toluene solution at reflux
temperature with ethylene glycol and an acid catalyst, as described
in J. Am. Chem. Soc., 1955, 77, 1904. Deprotection is effected by
reaction with pyridinium tosylate in aqueous acetone, as described
in as described in J. Chem. Soc. Chem. Comm., 1987, 1351.
[1145] Alternatively, the 20-ketone is protected by conversion to
the N,N-dimethylhydrazone. The dimethyl hydrazone is prepared by
the reaction of the ketone, 156A, with N,N-dimethylhydrazine in
ethanol-acetic acid, as described in Org. Syn., 1970, 50, 102. The
group is removed by treatment with sodium acetate and acetic acid
in aqueous tetrahydrofuran, as described in J. Am. Chem. Soc.,
1979, 101, 5841.
[1146] Alternatively, the 20-ketone is protected as the
diethylamine adduct. In this procedure, the substrate, 156A, is
reacted with titanium tetrakis(diethylamide), as described in J.
Chem. Soc. Chem. Comm., 1983, 406, to afford the adduct. The ketone
is deprotected by reaction with water in an aqueous organic
solvent.
[1147] The protected compound, 156.1, is then converted into the
phosphonate-containing analog, 156.2, using the procedures
described below, and the protecting group or groups are then
removed, as described above, to give the phosphonate, 156.3.
Example 157
##STR00352##
[1149] The ketone-protected derivative, 156.1, is reacted with a
hydroxylamine or amine, 157.1, in which R.sup.2 is an alkyl,
alkenyl, cycloalkyl or cycloalkenyl group, optionally incorporating
a heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone, etc., or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the oxime, 157.2. The preparation of oximes of
steroidal 3-ketones is described in Anal. Bioch. 1978, 86, 133 and
in J. Mass. Spectrom. 1995, 30, 497. The protecting group is then
removed, as described in Example 156, to afford the 20-keto
phosphonate product, 157.3.
Example 157A
##STR00353##
[1151] The preparation of hydroxylamine ethers incorporating a
phosphonate group is illustrated herein. A phosphonate, 157.4, in
which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxyl-amine,
157.5, (Aldrich) to produce the ether, 157.6. The reaction is
conducted between equimolar amounts of the reactants in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as potassium hydroxide or
dimethylaminopyridine. Deprotection, for example by treatment with
trifluoroacetic acid, then gives the hydroxylamine ether, 157.7.
The above procedure is also employed for the preparation of
substituted hydroxylamines which are precursors to
phosphonates.
Example 158
##STR00354##
[1153] The preparation of phosphonates, in which the phosphonate is
attached by means of an iminoxy group is illustrated herein. In
this procedure, the substrate, 156.1, in which the 20-ketone is
protected as the dimethyl hydrazone derivative, is reacted with a
dialkyl phosphonomethyl hydroxylamine, 158.1, prepared as described
above from a dialkyl trifluoromethylsulfonyloxymethyl phosphonate
(Tetrahedron Lett., 1986, 27, 1477) and BOC-hydroxylamine, to
afford the oxime, 158.2. Deprotection, as described in Example 156,
then affords the 20-keto phosphonate, 158.3. The oxime forming
reaction is performed at ambient temperature in ethanol-acetic acid
solution between equimolar amounts of the reactants.
[1154] Using the above procedures, but employing, in place of the
hydroxyl-amine ether, 158.1, different oxime ethers, 157.1, the
corresponding products, 157.3 are obtained.
Example 159
##STR00355##
[1156] The dienone, 156.1, in which the 20-ketone is protected as
the dimethyl hydrazone, is reacted, as described above, with
O-(5-bromo-3-pyridylmethoxy)-hydroxylamine, 159.1, prepared as
described above from 5-bromo-3-bromo-methylpyridine (WO 95/28400)
and BOC-protected hydroxylamine, 157.5, to give the oxime, 159.2.
The protecting group is then removed to yield the 20-keto product,
159.3. The latter product is then reacted, in the presence of a
palladium catalyst, with a dialkyl phosphite, 159.4, to afford the
phosphonate, 159.5. The preparation of arylphosphonates by means of
a coupling reaction between aryl bromides and dialkyl phosphites is
described in J. Med. Chem., 1992, 35, 1371. The reaction is
performed at ca. 100.degree. C. in an inert solvent such as
toluene, in the presence of a base such as triethylamine and a
catalytic amount of tetrakis(triphenylphosphine)palladium(0).
[1157] Alternatively, the bromo compound, 159.3, is coupled with a
dialkyl vinylphosphonate, 159.6, (Aldrich) to afford the
phosphonate, 159.7. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in F. A.
Carey and R. J. Sundberg, Advanced Organic Chemistry 503ff (Plenum,
2001) and in Acc. Chem. Res., 1979, 12, 146. The aryl bromide and
the olefin are coupled in a polar solvent such as dimethylformamide
or dioxan, in the presence of a palladium(0) catalyst such as
tetrakis(triphenyl-phosphine)palladium(0) or palladium(II) catalyst
such as palladium(II) acetate, and optionally in the presence of a
base such as triethylamine or potassium carbonate. Optionally, the
styrenoid double bond present in the product, 159.7, is reduced,
for example by reaction with diimide, to produce the saturated
analog, 159.8. The reduction of olefinic bonds is described in R.
C. Larock, Comprehensive Organic Transformations 6ff (VCH 1989).
The transformation is effected by means of catalytic hydrogenation,
for example using a palladium on carbon catalyst and hydrogen or a
hydrogen donor, or by the use of diimide or diborane.
[1158] Using the above procedures, but employing, in place of the
bromopyridyl reagent, 159.1, different bromo-substituted aryl or
heteroaryl alkoxy hydroxylamines, and/or different dialkyl alkenyl
phosphonates, products analogous to the compounds, 159.5, 159.7 and
159.8 are obtained.
Example 160
##STR00356##
[1160] The dienone, 156.1, in which the 20-ketone is protected as
the dimethylhydrazone, is reacted with 2-hydroxyethyl
hydroxylamine, 160.1, (J. Chem. Soc. Chem. Comm., 1986, 903) to
yield the oxime, 160.2. The reaction of unsaturated steroidal
ketones with hydroxylamines is described in J. Steroid Bioch. 1976,
7, 795; the reaction is performed between equimolar amounts of the
reactants in a polar organic solvent such as pyridine or methanol,
optionally in the presence of acetic acid or sodium acetate. The
product, 160.2, is then coupled with a dialkyl 4-aminophenyl
phosphonate, 160.3, (Epsilon) and carbonyl diimidazole, to yield,
after deprotection, the carbamate oxime, 160.4. The preparation of
carbamates is described in Comprehensive Organic Functional Group
Transformations, Vol. 6, 416ff (A. R. Katritzky, ed., Pergamon,
1995) and in S. R. Sandler and W. Karo, Organic Functional Group
Preparations 260ff (Academic Press, 1986). In the procedure, the
amine is reacted in an inert aprotic solvent such as
dichloromethane or tetrahydrofuran, with phosgene or a functional
equivalent thereof, such as carbonyl diimidazole, triphosgene,
pentafluorophenyl carbonate and the like, to afford the
corresponding activated acylamine. The latter compound is then
reacted with an alcohol to yield the carbamate.
[1161] Using the above procedures, but employing, in place of the
hydroxy-substituted hydroxylamine, 160.1, different
hydroxy-substituted hydroxylamines, and/or different
amino-substituted phosphonates, the products analogous to 160.4 are
obtained.
Example 161
##STR00357##
[1163] The enone, 161.1, in which the 20-ketone is protected as the
cyclic ethylene ketal, is reacted with ethyl formate and a base
such as sodium hydride, in an inert solvent such as toluene or
dimethylformamide, as described in J. Am. Chem. Soc. 86:1520
(1964), to afford the 2-formyl product, 161.2. This compound is
then reacted with an alkyl, aralkyl, aryl or heteroaryl hydrazine,
161.3, in which the substituent X is either a phosphonate group or
a group which is subsequently transformed into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxyl and the like. The
reaction yields, after deprotection of the 20-ketone, the isomeric
2'- and 1'-aryl pyrazoles, 161.4 and 161.5. The pyrazole-forming
reaction is performed between equimolar amounts of the reactants in
an acidic solvent such as acetic acid, as described in J. Am. Chem.
Soc., 1964, 86, 1520. The pyrazoles, 161.4 and 161.5, are then
transformed, for example by the procedures described herein, into
the phosphonates, 161.6 and 161.7.
Example 162
##STR00358##
[1165] The ketoaldehyde, 161.2, is reacted, as described above,
with 3-carboxyphenyl hydrazine, 162.1, (Apin) to give the
pyrazoles, 162.2 and 162.3. The 2'-substituted isomer, 162.2, is
then reacted in dimethylformamide solution at ambient temperature
with one molar equivalent of a dialkyl 2-aminoethyl phosphonate,
162.4, (Aldrich) and dicyclohexyl carbodiimide, to give the amide
phosphonate, 162.5. The preparation of amides from carboxylic acids
and derivatives is described, for example, in S. R. Sandler and W.
Karo, Organic Functional Group Preparations 274 (Academic Press,
1968) and R. C. Larock, Comprehensive Organic Transformations 972ff
(VCH, 1989). The carboxylic acid is reacted with the amine in the
presence of an activating agent, such as, for example,
dicyclohexylcarbodiimide or diisopropylcarbodiimide, optionally in
the presence of, for example, hydroxybenztriazole,
N-hydroxysuccinimide or N-hydroxypyridone, in a non-protic solvent
such as, for example, pyridine, DMF or dichloromethane, to afford
the amide.
[1166] Alternatively, the carboxylic acid may first be converted
into an activated derivative such as the acid chloride, anhydride,
mixed anhydride, imidazolide and the like, and then reacted with
the amine, in the presence of an organic base such as, for example,
pyridine, to afford the amide.
[1167] The conversion of a carboxylic acid into the corresponding
acid chloride can be effected by treatment of the carboxylic acid
with a reagent such as, for example, thionyl chloride or oxalyl
chloride in an inert organic solvent such as dichloromethane,
optionally in the presence of a catalytic amount of
dimethylformamide.
[1168] The isomeric pyrazole, 162.3, is reacted, as described
above, with one molar equivalent of a dialkyl 4-amino-2-thienyl
phosphonate, 162.6, prepared by the palladium catalyzed coupling
reaction, as described above, between 4-amino-2-bromothiophene
(Tetrahedron Lett., 1987, 43, 3295) and a dialkyl phosphite, to
give the amide phosphonate, 162.7.
[1169] Using the above procedures, but employing different
carboxy-substituted hydrazines, and/or different amino-substituted
phosphonates, the products analogous to 162.5 and 162.7 are
obtained.
Example 163
##STR00359##
[1171] The ketoaldehyde, 161.2, is reacted, as described above,
with 3-bromophenyl hydrazine, 163.1, (Fluka) to produce the
pyrazoles, 163.2 and 163.3. The 2'-substituted isomer, 163.2, is
then coupled, as described above, with a dialkyl phosphite, 163.4,
to afford the phosphonate, 163.5.
[1172] Alternatively, the 1'-substituted pyrazole, 163.3, is
coupled, as described above, with a dialkyl vinylphosphonate,
163.6, (Aldrich) and a palladium catalyst to prepare the vinyl
phosphonate, 163.7. Optionally, the product is reduced, as
described above, to give the analog, 163.8.
[1173] Using the above procedures, but employing, in place of the
bromophenyl hydrazine, 163.1, different bromo-substituted
hydrazines, and/or different dialkyl alkenyl phosphonates, the
products analogous to the compounds, 163.5 and 163.7, 163.8 are
obtained.
Example 164
##STR00360##
[1175] The ketoaldehyde, 161.2, is reacted with hydrazine to
afford, after deprotection of the 20-ketone, the pyrazole
derivative, 164.1. The reaction of steroidal 2-formyl-3-ketones
with hydrazine is described in J. Am. Chem. Soc., 1964, 86, 1520.
The reaction is performed in acetic acid at ambient temperature.
The pyrazole product is then reacted with a bromomethyl compound,
164.2, in which R.sup.2 and X are as defined above, or a reactive
bromoheteroaromatic reagent, to yield the alkylation products,
164.3 and 164.4. The alkylation of substituted pyrazoles is
described, for example, in T. L. Gilchrist, Heterocyclic Chemistry,
309 (Longman, 1992). The reaction is performed between equimolar
amounts of the substrates in a polar solvent such as
dimethylformamide or tetrahydrofuran, in the presence of a base
such as dimethylaminopyridine, lithium hexamethyldisilazide and the
like. The products, 164.3 and 164.4, are, except in cases where X
is dialkylphosphono, converted into the phosphonates, 164.5 and
164.6, using the procedures described herein.
Example 165
##STR00361##
[1177] The pyrazole, 164.1, is reacted in dimethylformamide
solution at 70.degree. C. with one molar equivalent of a dialkyl
4-bromomethyl phosphonate, 165.1, (Lancaster) and lithium
hexamethyl disilazide, to give the pyrazoles, 165.2 and 165.3.
[1178] Using the above procedures, but employing different
bromo-substituted phosphonates, the products analogous to 165.2 and
165.3 are obtained.
Example 166
##STR00362##
[1180] The pyrazole, 164.1, is reacted in tetrahydrofuran solution
with 4-bromomethyl cyclohexanone, 166.1, (WO 97/37959) and
potassium hexamethyl disilazide, to give the alkylation products,
166.2 and 166.3. The 2'-substituted isomer, 166.2, is then reacted,
in a reductive amination reaction, with a dialkyl aminomethyl
phosphonate, 166.5, (Interchim) and sodium triacetoxy borohydride,
to yield the amine phosphonate, 166.4. The preparation of amines by
means of reductive amination procedures is described, for example,
in R. C. Larock, Comprehensive Organic Transformations 421 (VCH)
and in F. A. Carey and R. J. Sundberg, Advanced Organic Chemistry,
Part B, 269 (Plenum, 2001). In this procedure, the amine component
and the aldehyde or ketone component are reacted together in the
presence of a reducing agent such as, for example, borane, sodium
cyanoborohydride, sodium triacetoxyborohydride or
diisobutylaluminum hydride, optionally in the presence of a Lewis
acid, such as titanium tetraisopropoxide, as described in J. Org.
Chem., 1990, 55, 2552.
[1181] The 1'-substituted pyrazole, 166.3, is converted by the same
reaction into the isomeric amine phosphonate, 166.6.
[1182] Using the above procedures, but employing different
bromo-substituted aldehydes and ketones, and/or different
amino-substituted phosphonates, products analogous to 166.4 and
166.6 are obtained.
Example 167
##STR00363## ##STR00364##
[1184]
9.alpha.-Chloro-16.alpha.-methyl-11.beta.,17.alpha.,21-trihydroxypr-
egn-1,4-dien-3,2,1-dione, 167A, (U.S. Pat. No. 4,472,393) is
reacted with paraformaldehyde and an acid catalyst such as
hydrochloric acid, as described in Protective Groups in Organic
Synthesis, by T. W. Greene and P. G. M. Wuts, Wiley, Second Edition
1990, p. 223, to yield the BMD derivative, 167.1. The phosphonate
moiety is then introduced, using the procedures described below, to
produce the phosphonate ester, 167.2. The BMD moiety is then
hydrolyzed, for example by treatment with 50% aqueous acetic acid,
as described in Protective Groups in Organic Synthesis, by T. W.
Greene and P. G. M. Wuts, Wiley, Second Edition 1990, p. 223, to
afford the triol, 167.3. The latter compound is then converted into
the 17,21-cyclic orthoester, 167.5, using the procedure described
in Chem. Pharm. Bull., 1986, 34, 1613. The substrate is reacted in
dimethylformamide at 70.degree. C. with two molar equivalents of
triethyl ortho-2-furoate, 165.4, (Zh. Org. Khim., 1980, 50, 1348)
and a catalytic amount of p-toluenesulfonic acid. The product is
then reacted with an excess of trimethylsilyl chloride in
dimethylformamide at ambient temperature to produce the 21-chloro
17-(2-furoate) product, 167.6.
[1185] Alternatively, the substrate, 167.3, is converted into the
product, 167.6, by means of the method described in J. Med. Chem.,
1987, 30, 1581. In this procedure, the 21-hydroxy group is
activated by conversion to the 21-mesylate, by reaction with mesyl
chloride in pyridine; the mesylate group is then displaced to yield
the 21-chloro intermediate, by reaction with lithium chloride in
dimethylformamide, and the 17-hydroxyl group is esterified to give
the 21-chloro-17-(2-furoate) derivative, 167.6. The selective
acylation of the 17.alpha.-hydroxyl group in the presence of an
11.beta. hydroxyl group is described in J. Med. Chem., 1987, 30,
1581.
Example 168
##STR00365##
[1187] The BMD-protected derivative, 167.1, is reacted with an
amine or hydroxylamine, 168.1, in which R.sup.2 is an alkyl,
alkenyl, cycloalkyl or cycloalkenyl group, optionally incorporating
a heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the imine or oxime. The preparation of oximes of
steroidal 3-ketones is described in Anal Bioch., 1978, 86, 133 and
in J. Mass. Spectrom., 1995, 30, 497. The BMD-protected side-chain
compound, 168.2, is then converted into the triol, 168.3, and then
to the 21-chloro 17-(2-furoate) product, 168.4, as described
herein.
##STR00366##
[1188] The preparation of hydroxylamine ethers incorporating a
phosphonate group is illustrated herein. In this procedure, a
phosphonate, 168.5, in which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxylamine,
168.6, (Aldrich) to produce the ether, 168.7. The reaction is
conducted between equimolar amounts of the reactants in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as potassium hydroxide or
dimethylaminopyridine. Deprotection, for example by treatment with
trifluoroacetic acid, then gives the hydroxylamine ether,
168.8.
Example 169
##STR00367##
[1190] The substrate, 167.1, is reacted with a dialkyl
phosphonomethyl hydroxylamine, 169.1, prepared as described above
from a dialkyl trifluoromethylsulfonyloxymethyl phosphonate (Tet.
Lett., 1986, 27, 1477) and BOC-hydroxylamine, to afford the oxime,
169.2. Deprotection then affords the triol, 169.3, from which the
21-chloro 17-(2-furoate) compound, 169.4, is prepared, using the
procedures described in Example 167. The oxime forming reaction is
performed at ambient temperature in ethanol-acetic acid solution
between equimolar amounts of the reactants.
[1191] Using the above procedures, but employing, in place of the
hydroxylamine ether, 169.1, different oxime ethers, 167.1, the
corresponding products, 169.4 are obtained.
Example 170
##STR00368##
[1193] The dienone, 167.1, is reacted, as described above, with
O-(5-bromo-3-pyridylmethoxy)hydroxylamine, 170.1, prepared as
described above from 5-bromo-3-bromomethylpyridine (EP 511865) and
BOC-protected hydroxylamine, 168.6, to give, after deprotection of
the side-chain, the oxime, 170.2. The product is then reacted, in
the presence of a palladium catalyst, with a dialkyl phosphite,
170.3, to afford the phosphonate, 170.4. The preparation of
arylphosphonates by means of a coupling reaction between aryl
bromides and dialkyl phosphites is described in J. Med. Chem.,
1992, 35, 1371. The reaction is performed at ca. 100.degree. C. in
an inert solvent such as toluene, in the presence of a base such as
triethylamine and a catalytic amount of
tetrakis(triphenyl-phosphine)palladium(0). The 21-hydroxy compound,
170.4, is then converted, as described in Example 167, into the
21-chloro 17-(2-furoate) derivative, 170.5.
[1194] Alternatively, the bromo compound, 170.2, is coupled with a
dialkyl vinyl phosphonate, 170.6, (Aldrich) to afford the
phosphonate, 170.7. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in F. A.
Carey and R. J. Sundberg, Advanced Organic Chemistry, 503ff
(Plenum, 2001) and in Acc. Chem. Res., 1979, 12, 146. The aryl
bromide and the olefin are coupled in a polar solvent such as
dimethylformamide or dioxan, in the presence of a palladium(0)
catalyst such as tetrakis(triphenyl-phosphine)palladium(0) or
palladium(II) catalyst such as palladium(II) acetate, and
optionally in the presence of a base such as triethylamine or
potassium carbonate. Optionally, the double bond present in the
product, 170.7, is reduced, for example by reaction with diimide,
to produce the saturated analog, 170.9. The reduction of olefinic
bonds is described in R. C. Larock, Comprehensive Organic
Transformations, 6ff (VCH, 1989). The transformation is effected by
means of catalytic hydrogenation, for example using a palladium on
carbon catalyst and hydrogen or a hydrogen donor, or by the use of
diimide or diborane. The products, 170.7 and 170.9, are then
converted into the 21-chloro 17-(2-furoate) analogs, 170.8 and
170.10.
[1195] Using the above procedures, but employing, in place of the
bromopyridylmethoxy reagent, 170.1, different bromo-substituted
aryl or heteroaryl alkoxy hydroxylamines, and/or different dialkyl
alkenyl phosphonates, the products analogous to the compounds,
170.5, 170.8 and 170.10 are obtained.
Example 171
##STR00369##
[1197] The preparation of phosphonates in which the phosphonate is
attached by means of an imino group is illustrated herein. In this
procedure, the substrate, 167.1, is reacted with a dialkyl
4-aminophenyl phosphonate, 171.1, (Epsilon) to give, after
deprotection, the imine product, 171.2. The imine forming reaction
is conducted in a hydrocarbon solvent such as toluene or xylene, at
reflux temperature, in the presence of a basic catalyst such as
sodium methoxide, or an acid catalyst such as p-toluenesulfonic
acid, under azeotropic conditions. The product is then converted
into the 21-chloro 17-(2-furoate) compound, 171.3.
[1198] Using the above procedures, but employing, in place of the
4-aminophenyl phosphonate, 171.1, different amino-substituted aryl
or heteroaryl phosphonates, products analogous to 171.3 are
obtained.
Example 172
##STR00370##
[1200] The dienone, 167.1, is reacted with
O-(2-aminoethyl)hydroxylamine, 172.1, (Pol. J. Chem., 1981, 55,
1163) to yield the oxime, 172.2. The reaction of steroidal
1,4-dien-3-ones with substituted hydroxylamines is described in J.
Steroid Bioch., 4976, 7, 795; the reaction is performed between
equimolar amounts of the reactants in a polar organic solvent such
as pyridine or methanol, optionally in the presence of acetic acid
or sodium acetate. The product is then reacted, in a reductive
amination procedure, with a dialkyl 4-formylphenyl phosphonate,
172.3, (Epsilon) and sodium triacetoxyborohydride, to yield the
amine oxime 172.4. The preparation of amines by means of reductive
amination procedures is described, for example, in R. C. Larock,
Comprehensive Organic Transformations, 421 (VCH), and in F. A.
Carey and R. J. Sundberg, Advanced Organic Chemistry, Part B, 269
(Plenum, 2001). In this procedure, the amine component and the
aldehyde or ketone component are reacted together in the presence
of a reducing agent such as, for example, borane, sodium
cyanoborohydride, sodium triacetoxyborohydride or
diisobutylaluminum hydride, optionally in the presence of a Lewis
acid, such as titanium tetraisopropoxide, as described in J. Org.
Chem., 1990, 55, 2552.
[1201] The amine product, 172.4, is then converted, as described
herein, into the 21-chloro 17-(2-furoate) product, 171.6.
[1202] Using the above procedures, but employing, in place of the
hydroxylamine, 172.3, different amino-substituted hydroxylamines,
and/or different formyl-substituted phosphonates, the products
analogous to 177.6 are obtained.
Example 173
##STR00371## ##STR00372##
[1204] The BMD-protected dienone, 167.1, is reduced to afford the
1,2-dihydro product, 173.1. The catalytic hydrogenation reaction is
effected by the use of tris(triphenylphosphine)rhodium (1)
chloride, for example as described in J. Med. Chem., 2001, 44, 602.
The product is then reacted with ethyl formate and a base such as
sodium hydride, in an inert solvent such as toluene or
dimethylformamide, as described in J. Am. Chem. Soc., 1964, 86,
1520, to afford the 2-formyl product, 173.2. This compound is then
reacted with an alkyl, aralkyl, aryl or heteroaryl hydrazine,
173.3, in which the substituent X is either a phosphonate group or
a group which is subsequently transformed into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxyl and the like. The
reaction yields the isomeric 2'- and 1'-aryl pyrazoles, 173.4 and
173.5. The pyrazole-forming reaction is performed between equimolar
amounts of the reactants in an acidic solvent such as acetic acid,
as described in J. Am. Chem. Soc., 1964, 86, 1520. The pyrazoles,
173.4 and 173.5, are then transformed, for example by the
procedures described herein, via the BMD-protected intermediates,
173.6 and 173.7, into the 21-chloro 17-(2-furoate) phosphonates,
173.9 and 173.11.
Example 174
##STR00373## ##STR00374##
[1206] The ketoaldehyde, 173.2, is reacted, as described above,
with 4-bromo-benzyl hydrazine, 174.1, (Ann., 1968, 717, 104) to
give the pyrazoles, 174.2 and 174.3. The 2'-substituted isomer,
174.2, is then coupled, as described in Example 170, with a dialkyl
phosphite, to yield the phosphonate, 173.4. The BMD protecting
group is then removed and the product is converted into the
21-chloro 17-(2-furoate) product, 173.6.
[1207] The isomeric pyrazole, 174.3, is subjected to the same
series of reactions to afford the isomeric product, 173.9.
[1208] Using the above procedures, but employing different
bromo-substituted hydrazines, the products analogous to 173.6 and
173.9 are obtained.
Example 174
##STR00375## ##STR00376##
[1210] The ketoaldehyde, 173.2, is reacted, as described above,
with 4-hydroxy-phenyl hydrazine, 174.1, (EP 437105) to produce the
pyrazoles, 174.2 and 174.3. The 1'-substituted isomer, 174.2, is
reacted in dimethylformamide at 70.degree. C., with a dialkyl
2-bromoethyl phosphonate, 174.4, (Aldrich) and potassium carbonate,
to give the ether phosphonate, 174.5. The product is then
deprotected to afford the triol, 174.6, which is converted into the
21-chloro 17-(2-furoate) compound, 174.7.
[1211] Alternatively, the 2'-substituted pyrazole, 174.3, is
coupled, in a Mitsonobu reaction, with a dialkyl 2-mercaptoethyl
phosphonate, 174.8, (Zh. Obschei. Khim., 1973, 43, 2364) to prepare
the thioether phosphonate, 174.9, which is deprotected, and the
product is converted into the 21-chloro 17-(2-furoate) analog,
174.11. The preparation of aromatic ethers and thioethers by means
of the Mitsonobu reaction is described, for example, in R. C.
Larock, Comprehensive Organic Transformations, 448 (VCH, 1989), and
in F. A. Carey and R. J. Sundberg, Advanced Organic Chemistry, Part
B, 153-4 (Plenum, 2001) and in Org. React., 1992, 42, 335. The
phenol and the alcohol or thiol component are reacted together in
an aprotic solvent such as, for example, tetrahydrofuran, in the
presence of a dialkyl azodicarboxylate and a triaryl-phosphine, to
afford the ether or thioether products. The procedure is also
described in Org. React., 1992, 42, 335-656.
[1212] Using the above procedures, but employing, in place of the
4-hydroxy-phenyl hydrazine, 174.1, different hydroxy-substituted
hydrazines, and/or different dialkyl bromo- or mercapto-substituted
phosphonates, the products analogous to the compounds, 174.7 and
174.11 are obtained.
Example 175
##STR00377## ##STR00378##
[1214] The ketoaldehyde, 173.2, is reacted with hydrazine, to
afford the pyrazole derivative, 175.1. The reaction of steroidal
2-formyl-3-ketones with hydrazine is described in J. Am. Chem. Soc,
1964, 86, 1520. The reaction is performed in acetic acid at ambient
temperature. The pyrazole product is then reacted with a
bromomethyl compound, 175.6, in which R.sup.2 and X are as defined
above, or a reactive bromoheteroaromatic reagent, to yield the
alkylation products, 175.3 and 175.4. The alkylation of substituted
pyrazoles is described, for example, in T. L. Gilchrist,
Heterocyclic Chemistry, 309 (Longman, 1992). The reaction is
performed between equimolar amounts of the substrates in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as dimethylaminopyridine, lithium
hexamethyldisilazide and the like. The products, 175.3 and 175.4,
are, except in cases where X is dialkyl-phosphono, converted into
the phosphonates, 175.5 and 175.6, using the procedures described
herein, and deprotection/chlorination/acylation then affords the
21-chloro 17-(2-furoate) compounds, 175.8 and 175.10.
Example 176
##STR00379##
[1216] The pyrazole, 175.1, is reacted with 2,5-dibromopyrimidine,
176.1, (Chem. Lett., 1992, 583) to give the pyrazoles, 176.2 and
176.3. The products are then coupled, as described above, with a
dialkyl phosphite, to afford after side-chain deprotection and
modification, as described above, the 21-chloro 17-(2-furoates),
176.5 and 176.7.
Example 177
##STR00380##
[1218] The pyrazole, 175.1, is reacted in tetrahydrofuran solution,
with 1,2-bis(bromomethyl)cyclobutane, 177.1 (J. Org. Chem., 1981,
46, 3530) and potassium hexamethyl disilazide, to give the
alkylation products, 177.1 and 177.2. The 1'-substituted isomer,
177.2, is then reacted, in an Arbuzov reaction, with a trialkyl
phosphite to yield, after deprotection and side-chain modification,
the 21-chloro 17-(2-furoate), 177.5. The Arbuzov reaction is
described in Handb. Organophosphorus Chem., 1992, 115. In this
procedure, in which a bromo substituent is converted into the
corresponding phosphonate, the substrate is heated at from about
60.degree. C. to about 160.degree. C. with a five to fifty-fold
molar excess of a trialkyl phosphite, to effect the
transformation.
[1219] The 2'-substituted pyrazole, 177.3, is subjected to the same
series of reaction to give the amine phosphonate, 177.7.
[1220] Using the above procedures, but employing different
dibromides, the products analogous to 177.5 and 177.7 are
obtained.
Example 178
##STR00381##
[1222] A protection-deprotection sequence in which the 20-ketone
group and/or the 21-hydroxyl group of Budesonide, 178A, are
protected to afford the derivative, 178.1. The ketone is protected,
for example, by conversion to the cyclic ethylene ketal, by
reaction in toluene solution at reflux temperature with ethylene
glycol and an acid catalyst, as described in J. Am. Chem. Soc.,
1955, 77, 1904. Deprotection is effected by reaction with
pyridinium tosylate in aqueous acetone, as described in J. Chem.
Soc. Chem. Comm., 1987, 1351.
[1223] Alternatively, the 20-ketone is protected by conversion to
the N,N-dimethylhydrazone. The dimethyl hydrazone is prepared by
the reaction of the ketone, 178A, with N,N-dimethylhydrazine in
ethanol-acetic acid, as described in Org. Syn., 1970, 50, 102. The
group is removed by treatment with sodium acetate and acetic acid
in aqueous tetrahydrofuran, as described in J. Am. Chem. Soc.,
1979, 101, 5841.
[1224] Alternatively, the 20-ketone is protected as the
diethylamine adduct. In this procedure, the substrate, 178A, is
reacted with titanium tetrakis(diethylamide), as described in J.
Chem. Soc., Chem. Comm., 1983, 406, to afford the adduct. The
ketone is deprotected by reaction with water in an aqueous organic
solvent.
[1225] The 21-hydroxyl group is protected, for example, by
conversion to the acetate ester, by reaction with one molar
equivalent of acetyl chloride in dichloromethane/pyridine. The
21-acetoxy group is removed by reaction with one molar equivalent
of lithium hydroxide in aqueous dimethoxyethane.
[1226] Alternatively, the 21-hydroxyl group is protected by
conversion to the tert. butyl dimethylsilyl ether, by reaction in
dimethylformamide solution with one molar equivalent of tert.
butylchlorodimethylsilane and imidazole, as described in J. Am.
Chem. Soc., 1972, 94, 6190. The silyl ether is removed by reaction
with tetrabutylammonium fluoride in tetrahydrofuran solution, as
described in J. Am. Chem. Soc., 1972, 94, 6190.
[1227] The protected compound, 178.1, is then converted into the
phosphonate-containing analog, 178.2, using the procedures
described below, and the protecting group or groups are then
removed, as described above, to give the phosphonate, 178.3.
Example 179
##STR00382##
[1229] The ketone-protected derivative, 179.1, is reacted with an
amine or hydroxylamine, 179.2, in which R.sup.2 is an alkyl,
alkenyl, cycloalkyl or cycloalkenyl group, optionally incorporating
a heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the imine or oxime, 179.3. The preparation of
oximes of steroidal 3-ketones is described in Anal. Bioch., 1978,
86, 133 and in J. Mass. Spectrom., 1995, 30, 497. The protecting
group is then removed, as described herein, to afford the 20-keto
phosphonate product, 179.4.
Example 179A
##STR00383##
[1231] The preparation of hydroxylamine ethers incorporating a
phosphonate group is also illustrated. In this procedure, a
phosphonate, 179.5, in which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxylamine,
179.6, (Aldrich) to produce the ether, 179.7. The reaction is
conducted between equimolar amounts of the reactants in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as potassium hydroxide or
dimethylaminopyridine. Deprotection, for example by treatment with
trifluoroacetic acid, then gives the hydroxylamine ether, 179.8.
The above procedure is also employed for the preparation of
substituted hydroxylamines which are precursors to
phosphonates.
Example 180
##STR00384##
[1233] The substrate, 179.1, in which the 20-ketone is protected as
the dimethyl hydrazone derivative, is reacted with a dialkyl
phosphonomethyl hydroxylamine, 180.1, prepared as described above
from a dialkyl trifluoromethylsulfonyl-oxymethyl phosphonate (Tet.
Lett., 1986, 27, 1477) and BOC-hydroxylamine, to afford the oxime,
180.2. Deprotection, as described in Example 179, affords the
20-keto phosphonate, 180.3. The oxime forming reaction is performed
at ambient temperature in ethanol-acetic acid solution between
equimolar amounts of the reactants.
[1234] Using the above procedures, but employing, in place of the
hydroxyl-amine ether, 180.1, different oxime ethers, 179.2, the
corresponding products, 179.4 are obtained.
Example 181
##STR00385##
[1236] The preparation of compounds, 179.1, in which the
phosphonate group is attached by means of a benzyloxy oxime group
is illustrated above. In this procedure, the dienone, 179.1, in
which the 20-ketone is protected as the dimethyl hydrazone, is
reacted, as described above, with O-(2-bromobenzyl)hydroxylamine,
181.1, prepared as described above from 2-bromobenzyl bromide and
BOC-protected hydroxylamine, 179.6, to give the oxime, 181.2. The
protecting group is then removed to yield the 20-keto product,
181.3. The latter product is then reacted, in the presence of a
palladium catalyst, with a dialkyl phosphite, 181.4, to afford the
phosphonate, 181.5. The preparation of arylphosphonates by means of
a coupling reaction between aryl bromides and dialkyl phosphites is
described in J. Med. Chem., 1992, 35, 1371. The reaction is
performed at ca. 100.degree. in an inert solvent such as toluene,
in the presence of a base such as triethylamine and a catalytic
amount of tetrakis(triphenylphosphine)palladium(0).
[1237] Alternatively, the bromo compound, 181.3, is coupled with a
dialkyl vinylphosphonate, 181.6, (Aldrich) to afford the
phosphonate, 181.7. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in Advanced
Organic Chemistry, by F. A. Carey and R. J. Sundberg, Plenum, 2001,
p. 503ff and in Acc. Chem. Res., 1979, 12, 146. The aryl bromide
and the olefin are coupled in a polar solvent such as
dimethyl-formamide or dioxan, in the presence of a palladium(0)
catalyst such as tetrakis(triphenylphosphine)palladium(0) or
palladium(II) catalyst such as palladium(II) acetate, and
optionally in the presence of a base such as triethylamine or
potassium carbonate. Optionally, the styrenoid double bond present
in the product, 181.7, is reduced, for example by reaction with
diimide, to produce the saturated analog, 181.8. The reduction of
olefinic bonds is described in Comprehensive Organic
Transformations, by R. C. Larock, VCH, 1989, p. 6ff. The
transformation is effected by means of catalytic hydrogenation, for
example using a palladium on carbon catalyst and hydrogen or a
hydrogen donor, or by the use of diimide or diborane.
[1238] Using the above procedures, but employing, in place of the
bromobenzyl reagent, 181.1, different bromo-substituted aryl or
heteroaryl alkoxy hydroxylamines, and/or different dialkyl alkenyl
phosphonates, the products analogous to the compounds, 181.5, 181.7
and 181.8 are obtained.
Example 182
##STR00386##
[1240] The substrate, 171.1, in which the 20-ketone is protected as
the dimethyl-hydrazone, is reacted with a dialkyl 4-aminophenyl
phosphonate, 182.1, (Epsilon), to give, after deprotection, the
imine product, 182.2. The imine forming reaction is conducted in a
hydrocarbon solvent such as toluene or xylene, at reflux
temperature, in the presence of a basic catalyst such as sodium
methoxide, or an acid catalyst such as p-toluenesulfonic acid,
under azeotropic conditions.
[1241] Using the above procedures, but employing, in place of the
4-amino-phenyl phosphonate, 182.1 different amino-substituted aryl
or heteroaryl phosphonates, products analogous to 182.2 are
obtained.
Example 183
##STR00387##
[1243] The preparation of phosphonates in which the phosphonate is
attached by means of an oximino group and a carbamate linkage is
illustrated herein. In this procedure, the dienone, 171.1, in which
the 20-ketone is protected as the dimethylhydrazone, is reacted
with 4-aminobutyl hydroxylamine, 183.1, (Pol. J. Chem., 1981, 55,
1163) to yield the oxime, 183.2. (The reaction of steroidal
1,4-dien-3-ones with hydroxylamines is described in J. Steroid
Bioch., 1976, 7, 795.)
[1244] The reaction is performed between equimolar amounts of the
reactants in a polar organic solvent such as pyridine or methanol,
optionally in the presence of acetic acid or sodium acetate. The
product, 183.2, is then coupled with a dialkyl 2-hydroxyethyl
phosphonate, 183.3, (Epsilon) and carbonyl diimidazole (CDI), to
yield, after deprotection, the carbamate oxime, 183.4. The
preparation of carbamates is described in Comprehensive Organic
Functional Group Transformations, A. R. Katritzky, ed., Pergamon,
1995, Vol. 6, p 416ff, and in Organic Functional Group
Preparations, by S. R. Sandler and W. Karo, Academic Press, 1986,
p. 260ff. In the procedure, the amine is reacted in an inert
aprotic solvent such as dichloromethane or tetrahydrofuran, with
phosgene or a functional equivalent thereof, such as carbonyl
diimidazole, triphosgene, pentafluorophenyl carbonate and the like,
to afford the corresponding activated acylamine. The latter
compound is then reacted with an alcohol to yield the
carbamate.
[1245] Using the above procedures, but employing, in place of the
amino-substituted hydrazine, 183.1, different amino-substituted
hydrazines, and/or different hydroxy-substituted phosphonates, the
products analogous to 183.4 are obtained.
Example 184
##STR00388##
[1247] The dienone, 178.3, in which the 21-hydroxyl group is
protected as described in Example 178 is reduced to afford the
1,2-dihydro product, 184.1. The catalytic hydrogenation reaction is
effected by the use of tris(triphenyl-phosphine)rhodium (I)
chloride, for example as described in J. Med. Chem., 2001, 44, 602.
The product is then reacted with ethyl formate and a base such as
sodium hydride, in an inert solvent such as toluene or
dimethylformamide, as described in J. Am. Chem. Soc., 1964, 86,
1520, to afford the 2-formyl product, 184.2. This compound is then
reacted with an alkyl, aralkyl, aryl or heteroaryl hydrazine,
184.3, in which the substituent X is either a phosphonate group or
a group which is subsequently transformed into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxyl and the like. The
reaction yields, after deprotection of the 21-hydroxyl group, the
isomeric 2'- and 1'-aryl pyrazoles, 184.4 and 184.5. The
pyrazole-forming reaction is performed between equimolar amounts of
the reactants in an acidic solvent such as acetic acid, as
described in J. Am. Chem. Soc., 1964, 86, 1520. The pyrazoles,
184.4 and 184.5, are then transformed, for example by the
procedures described in Examples 180 and 181, into the
phosphonates, 184.6 and 184.7.
Example 185
##STR00389##
[1249] The ketoaldehyde, 184.2, is reacted, as described above,
with 4-bromophenyl hydrazine, 185.1, (J. Organomet. Chem., 1999,
62, 581) to give the pyrazoles, 185.2 and 185.3. The 2'-substituted
isomer 185.2 is then reacted, as described above, with a dialkyl
phosphate, 184.4, to give the phosphonate, 185.5.
[1250] The isomeric pyrazole, 185.3, is reacted in a Heck reaction,
as described above, with one molar equivalent of a dialkyl
4-vinylphenyl phosphonate, 185.6, (Macromolecules, 1998, 31, 2918)
to yield the phosphonate, 185.7.
[1251] Using the above procedures, but employing different
bromo-substituted hydrazines, and/or different alkenyl-substituted
phosphonates, the products analogous to 185.5 and 185.7 are
obtained.
Example 186
##STR00390##
[1253] The ketoaldehyde, 184.2, is reacted, as described above,
with 4-hydroxy-phenyl hydrazine, 186.1, (EP 437105) to produce the
pyrazoles, 186.2 and 186.3. The 2'-substituted isomer, 186.2, is
then reacted in dimethylformamide solution at 70.degree. with one
molar equivalent of a dialkyl bromopropyl phosphonate, 186.4, (J.
Amer. Chem. Soc., 2000, 122, 1554) and cesium carbonate, to give
the ether phosphonate, 186.5.
[1254] Alternatively, the 1'-substituted pyrazole, 186.3, is
coupled in a Mitsonobu reaction, with a dialkyl 2-mercaptoethyl
phosphonate, 186.6, (Zh. Obschei. Khim., 1973, 43, 2364) to prepare
the thioether phosphonate, 186.7. The preparation of aromatic
ethers and thioethers by means of the Mitsonobu reaction is
described, for example, in Comprehensive Organic Transformations,
by R. C. Larock, VCH, 1989, p. 448, and in Advanced Organic
Chemistry, Part B, by F. A. Carey and R. J. Sundberg, Plenum, 2001,
p. 153-4 and in Org. React., 1992, 42, 335. The phenol and the
alcohol or thiol component are reacted together in an aprotic
solvent such as, for example, tetrahydrofuran, in the presence of a
dialkyl azodicarboxylate and a triarylphosphine, to afford the
ether or thioether products. The procedure is also described in
Org. React., 1992, 42, 335-656.
[1255] Using the above procedures, but employing, in place of the
hydroxyl-phenyl hydrazine, 186.1, different hydroxyaryl hydrazines,
and/or different dialkyl bromo- or mercapto-substituted
phosphonates, the products analogous to the compounds, 186.5 and
186.7 are obtained.
Example 187
##STR00391##
[1257] The ketoaldehyde, 184.2, is reacted with hydrazine to afford
the pyrazole derivative, 187.1. The reaction of steroidal
2-formyl-3-ketones with hydrazine is described in J. Am. Chem.
Soc., 1964, 86, 1520. The reaction is performed in acetic acid at
ambient temperature. The pyrazole product is then reacted with a
bromomethyl compound, 187.2, in which R.sup.2 and X are as defined
above, or a reactive bromoheteroaromatic reagent, to yield the
alkylation products, 187.3 and 187.4. The alkylation of substituted
pyrazoles is described, for example, in Heterocyclic Chemistry, by
T. L. Gilchrist, Longman, 1992, p. 309. The reaction is performed
between equimolar amounts of the substrates in a polar solvent such
as dimethylformamide or tetrahydrofuran, in the presence of a base
such as dimethylaminopyridine, lithium hexamethyldisilazide and the
like. The products, 187.3 and 187.4, are, except in cases where X
is dialkylphosphono, converted into the phosphonates, 187.5 and
187.6, using the procedures described herein.
Example 188
##STR00392##
[1259] The pyrazole, 187.1, is reacted in dimethylformamide
solution at 700 with one molar equivalent of a dialkyl
4-bromomethylphenyl phosphonate, 188.1, (Tet., 1998, 54, 9341) and
lithium hexamethyl disilazide, to give the pyrazoles, 188.2 and
188.3. Using the above procedures, but employing different
bromomethyl-substituted phosphonates, the products analogous to
188.2 and 188.3 are obtained.
Example 189
##STR00393##
[1261] The pyrazole, 187.1, is reacted in tetrahydrofuran solution
with 1,3-bis(bromomethyl)cyclopentane, 189.1, (Bull. Soc. Chim.
Fr., 1975, 1295) and sodium hydride, to give the alkylation
products, 189.2 and 189.3. The 2'-substituted isomer, 189.2, is
then reacted, in a Arbuzov reaction, with a trialkyl phosphite to
yield the phosphonate, 189.4. The Arbuzov reaction is described in
Handb. Organophosphorus Chem., 1992, 115. In this procedure, in
which a bromo substituent is converted into the corresponding
phosphonate, the substrate is heated at from about 60.degree. to
about 160.degree. with a five to fifty-fold molar excess of a
trialkyl phosphite, to effect the transformation.
[1262] The 2'-substituted pyrazole, 189.3, is reacted at 70.degree.
in dimethyl-formamide solution with one molar equivalent of a
dialkyl methylaminomethyl phosphonate, 189.5, and cesium carbonate,
to give the amine phosphonate, 189.6.
[1263] Using the above procedures, but employing different
dihalides, and/or different amino-substituted phosphonates, the
products analogous to 189.4 and 189.6 are obtained.
Example 190
##STR00394##
[1265] A protection-deprotection sequence in which the 20-ketone
group of Rimexolone, 190A, is protected to afford the derivative,
190.1. The ketone is protected, for example, by conversion to the
cyclic ethylene ketal, by reaction in toluene solution at reflux
temperature with ethylene glycol and an acid catalyst, as described
in J. Am. Chem. Soc., 1955, 77, 1904. Deprotection is effected by
reaction with pyridinium tosylate in aqueous acetone, as described
in J. Chem. Soc., Chem. Comm., 1987, 1351.
[1266] Alternatively, the 20-ketone is protected by conversion to
the N,N-dimethylhydrazone. The dimethyl hydrazone is prepared by
the reaction of the ketone, 190A, with N,N-dimethylhydrazine in
ethanol-acetic acid, as described in Org. Syn., 1970, 50, 102. The
group is removed by treatment with sodium acetate and acetic acid
in aqueous tetrahydrofuran, as described in J. Am. Chem. Soc.,
1979, 101, 5841.
[1267] Alternatively, the 20-ketone is protected as the
diethylamine adduct. In this procedure, the substrate, 190.1, is
reacted with titanium tetrakis-(diethylamide), as described in J.
Chem. Soc., Chem. Comm., 1983, 406, to afford the adduct. The
ketone is deprotected by reaction with water in an aqueous organic
solvent.
[1268] The protected compound, 190.2, is then converted into the
phosphonate-containing analog, 190.3, using the procedures
described below, and the protecting group or groups are then
removed, as described above, to give the phosphonate, 190.3.
Example 191
##STR00395##
[1270] The ketone-protected derivative, 190.1, is reacted with an
amine or hydroxylamine, 191.1, in which R.sup.2 is an alkyl,
alkenyl, cycloalkyl or cycloalkenyl group, optionally incorporating
a heteroatom O, S or N, or a functional group such as an amide,
ester, oxime, sulfoxide or sulfone etc, or an optionally
substituted aryl, heteroaryl or aralkyl group, optionally
incorporating a heteroatom O, S or N, and X is either a phosphonate
group or a group which is subsequently converted into a
phosphonate-containing substituent. For example, X is
dialkylphosphono, bromo, hydroxy, amino, carboxy and the like. The
reaction is conducted between equimolar amounts of the reactants in
an aprotic solvent such as pyridine or xylene, or in an alcoholic
solvent such as ethanol, optionally in the presence of an acid
catalyst, to give the imine or oxime, 191.2. The preparation of
oximes of steroidal 3-ketones is described in Anal. Bioch., 1978,
86, 133 and in J. Mass. Spectrom., 1995, 30, 497. The protecting
group is then removed, as described in Example 190, to afford the
20-keto phosphonate product, 191.3.
Example 191A
##STR00396##
[1272] The preparation of hydroxylamine ethers incorporating a
phosphonate group is also illustrated. In this procedure, a
phosphonate, 191.4, in which Lv is a leaving group such as bromo or
trifluoromethylsulfonyloxy, is reacted with BOC-hydroxylamine,
191.5, (Aldrich) to produce the ether, 191.6. The reaction is
conducted between equimolar amounts of the reactants in a polar
solvent such as dimethylformamide or tetrahydrofuran, in the
presence of a base such as potassium hydroxide or
dimethylaminopyridine. Deprotection, for example by treatment with
trifluoroacetic acid, then gives the hydroxylamine ether, 191.7.
The above procedure is also employed for the preparation of
substituted hydroxylamines which are precursors to
phosphonates.
Example 192
##STR00397##
[1274] The substrate, 190.1, in which the 20-ketone is protected as
the dimethyl hydrazone derivative, is reacted with a dialkyl
phosphonomethyl hydroxylamine, 192.1, prepared as described above
from a dialkyl trifluoromethyl-sulfonyl-oxymethyl phosphonate (Tet.
Lett., 1986, 27, 1477) and BOC-hydroxylamine, to afford the oxime,
192.2. Deprotection, as described in Example 191, then affords the
20-keto phosphonate, 192.3. The oxime forming reaction is performed
at ambient temperature in ethanol-acetic acid solution between
equimolar amounts of the reactants.
[1275] Using the above procedures, but employing, in place of the
hydroxyl-amine ether, 192.1, different oxime ethers, 191.1, the
corresponding products, 191.3 are obtained.
Example 193
##STR00398##
[1277] The dienone, 190.1, in which the 20-ketone is protected as
the dimethyl hydrazone, is reacted, as described above, with
O-(3-bromobenzyl)hydroxyl-amine, 193.1, prepared as described above
from 3-bromobenzyl bromide and BOC-protected hydroxylamine, 191.5,
to give the oxime, 193.2. The protecting group is then removed to
yield the 20-keto product 193.3. The latter product is then
reacted, in the presence of a palladium catalyst, with a dialkyl
phosphate, 193.4, to afford the phosphonate, 193.5. The preparation
of arylphosphonates by means of a coupling reaction between aryl
bromides and dialkyl phosphites is described in J. Med. Chem.,
1992, 35, 1371. The reaction is performed at ca. 100.degree. C. in
an inert solvent such as toluene, in the presence of a base such as
triethylamine and a catalytic amount of
tetrakis(triphenylphosphine)-palladium(0).
[1278] Alternatively, the bromo compound, 193.3, is coupled with a
dialkyl propenylphosphonate, 193.6, (Aldrich) to afford the
phosphonate, 193.7. The coupling of aryl halides with olefins by
means of the Heck reaction is described, for example, in F. A.
Carey and R. J. Sundberg, Advanced Organic Chemistry, 503ff
(Plenum, 2001) and in Acc. Chem. Res., 1979, 12, 146. The aryl
bromide and the olefin are coupled in a polar solvent such as
dimethylformamide or dioxan, in the presence of a palladium(0)
catalyst such as tetrakis(triphenyl-phosphine)palladium(0) or
palladium(II) catalyst such as palladium(II) acetate, and
optionally in the presence of a base such as triethylamine or
potassium carbonate. Optionally, the styrenoid double bond present
in the product, 193.7, is reduced, for example by reaction with
diimide, to produce the saturated analog, 193.8. The reduction of
olefinic bonds is described in R. C. Larock, Comprehensive Organic
Transformations, 6ff (VCH, 1989). The transformation is effected by
means of catalytic hydrogenation, for example using a palladium on
carbon catalyst and hydrogen or a hydrogen donor, or by the use of
diimide or diborane.
[1279] Using the above procedures, but employing, in place of the
bromobenzyl reagent, 193.1, different bromo-substituted aryl or
heteroaryl alkoxy hydroxyl-amines, and/or different dialkyl alkenyl
phosphonates, the products analogous to the compounds, 193.5, 193.7
and 193.8 are obtained.
Example 194
##STR00399##
[1281] The substrate, 190.1, in which the 20-ketone is protected as
the dimethylhydrazone, is reacted with a dialkyl 4-amino-2-furyl
phosphonate, 194.1, prepared by the palladium catalyzed coupling
reaction, as described above, between 4-amino-2-bromofuran (Tet.,
1987, 43, 3295) and a dialkyl phosphite, to give, after
deprotection, the imine product, 194.2. The imine forming reaction
is conducted in a hydrocarbon solvent such as toluene or xylene, at
reflux temperature, in the presence of a basic catalyst such as
sodium methoxide, or an acid catalyst such as p-toluenesulfonic
acid, under azeotropic conditions.
[1282] Using the above procedures, but employing, in place of the
4-aminofuryl phosphonate, 194.1, different amino-substituted aryl
or heteroaryl phosphonates, products analogous to 194.2 are
obtained.
Example 195
##STR00400##
[1284] The dienone, 190.1, in which the 20-ketone is protected as
the dimethylhydrazone, is reacted with 2-carboxyethyl
hydroxylamine, 195.1, (J. Med. Chem., 1990, 33, 1423) to yield the
oxime, 195.2. The reaction of steroidal 1,4-dien-3-ones with
hydroxylamines is described in J. Steroid Bioch., 1976, 7, 795; the
reaction is performed between equimolar amounts of the reactants in
a polar organic solvent such as pyridine or methanol, optionally in
the presence of acetic acid or sodium acetate. The product, 195.2,
is then coupled with a dialkyl 4-aminophenyl phosphonate, 195.3,
(Epsilon) and dicyclohexyl carbodiimide, to yield, after
deprotection, the amide oxime, 195.4. The preparation of amides
from carboxylic acids and derivatives is described, for example, in
S. R. Sandier and W. Karo, Organic Functional Group Preparations,
274 (Academic Press, 1968), and R. C. Larock, Comprehensive Organic
Transformations, 972ff (VCH, 1989). The carboxylic acid is reacted
with the amine in the presence of an activating agent, such as, for
example, dicyclohexylcarbodiimide or diisopropylcarbodiimide,
optionally in the presence of, for example, hydroxybenztriazole,
N-hydroxysuccinimide or N-hydroxypyridone, in a non-protic solvent
such as, for example, pyridine, DMF or dichloromethane, to afford
the amide.
[1285] Alternatively, the carboxylic acid may first be converted
into an activated derivative such as the acid chloride, anhydride,
mixed anhydride, imidazolide and the like, and then reacted with
the amine, in the presence of an organic base such as, for example,
pyridine, to afford the amide.
[1286] The conversion of a carboxylic acid into the corresponding
acid chloride can be effected by treatment of the carboxylic acid
with a reagent such as, for example, thionyl chloride or oxalyl
chloride in an inert organic solvent such as dichloromethane,
optionally in the presence of a catalytic amount of
dimethylformamide.
[1287] Using the above procedures, but employing, in place of the
carboxy-substituted hydroxylamine, 195.1, different
carboxy-substituted hydroxylamines, and/or different
amino-substituted phosphonates, the products analogous to 195.4 are
obtained.
Example 196
##STR00401##
[1289] The dienone, 190A, is reduced to afford the 1,2-dihydro
product, 196.1. The catalytic hydrogenation reaction is effected by
the use of tris(triphenyl-phosphine)rhodium (I) chloride, for
example as described in J. Med. Chem., 2001, 44:, 602. The product
is then reacted with ethyl formate and a base such as sodium
hydride, in an inert solvent such as toluene or dimethylformamide,
as described in J. Am. Chem. Soc., 1964, 86, 1520, to afford the
2-formyl product, 196.2. This compound is then reacted with an
alkyl, aralkyl, aryl or heteroaryl hydrazine, 196.3, in which the
substituent X is either a phosphonate group or a group which is
subsequently transformed into a phosphonate-containing substituent.
For example, X is dialkylphosphono, bromo, hydroxy, amino, carboxyl
and the like. The reaction yields the isomeric 2'- and 1'-aryl
pyrazoles, 196.4 and 196.5. The pyrazole-forming reaction is
performed between equimolar amounts of the reactants in an acidic
solvent such as acetic acid, as described in J. Am. Chem. Soc.,
1964, 86, 1520. The pyrazoles, 196.4 and 196.5, are then
transformed, for example, by the procedures described in Examples
192 and 193, into the phosphonates, 196.6 and 196.7. Optionally,
the reduction and formylation reactions are performed on the
substrate, 190.1, in which the 20-ketone is protected as the cyclic
ethylene ketal.
Example 197
##STR00402##
[1291] The ketoaldehyde, 196.2, is reacted, as described above,
with 3-hydroxy-phenyl hydrazine, 197.1, (JP 03011081) to give the
pyrazoles, 197.2 and 197.3. The 2'-substituted isomer, 197.2, is
then reacted in dimethylformamide solution at 70.degree. with one
molar equivalent of a dialkyl 2-bromoethyl phosphonate, 197.4,
(Aldrich) and potassium carbonate, to give the ethoxy phosphonate,
197.5.
[1292] The isomeric pyrazole, 197.3, is reacted in a Mitsonobu with
one molar equivalent of a dialkyl 3-hydroxypropyl phosphonate,
197.6, (Zh. Obschei. Khim., 1974, 44, 1834) to yield the
phosphonate, 197.7. The preparation of aromatic ethers by means of
the Mitsonobu reaction is described, for example, in R. C. Larock,
Comprehensive Organic Transformations, 448 (VCH, 1989), and in F.
A. Carey and R. J. Sundberg, Advanced Organic Chemistry, Part B,
153-4 (Plenum, 2001) and in Org. React., 1992, 42, 335. The phenol
and the alcohol or thiol component are reacted together in an
aprotic solvent such as, for example, tetrahydrofuran, in the
presence of a dialkyl azodicarboxylate and a triarylphosphine, to
afford the ether or thioether products. The procedure is also
described in Org. React., 1992, 42, 335-656.
[1293] Using the above procedures, but employing different
hydroxy-substituted hydrazines, and/or different bromo or
hydroxy-substituted phosphonates, the products analogous to 195.5
and 197.6 are obtained.
Example 198
##STR00403##
[1295] The ketoaldehyde, 196.2, is reacted, as described above,
with 4-amino-phenyl hydrazine, 198.1, (Syn. Comm., 1974, 4, 57) to
produce the pyrazoles, 198.2 and 198.3. The 2'-substituted isomer,
198.2, is then reacted in dimethylformamide solution at 70.degree.
with one molar equivalent of a dialkyl 3-bromopropyl phosphonate,
198.4, (J. Amer. Chem. Soc., 2000, 122, 1554) and cesium carbonate,
to give the amine phosphonate, 198.5.
[1296] Alternatively, the 1'-substituted pyrazole, 198.3, is
coupled with a dialkyl 4-hydroxymethylphenyl phosphonate, 198.6,
(U.S. Pat. No. 5,569,664) and carbonyl diimidazole to prepare the
carbamate phosphonate, 198.7. The preparation of carbamates is
described in Comprehensive Organic Functional Group
Transformations, A. R. Katritzky, ed., Pergamon, 1995, Vol. 6, p
416ff, and in Organic Functional Group Preparations, by S. R.
Sandler and W. Karo, Academic Press, 1986, p. 260ff. In the
procedure, the amine is reacted in an inert aprotic solvent such as
dichloromethane or tetrahydrofuran, with phosgene or a functional
equivalent thereof, such as carbonyl diimidazole, triphosgene,
pentafluorophenyl carbonate and the like, to afford the
corresponding activated acylamine. The latter compound is then
reacted with an alcohol to yield the carbamate.
[1297] Using the above procedures, but employing, in place of the
aminophenyl hydrazine, 198.1, different amino-substituted
hydrazines, and/or different dialkyl bromo or hydroxy-substituted
phosphonates, the products analogous to the compounds, 198.5 and
198.7 are obtained.
Example 199
##STR00404##
[1299] The ketoaldehyde, 196.2, is reacted with hydrazine to afford
the pyrazole derivative, 199.1. The reaction of steroidal
2-formyl-3-ketones with hydrazine is described in J. Am. Chem.
Soc., 1964, 86, 1520. The reaction is performed in acetic acid at
ambient temperature. The pyrazole product is then reacted with a
bromomethyl compound, 199.2, in which R.sup.2 and X are as defined
above, or a reactive bromoheteroaromatic reagent, to yield the
alkylation products, 199.3 and 199.4. The alkylation of substituted
pyrazoles is described, for example, in Heterocyclic Chemistry, by
T. L. Gilchrist, Longman, 1992, p. 309. The reaction is performed
between equimolar amounts of the substrates in a polar solvent such
as dimethylformamide or tetrahydrofuran, in the presence of a base
such as dimethylaminopyridine, lithium hexamethyldisilazide and the
like. The products, 199.3 and 199.4, are, except in cases where X
is dialkylphosphono, converted into the phosphonates, 199.5 and
199.6, using the procedures described herein.
Example 200
##STR00405##
[1301] The pyrazole, 199.1, is reacted in dimethylformamide
solution at 70.degree. C. with one molar equivalent of a dialkyl
4-bromobutenyl phosphonate, 200.1, (J. Med. Chem., 1992, 35, 1371)
and lithium hexamethyl disilazide, to give the pyrazoles, 200.2 and
200.3.
[1302] Using the above procedures, but employing different
bromo-substituted phosphonates, the products analogous to 200.2 and
200.3 are obtained.
Example 201
##STR00406##
[1304] The pyrazole, 199.1, is reacted in tetrahydrofuran solution
with 2,5-bis(bromomethyl)furan, 201.1, (Tet., 1999, 55, 4709) and
potassium hexamethyl disilazide, to give the alkylation products,
201.2 and 201.3. The 2'-substituted isomer, 201.2, is then reacted,
in a Arbuzov reaction, with a trialkyl phosphite to yield the
phosphonate, 201.4. The Arbuzov reaction is described in Handb.
Organophosphorus Chem., 1992, 115. In this procedure, in which a
bromo substituent is converted into the corresponding phosphonate,
the substrate is heated at from about 60.degree. to about
160.degree. with a five to fifty-fold molar excess of a trialkyl
phosphite, to effect the transformation.
[1305] The 1'-substituted pyrazole, 201.3, is reacted at ambient
temperature in dimethylformamide solution with one molar equivalent
of a dialkyl mercapto-methyl phosphonate, 201.5, (J. Med. Chem.,
1985, 26, 1688) and cesium carbonate, to give the thioether
phosphonate, 201.6.
[1306] Using the above procedures, but employing different
dihalides, and/or different mercapto-substituted phosphonates, the
products analogous to 201.4 and 201.6 are obtained.
Example 202
##STR00407##
[1308] Derivatives of the C-21 primary hydroxy group of the type,
202.1, are readily prepared by alkylating triamcinolone acetonide,
202A, with the appropriate phosphonate as shown.
Example 203
##STR00408##
[1310] After chemoselective extraction of the primary hydroxy
proton of compound, 202A, using one equivalent of sodium hydride,
the phosphonate triflate is added to provide the ether, 203.1.
Example 204
##STR00409##
[1312] The primary hydroxy group is masked by an appropriate
protecting group. After alkylation at the secondary hydroxy moiety
of, 204.1, with a leaving group-attached phosphonate and subsequent
deprotection, desired analog, 204.2, is obtained.
Example 205
##STR00410##
[1314] Triamcinolone acetonide, 202A, is chemoselectively protected
as its silyl ether using the standard TBSCl and imidazole
conditions (J. Am. Chem. Soc. 1972, 94, 6190). Alkylation at the
exposed secondary hydroxy group with sodium hydride and the
phosphonate triflate furnishes the intermediate, 205.6. Final TBAF
deprotection of the silyl ether affords the desired product,
205.7.
Example 206
##STR00411##
[1316] Phosphonate derivatives of the acetal are readily prepared
from acidic hydrolysis of triamcinolone acetonide, 202A, to the
diol, 206.1, as illustrated in Scheme 3.1. Acetylization of the
diol with a phosphonate aldehyde furnishes the desired acetal,
206.2.
Example 207
##STR00412##
[1318] Triamcinolone acetonide, 202A, is first hydrolized in
aqueous acetic acid. (Can. J. Chem. 1983, 61, 634) The resulting
diol, 207.1, is acetalized with the phosphonate aldehyde and
perchloric acid, affording the acetal, 207.2 (J. Med. Chem. 1996,
39, 4888-4896).
Example 208
##STR00413##
[1320] Derivatization at the C-11 hydroxy group is accomplished
through alkylation of rimexolone, 208A, with the appropriate
phosphonate, furnishing analogs of the type, 208.1.
##STR00414##
[1321] After sodium hydride extraction of the hydroxy proton in,
208A, diethyl phosphonate triflate is added to afford ether,
208.2.
Example 209
##STR00415##
[1323] Derivatives of the carbonyl at C-17 are readily prepared
from saponification of fluticasone, 209A, to the carboxylic acid,
209.1. Activation of the carboxylic acid, followed by reaction with
thiophosphonate or aminophosphonate nucleophile furnishes the
desired thioester, 209.2, and amide, 209.3, respectively.
Example 210
##STR00416##
[1325] Fluticasone, 209A, is first saponified with potassium
hydroxide in acetone. (Synthesis, 2002, 921-927) The resulting
carboxylic acid, 209.1, is activated to the carboxylic acid
imidazole by the addition of 1,1'-carbonyldiimidazole (CDI) (J.
Med. Chem. 1994, 37, 3717-3729). Treatment with the thiophosphonate
affords thioester, 210.1. Magnesium ethoxide may be added to help
enhance the reactivity (Tetrahedron Lett. 1981, 22, 3245-3246).
Alternatively, the carboimidazole intermediate derived from, 209.1,
can be reacted with the aminophosphonate to produce amide,
210.2.
Example 211
##STR00417##
[1327] The less sterically hindered C-11 hydroxy group is
selectively alkylated with the appropriate phosphonate to give
analogs of formula, 211.1.
Example 212
##STR00418##
[1329] After regioselective extraction of the C-11 hydroxy proton
in, 209A, using one equivalent of sodium hydride, the phosphonate
triflate is added to provide the ether, 212.1.
Example 213
##STR00419##
[1331] The C-11 hydroxy group is masked by an appropriate
protecting group. After alkylation at the C-17 hydroxy moiety of,
213.1, with a leaving group-attached phosphonate and subsequent
deprotection, desired analog, 213.3, is obtained.
Example 214
##STR00420##
[1333] Fluticasone 209A is regioselectively protected as its C-11
acetate ester using the standard acetic anhydride and DMAP
conditions (J. Org. Chem. 1998, 63, 2342-2347). Alkylation at the
exposed C-17 hydroxy group with sodium hydride and the phosphonate
triflate furnishes the intermediate, 214.2. Final ammonia
deprotection of the acetate affords the desired ether, 214.3.
Example 215
##STR00421##
[1335] Derivatization at the C-11 hydroxy group is accomplished
through alkylation of mometasone fuorate, 215A, with the
appropriate phosphonate, furnishing analogs of the type, 215.1.
Example 216
##STR00422##
[1337] After sodium hydride extraction of the hydroxy proton in
215A, diethyl phosphonate triflate is added to afford ether,
216.1.
Example 217
##STR00423##
[1339] Following protection of the only exposed hydroxy group in
mometasone fuorate, 215A, intermediate, 217.1, is saponified to
give alcohol, 217.3. Alkylation at the C-17 hydroxy group with the
appropriate phosphonate and subsequent deprotection provides the
desired product, 217.4.
Example 218
##STR00424##
[1341] Mometasone fuorate, 215A, is protected as its silyl ether
using the standard TBSCl and imidazole conditions (J. Am. Chem.
Soc., 1972, 94, 6190). Saponification of the fuoryl ester moiety
using aqueous sodium hydroxide provides the alcohol, 218.1 (J.
Chem. Soc. Perkin Trans. 1, 1993, 12, 1359-1366). The tertiary
hydroxy group is alkylated by the addition of sodium hydroxide and
the phosphonate triflate. After deprotection of the silyl ether in
intermediate, 218.3, with TBAF, diethyl phosphonate, 218.4,
results.
Example 219
##STR00425##
[1343] Derivatization at the C-11 hydroxy group is accomplished
through alkylation of methylprednisolone aceponate (219A) with the
appropriate phosphonate, furnishing analogs of Example 219.1.
Example 220
##STR00426##
[1345] After sodium hydride extraction of the hydroxy proton in
219A, diethyl phosphonate triflate is added to afford ether,
220.1.
Example 221
##STR00427##
[1347] Following protection of the only exposed hydroxy group in
219A, intermediate, 221.1, is saponified to give diol, 221.2.
Alkylation at the primary hydroxy group with the appropriate
phosphonate and subsequent acylation provides the propionate ester,
221.4. The desired product, 221.5, is achieved after
deprotection.
Example 222
##STR00428##
[1349] Methylprednisolone aceponate, 219A, is protected as its
silyl ether using the standard TBSCl and imidazole conditions (J.
Am. Chem. Soc., 1972, 94, 6190). Saponification of both ester
moieties using aqueous sodium hydroxide provides the diol, 222.2.
The less sterically hindered primary hydroxy group is alkylated by
the addition of sodium hydroxide and the phosphonate triflate.
After treating intermediate, 222.3, with propionic anhydride in
pyridine, the previously hydrolized C-17 propionic ester is
replaced (J. Med. Chem., 1980, 23, 430-437). TBAF deprotection of
the silyl ether furnishes diethyl phosphonate, 222.5.
Example 223
##STR00429##
[1351] The two hydroxy groups of diol, 221.2, are regioselectively
differentiated by protection at the primary site, thus allowing
alkylation at the tertiary hydroxy group. The resulting phosphonate
intermediate, 223.1, is then deprotected to afford the diol, 223.3.
Again the more accessible primary hydroxy group is acylated to
produce the desired analog, 223.4.
Example 224
##STR00430##
[1353] Diol, 222.2, is alkylated with the diethyl phosphonate
triflate, the resulting intermediate, 224.2, is treated with TBAF
to give diol, 224.3. Acetic anhydride and pyridine are used to
generate the final product, 224.4 (J. Mol. Biol., 1972, 72,
219).
Example 225
##STR00431##
[1355] Compounds such as, 225.1, can be made according to the
general route outlined below.
##STR00432##
Example 226
##STR00433##
[1357] PNP-405, 225A, is prepared according to the method of
Littler, B. J. et al., 7.sup.th International Conference on Organic
Process Research and Development, New Orleans, La., Mar. 16-19,
2003. PNP-405 is treated in a solvent such as tetrahydrofuran or
dimethylformamide with a base such as sodium hydride. When bubbling
ceases, diethyl phosphonomethyltriflate (prepared according to
Tetrahedron Lett., 1986, 27, 1477) is added, to provide compound,
226.1, as the desired product.
Example 227
##STR00434##
[1359] Compounds such as 227.1 (where X.dbd.O, Z=CH.sub.2OH), can
be prepared according to the procedure of Littler, B. J. et al.,
7.sup.th International Conference on Organic Process Research and
Development, New Orleans, La., Mar. 16-19, 2003 (Schemes 3 and 4).
The starting material, 2-benzyloxyphenylacetic acid, 227.1,
(provided by Avocado) can be acylated via the mixed anhydride with
the oxazolidinone shown at 80-85.degree. C., with triethylamine as
base to provide compound, 227.2. A low-temperature alkylation with
bromoacetonitrile results in the formation of compound, 227.3, with
good diastereomeric ratio. Removal of the chiral auxiliary under
reductive conditions yields compound, 227.4, without racemization.
Protection of the resulting alcohol with the trityl group provides
compound, 227.5. Subsequent pyrrole ring construction as well as
cyclo-guanidinylation reaction to prepare the six-membered
2-aminopyrimidone ring is performed as described in Example 228 for
compound, 228.9, to provide compound, 227.6.
Example 228
##STR00435## ##STR00436##
[1361] Compound, 228.1, (where X.dbd.O, Z=H) can be prepared
according to the general route outlined above. The starting
material, 3-(2-benzyloxy-phenyl)-propionitrile, 228.1, is available
by Lewis acid-mediated reaction of phenol with acrylonitrile
according to U.S. Pat. No. 2,789,995, published in 1954.
Intermediate, 227.5, can follow the same synthetic steps as
outlined here to provide compound, 227.1.
[1362] Pyrrole ring construction can be completed in three steps
from 3-(2-benzyloxy-phenyl)-propionitrile, 228.1. Formation of
3-hydroxy-acrylonitrile, 228.2, can be achieved by exposure of,
228.1, to LDA and ethyl formate. Condensation of this product with
2-Amino-malonic acid diethyl ester in EtOH and sodium acetate
yields compound, 228.3, which undergoes a decarboxylative
cyclization in the basic medium of NaOH and EtOH to provide
pyrrole, 228.4. In case of compound, 227.1, synthesis, the trityl
protecting group on the benzylic alcohol is removed at this stage.
Subsequently, guanidinylation reaction using cyanamide provides
compound, 228.5, which, upon treatment with sodium hydroxide,
cyclizes to form the 2-aminopyrimidone ring (compound, 228.6).
Removal of the phenolic protecting group under hydrogenolysis
conditions provides the free phenol, which is used as the
attachment site for the pro-drug group. A variety of linkers may be
utilized to attach the pro-drug moiety to the backbone molecule. A
particular example in which diethyl phosphono-methyltriflate is
used as the starting materials is shown is above. Therefore,
compound, 228.7, is treated in a solvent such as tetrahydrofuran or
dimethylformamide with a base such as sodium hydride or cesium
carbonate. When bubbling ceases, diethyl phosphonomethyltriflate
(prepared according to Tetrahedron Lett., 1986, 27, 1477) is added,
to provide compound, 228.2, as the desired product.
Example 229
##STR00437##
[1364] Compounds such as, 229.1, (where X.dbd.O, Y.dbd.H,
Z=CH.sub.2OH) can be prepared from 4-benzyloxyphenylacetic acid
(available from Aldrich). Following a similar sequence to that
demonstrated above, intermediate, 229.5, can be prepared.
Proceeding with the sequence shown above, 229.5, can be transformed
to the desired product, 229.1.
##STR00438##
[1365] Compounds such as, 230A, can be made according to the
general route outlined above.
Example 231
##STR00439##
[1367] Preparation of DADMe-ImmG is reported in Lewandowics A. et
al., Biochemistry, 2003, 42, 6057. The tertiary nitrogen of the
ring may not interfere with the alkylation of the secondary alcohol
and in that case does not need to be protected, although standard
protection and deprotection protocols as described in Greene, T.,
Protective Groups in Organic Synthesis, Wiley-Interscience, 1999
may be used if necessary. Reaction of the primary alcohol, 231.1,
with base followed by addition of the appropriately activated
phosphonate yields the protected product. Global deprotection
yields the desired phosphonate, 231.2.
Example 232
##STR00440##
[1369] Compounds such as, 232.1, can be made according to the
general route outlined above.
Example 233
##STR00441##
[1371] The protected DADMe derivative can be treated with treated
in a solvent such as tetrahydrofuran or dimethylformamide with a
base such as sodium hydride. When bubbling ceases, diethyl
phosphonoethylltriflate (prepared according to Tetrahedron Lett.,
1986, 27, 1477) is added, yielding the desired phosphonate ester.
Removal of the protecting group can be performed as described in
Greene, T., Protective Groups in Organic Synthesis,
Wiley-Interscience, 1999 to provide the desired phosphonate ester,
233.1.
Example 234
##STR00442##
[1373] Compounds such as, 234.2, can be made according to the
general route outlined above.
##STR00443##
[1374] CP-690,550,
3-{4-methyl-3-[methyl-(7H-pyrrolo[2,3-d]pyrimidin-4-yl)-amino]-piperidin--
1-yl}-3-oxo-propionitrile, 234.1, can be prepared as described in
WO 02096909 and WO 03048162. Enolate formation at the
.alpha.-cyanoamide position using over 2 equivalents of base
followed by addition of diethyl phosphonomethyltriflate (prepared
according to Tetrahedron Lett., 1986, 27, 1477) yields the desired
compound, 234.3. A solvent such as THF, DMF or other anhydrous
solvents may be used for this reaction. In case the pyrrole
nitrogen interferes with the desired alkylation, a protecting group
such as BOC may be introduced before the alkylation reaction.
Removal of the BOC group can be accomplished by exposure of the
reaction product to TFA as described in Greene, T., Protective
groups in Organic Synthesis, Wiley-Interscience, 1999.
Example 235
##STR00444##
[1376] Compound, 235.1, is prepared according to WO 02096909.
Protection of the pyrrole nitrogen using a tosyl group is achieved
as described in Sakamoto, T. et al., Tetrahedron Lett. 1994, 35,
18, 2919. Ortho lithiation using t-BuLi and quenching with
formaldehyde as described in the above reference as well as Seela,
F. et al., Chem. Ber. 1977, 110, 4, 1462 introduces a substituent
at the requisite site. The primary alcohol so formed may be used
for attachment of the phosphonate moiety via ether formation using
base and diethyl phosphono-methyltriflate (prepared according to
Tetrahedron Lett., 1986, 27, 1477) in an anhydrous solvent. Removal
of the benzyl protecting group is achieved using hydrogenolysis
conditions. The piperidine nitrogen is then coupled with
cyano-acetic acid 2,5-dioxo-pyrrolidine-1-yl ester to provide
compound, 235.5. Removal of the tosyl protecting group can be
achieved using basic conditions to provide the desired product,
235.6.
Example 236
##STR00445##
[1378] Specifically,
(1-benzyl-4-methyl-piperidin-3-yl)-methyl-(7H-pyrrolo[2,3-d]pyrimidin-4-y-
l)-amine, compound, 236.1, (prepared as described in WO 02,096,909)
is first protected on the pyrrole nitrogen using a tosyl group.
Subsequent formylation using the procedure reported by Sakamoto, T.
et al., (Tetrahedron Lett. 1994, 35, 2919) provides compound,
236.3. The primary alcohol is then treated in a solvent such as
tetrahydrofuran or dimethyl-formamide with a base such as sodium
hydride. When bubbling ceases, diethyl phosphonomethyltriflate
(prepared according to Tetrahedron Lett., 1986, 27, 1477) is added,
yielding the desired product, 236.4. Debenzylation of the
piperidine nitrogen following by coupling to cyano-acetic acid
2,5-dioxo-pyrrolidine-1-yl ester gives compound, 236.5. Removal of
the tosyl protecting group provides the desired pro-drug,
236.6.
Example 237
##STR00446##
[1380] The syntheses of phosphonate compounds of the invention and
of intermediate compounds necessary for their synthesis are
illustrated herein.
Example 238
##STR00447##
[1382] The preparation of phosphonates of phosphonate compounds of
the invention is illustrated above. The
5-hydroxy-1-.beta.-D-ribofuranosyl-1H-imidazole-4-carboxamide,
238.1 (prepared according to U.S. Pat. No. 3,888,843), can be
treated in a solvent such as tetrahydrofuran or dimethyl-formamide
with a base such as sodium hydride. When bubbling ceases, diethyl
phosphonomethyltriflate (prepared according to Tetrahedron Lett.,
1986, 27, 1477) is added, yielding the desired phosphonate diester
238.2.
Example 239
##STR00448##
[1384] The preparation of the phosphonate esters is illustrated
above. Compound 239.1,
5-hydroxy-1-(4-hydroxy-5-hydroxymethyl-tetrahydro-furan-2-ylmethyl)-1H-im-
idazole-4-carboxylic acid amide, prepared by addition of the
imidazole base (JP Kokai 76 88965) onto the 3,5-bis-protected
2-deoxy-D-erythro-pentofuranosyl chloride (Hayashi, M. et al.,
Chem. Pharm. Bull., 1975, 23, 1, 245; Montgomery, J. A. et al., J.
Med. Chem., 1969, 12, 3, 498; and Iwamoto, R. H. et al., J. Med.
Chem., 1963, 6, 684), is protected on the imidazol-4-ol. Oxidation
of the 5'-OH followed by elimination provides glycal, 239.2. (See
the procedure in Zemlicka J. et al., J. Am. Chem. Soc., 1972, 94,
9, 3213.) Selenoetherification provides the protected phosphonate,
239.3 (Kim, C. et al., J. Org. Chem., 1991, 56, 2642). Oxidative
elimination of the phenylselenide (as described in Kim, C. et al.,
J. Org. Chem., 1991, 56, 2642) followed by stereoselective
dihydroxylation provides the diol 239.4. Finally, the protecting
group is removed to provide compound 239.5.
Example 240
##STR00449## ##STR00450##
[1386] The preparation of the phosphonatesis illustrated above.
Specifically, compound 239.1,
5-hydroxy-1-(4-hydroxy-5-hydroxymethyl-tetrahydrofuran-2-ylmethyl)-1H-imi-
dazole-4-carboxylic acid amide, is first protected using a TBS
group. Subsequent oxidation with PtO.sub.2 proceeds to provide
carboxylic acid 240.1. Decarboxylative elimination is achieved
using dimethylformamide dineopentyl acetal in DMF at high
temperature (Zemlicka J. et al., J. Am. Chem. Soc., 1972, 94, 9,
3213). Once the furanoid glycal 240.2 is in hand, it is treated
with silver perchlorate in the presence of
diethyl(hydroxylmethyl)phosphonate (Phillion, D. et al.,
Tetrahedron Lett., 1986, 27, 1477) to provide the phosphonate 240.3
(Kim, C. et al., J. Org. Chem., 1991, 56, 2642). Oxidative
elimination of the selenide followed by dihydroxylation using
osmium tetraoxide provides a diol, 240.5, with the desired
stereochemistry. Deprotection of the TBS group can be achieved
using TBAF to provide compound 240.6.
Example 241
[1387] The synthesis of compounds of the invention that are analogs
of CsA, 241A, (and related cyclosporins) are shown herein.
##STR00451##
Example 242
##STR00452##
[1389] The syntheses of phosphonate compounds of the invention and
of intermediate compounds necessary for their synthesis are
illustrated herein. The olefin metathesis methodology is described
in J. Med. Chem., 2003, 46, 674.
Example 243
##STR00453##
[1391] The preparation of compounds of the invention having
phosphonate groups and intermediate compounds useful for their
synthesis are illustrated herein.
Example 244
##STR00454##
[1393] The preparation of compounds of the invention having
phosphonate groups and intermediate compounds useful for their
synthesis are illustrated herein.
Example 245
##STR00455##
[1395] The conversion of various substituents into the group
link-P(O)(OR.sup.1).sub.2, where R.sup.1 is as defined above, or
indeed the final stage of P(O)RR.sup.o, as defined above, can be
effected at any convenient stage of the synthetic sequence, or in
the final step. The selection of an appropriate step for the
introduction of the phosphonate substituent is made after
consideration of the chemical procedures required and the stability
of the substrates to those procedures. It may be necessary to
protect reactive groups, for example hydroxyl, amino, during the
introduction of the group link-P(O)(OR.sup.1).sub.2 or
P(O)RR.sup.o. Specific examples of compounds of the invention
having formulae, 245.5-245.8, are shown herein.
##STR00456##
[1396] The compounds of the invention are synthesized according to
the methods described herein. Exemplary intermediate phosphonate
esters are shown, wherein R.sup.1 is hydrogen, alkyl, aryl,
haloalkyl, alkenyl, aralkyl, or aryl. These compounds can be used
to prepare the compounds of the invention, such as those
illustrated herein, by one skilled in the art, using known methods
for synthesis of substituted phosphonates. These methods are
similar to those described for the synthesis of amides. The
preparation of amides from carboxylic acids and derivatives is
described, for example, in "Organic Functional Group Preparations,"
by S. R. Sandler and W. Karo, Academic Press, 1968, p. 274. Further
methods described in the following Examples for the synthesis of
the phosphonate diesters and can in some cases be applied to the
synthesis of phosphoramides.
[1397] The phosphonate esters, 245.1-245.4, for conversion into the
phosphonate moieties bearing an amino acid, or a lactate esters are
shown in herein. Cyclosporin A (CsA) 245.10, can be purchased from
Sigma Aldrich, synthesized (See U.S. Pat. No. 4,396,542) or
obtained from biological sources as described in U.S. Pat. No.
4,117,118. Other cyclosporin derivatives can be either synthetic in
nature (See U.S. Pat. No. 4,396,542) or isolated by similar means
to CsA (See U.S. Pat. No. 6,410,696 B1).
##STR00457##
[1398] The preparation of the phosphonate linkage to CsA through
the hydroxyl group of amino acid 1 to give compounds of formula
245.1 is illustrated herein. CsA, 245.10, is dissolved in a
suitable solvent such as, for example, DMF or other non-protic
solvent, and is then treated with the phosphonate reagent, 245.9,
bearing a leaving group, for example, bromine, mesyl, tosyl, or
trifluoro-methanesulfonyl in the presence of a suitable organic or
inorganic base.
##STR00458##
[1399] For example, 245.10 dissolved in DMF, is treated with one
equivalent of sodium hydride and one equivalent of
(toluene-4-sulfonylmethyl)-phosphonic acid dibenzyl ester 245.11,
prepared according to the procedures in J. Org. Chem. 1996, 61,
7697, to give CsA phosphonate 245.5. Using the above procedure but
employing different phosphonate reagents, 245.9, in place of
compound, 245.11, there are obtained the corresponding products,
245.1, bearing different linking groups.
Example 246
##STR00459## ##STR00460##
[1401] The preparation of CsA--phosphonate conjugates is
illustrated above. The hydroxyl group of amino acid 1 is first
protected with a suitable protecting group, for example silyl
ethers, benzyl ethers, trityl ethers etc as described in Greene and
Wuts, "Protecting Groups in Organic Synthesis," 3.sup.rd Edition,
John Wiley and Sons, Inc. The protected product, 246.1, is then
treated with an oxidizing agent, many examples of which are
described in "Comprehensive Organic Transformations," John Wiley
& Sons, 2.sup.nd Ed, R. C. Larock, p 1211-1215 to give the
aldehyde, 246.2.
[1402] Aldehyde, 246.2, is then treated with a amine phosphonic
acid ester of the general formula 246.3 under reductive amination
conditions to afford amine, 246.4. The preparation of amines by
means of reductive amination procedures is described, for example,
in "Comprehensive Organic Transformations," by R. C. Larock,
2.sup.nd edition, p. 835. In this procedure, the amine component
and the aldehyde component are reacted together in the presence of
a reducing agent such as, for example, borane, sodium
cyanoborohydride or diisobutylaluminum hydride, to yield the amine
product. Finally, deprotection of the hydroxyl group following
procedures documented in Greene and Wuts, "Protecting Groups in
Organic Synthesis," 3.sup.rd Edition, John Wiley and Sons Inc. p
116-121 gives the phosphonate 246.5.
Example 247
##STR00461## ##STR00462##
[1404] For example, 245.10, is treated in pyridine and
dichloromethane with trimethylsilyl chloride, as described in U.S.
Pat. No. 6,410,696 B1, to give silyl ether, 247.1. Silyl ether,
247.1, is then treated with ozone followed by work up with dimethyl
sulfide to give aldehyde 247.2. Aldehyde, 247.2, is treated with
one equivalent of the hydrochloride salt of
(2-amino-ethyl)-phosphonic acid ester diethyl ester, 247.3,
prepared according to J. Med. Chem., 1998, 41, 23, p 4439, and a
suitable base, e.g. hunigs base, triethylamine, or the likes, until
the imine is formed. The intermediate imine solution is then
treated with sodium cyanoborohydride to give the amine, 247.4.
Amine, 247.4, is then deprotected by treatment with TBAF in an
aprotic solvent such as THF or dioxane to give phosphonate, 247.5.
Using the above procedure but employing different phosphonate
reagents, 246.3, in place of phosphonate, 247.3, there are obtained
the corresponding products, 246.5, bearing different linking
groups.
Example 248
##STR00463##
[1406] The preparation of CsA phosphonate conjugates where the
phosphonate is linked onto the alanine nitrogen in amino acids 7
and 8, compounds, 245.3 and 245.4, is illustrated herein. Protected
CsA, 246.1 (Example 246), is treated with a base, sufficiently
basic to remove the amide proton, for example, metal hydrides,
metal amides. The product is then treated with a phosphonate
reagent, 245.9, bearing a leaving group such as, for example,
bromine, mesyl, tosyl, or trifluoromethanesulfonyl phosphonates, to
give 248.1 and 248.2. The alkylated products are then separated by
chromatography and independently deprotected using conventional
conditions described in Greene and Wuts, "Protecting Groups in
Organic Synthesis," 3.sup.rd Edition, John Wiley and Sons Inc. p
116-121 to give compounds having Formulae, 245.3 and 245.4.
Example 249
##STR00464##
[1408] Silyl ether, 247.1, in toluene is treated with sodium
hydride and 15-crown-5-ether followed by one equivalent of
bromomethyl phosphonic acid diallyl ester, 249.1 (Lancaster), to
give phosphonates, 249.2 and 249.3, respectively. Phosphonates,
249.2 and 249.3, are deprotected by treatment with TBAF in an
aprotic solvent such as THF or dioxane to give compounds having
Formulae, 249.4 and 249.5, respectively, wherein the linkage is a
methylene group. Using the above procedure but employing different
phosphonate reagents, 245.9, in place of phosphonate reagents,
249.1, there are obtained the corresponding products having
Formulae, 245.3 and 245.4, with different linking groups.
Example 250
[1409] The preparation of compounds of the invention having
phosphonate groups and intermediate compounds useful for their
synthesis are illustrated herein. The substructure on the right is
meant to represent Cyclosporin A in the following examples.
##STR00465## ##STR00466##
Example 251
cyclo-[[(2S,3R,4R,6E)-7-(4-Acetoxyphenyl)-4-methyl-3-hydroxy-2-(methylamin-
o)-6-heptenoyl]-L-2-aminobutyryl-sarcosyl-N-methyl-L-leucyl-L-valyl-N-meth-
yl-L-leucyl-L-alanyl-D-alanyl-N-methyl-L-leucyl-N-methyl-L-leucyl-N-methyl-
-L-valyl]
##STR00467##
[1411] A mixture of cyclosporin A (360 mg, 0.3 mmol),
4-acetoxystyrene (730 mg, 4.5 mmol) and
(1,3-bis-(2,4,6-trimethylphenyl)-2-imidazolidene)dichloro-(O-isopropoxyph-
enylmethylene)ruthenium (Hoveyda-Grubbs catalyst, 20 mg, 0.032
mmol) in dichloromethane (1 mL) was purged with nitrogen and
stirred under reflux for 16 hours. After cooling, the reaction
mixture was purified by silica gel column chromatography using
MeOH--CH.sub.2Cl.sub.2 to provide the product as a solid (395 mg,
99%).
[1412] MS (m/z) 1322.9 [M+H].sup.+, 1344.9 [M+Na].sup.+; HPLC
retention time 3.3 min. (relative to 4.1 min. of cyclosporin A;
Phenominex Synergi 4 micron hydro-RP 80A 50.times.4.6 mm; solvents,
35% water and 65% acetonitrile; flow rate 2 mL/min.; column
temperature 60.degree. C.).
Example 252
cyclo-[[(2S,3R,4R,6E)-7-(4-Hydroxyphenyl)-4-methyl-3-hydroxy-2-(methylamin-
o)-6-heptenoyl]-L-2-aminobutyryl-sarcosyl-N-methyl-L-leucyl-L-valyl-N-meth-
yl-L-leucyl-L-alanyl-D-alanyl-N-methyl-L-leucyl-N-methyl-L-leucyl-N-methyl-
-L-valyl]
##STR00468##
[1414] A solution of
cyclo-[[(2S,3R,4R,6E)-7-(4-acetoxyphenyl)-4-methyl-3-hydroxy-2-(methylami-
no)-6-heptenoyl]-L-2-aminobutyryl-sarcosyl-N-methyl-L-leucyl-L-valyl-N-met-
hyl-L-leucyl-L-alanyl-D-alanyl-N-methyl-L-leucyl-N-methyl-L-leucyl-N-methy-
l-L-valyl] (385 mg, 0.29 mmol) and triethylamine (1 mL) in MeOH (10
mL) was stirred at ambient temperature for 16 hours. The reaction
mixture was concentrated in vacuo and the residue was purified by
silica gel column chromatography using MeOH--CH.sub.2Cl.sub.2 to
provide the desired product (310 mg, 83%).
[1415] MS (m/z) 1280.9 [M+H].sup.+, 1278.8 [M-H].sup.-; HPLC
retention time 1.6 min. (relative to 4.0 min. of cyclosporin A;
Phenominex Synergi 4 micron hydro-RP 80A 50.times.4.6 mm; solvents,
35% water and 65% acetonitrile; flow rate 2 mL/min.; column
temperature 60.degree. C.).
Example 253
cyclo-[[(2S,3R,4R,6E)-7-(4-(Diethoxyphosphorylmethoxy)-phenyl)-4-methyl-3--
hydroxy-2-(methylamino)-6-heptenoyl]-L-2-amino-butyryl-sarcosyl-N-methyl-L-
-leucyl-L-valyl-N-methyl-L-leucyl-L-alanyl-D-alanyl-N-methyl-L-leucyl-N-me-
thyl-L-leucyl-N-methyl-L-valyl]
##STR00469##
[1417] To a mixture of
cyclo-[[(2S,3R,4R,6E)-7-(4-hydroyphenyl)-4-methyl-3-hydroxy-2-(methylamin-
o)-6-heptenoyl]-L-2-aminobutyryl-sarcosyl-N-methyl-L-leucyl-L-valyl-N-meth-
yl-L-leucyl-L-alanyl-D-alanyl-N-methyl-L-leucyl-N-methyl-L-leucyl-N-methyl-
-L-valyl] (113 mg, 0.088 mmol) and cesium carbonate (33 mg, 0.1
mmol) in DMF (1 mL) was added trifluoromethanesulfonic acid
diethoxyphosphorylmethyl ester (60 mg, 0.2 mmol). The mixture was
stirred at room temperature for 16 hours. The reaction was quenched
with 2% aqueous lithium chloride and the mixture was extracted with
ethyl acetate. The ethyl acetate extract was concentrated in vacuo.
The residue was purified by silica gel column chromatography to
provide the desired product (310 mg, 83%) contaminated with the
unreacted starting materials, which was further purified by RP HPLC
using a Phenomenex Synergi 5.mu. Hydro RP 80A column (50.times.21.2
mm) with eluents of H.sub.2O--CH.sub.3CN. The fractions containing
the desired product were pooled and concentrated to dryness (62 mg,
49%).
[1418] MS (m/z) 1431.0 [M+H].sup.+, 1428.7 [M-H].sup.-; .sup.31P
(121.4 MHz, CDCl.sub.3) .delta. 19.5.
Example 254
cyclo-[[(2S,3R,4R,6E)-7-(4-(Dibenzyloxyphosphorylmethoxy)phenyl)-4-methyl--
3-hydroxy-2-(methylamino)-6-heptenoyl]-L-2-aminobutyryl-sarcosyl-N-methyl--
L-leucyl-L-valyl-N-methyl-L-leucyl-L-alanyl-D-alanyl-N-methyl-L-leucyl-N-m-
ethyl-L-leucyl-N-methyl-L-valyl]
##STR00470##
[1420] To a mixture of
cyclo-[[(2S,3R,4R,6E)-7-(4-hydroyphenyl)-4-methyl-3-hydroxy-2-(methylamin-
o)-6-heptenoyl]-L-2-aminobutyryl-sarcosyl-N-methyl-L-leucyl-L-valyl-N-meth-
yl-L-leucyl-L-alanyl-D-alanyl-N-methyl-L-leucyl-N-methyl-L-leucyl-N-methyl-
-L-valyl] (300 mg, 0.234 mmol) and cesium carbonate (326 mg, 1
mmol) in DMF (2 mL) was added trifluoromethanesulfonic acid
dibenzyloxyphosphorylmethyl ester (60 mg, 0.2 mmol). The mixture
was stirred at room temperature for 16 hours. The reaction mixture
was filtered through Acrodisc (13 mm syringe filter with 0.45
micron Nylon membrane) and purified by RP HPLC using a Phenomenex
Synergi 5.mu. Hydro RP 80A column (50.times.21.2 mm) with eluents
of H.sub.2O--CH.sub.3CN. The fractions containing the desired
product were pooled and concentrated to dryness, affording a white
solid (115 mg, 32%).
[1421] MS (m/z) 1554.9 [M+H].sup.+, 1552.7 [M-H].sup.-; .sup.31P
(121.4 MHz, CDCl.sub.3) .delta. 20.5.
Example 255
cyclo-[[(2S,3R,4R,6E)-7-(4-(Dihydroxyphosphorylmethoxy)phenyl)-4-methyl-3--
hydroxy-2-(methylamino)-6-heptenoyl]-L-2-aminobutyryl-sarcosyl-N-methyl-L--
leucyl-L-valyl-N-methyl-L-leucyl-L-alanyl-D-alanyl-N-methyl-L-leucyl-N-met-
hyl-L-leucyl-N-methyl-L-valyl]
##STR00471##
[1423] To a mixture of
cyclo-[[(2S,3R,4R,6E)-7-(4-(dibenzyloxyphosphorylmethoxy)phenyl)-4-methyl-
-3-hydroxy-2-(methylamino)-6-heptenoyl-L-2-aminobutyryl-sarcosyl-N-methyl--
L-leucyl-L-valyl-N-methyl-L-leucyl-L-alanyl-D-alanyl-N-methyl-L-leucyl-N-m-
ethyl-L-leucyl-N-methyl-L-valyl] (115 mg, 0.074 mmol) and
2,6-lutidine (40 .mu.L, 0.35 mmol) in dichloromethane (2 mL) was
added trimethylsilyl bromide (50 .mu.L, 0.35 mmol). The mixture was
stirred at room temperature for 2 hours. The reaction was quenched
with methanol (1 mL) and the mixture was concentrated. The residue
was treated with a solution of ammonium fluoride (0.5 M, 2 mL),
stirred for 1 hour, concentrated, and partitioned between
dichloromethane and 1 N HCl. The dichloromethane layer was
concentrated and the crude product was purified by RP HPLC using a
Phenomenex Synergi 5.mu. Hydro RP 80A column (50.times.21.2 mm)
with eluents of 0.1% TFA H.sub.2O--0.1% TFA CH.sub.3CN. The
fractions containing the desired product were pooled and
concentrated to dryness, affording a hygroscopic solid (68 mg,
63%).
[1424] MS (m/z) 1374.9 [M+H].sup.+, 1373.1 [M-H].sup.-; HPLC
retention time 0.3 min. (relative to 4.0 min. of cyclosporin A;
Phenominex Synergi 4 micron hydro-RP 80A 50.times.4.6 mm; solvents,
35% water and 65% acetonitrile; flow rate 2 mL/min.; column
temperature 60.degree. C.).
Example 256
cyclo-[[(2S,3R,4R,6E)-7-(4-(1-(S)-Ethoxycarbonylethoxy)-phenoxyphosphorylm-
ethoxy)phenyl)-4-methyl-3-hydroxy-2-(methylamino)-6-heptenoyl]-L-2-aminobu-
tyryl-sarcosyl-N-methyl-L-leucyl-L-valyl-N-methyl-L-leucyl-L-alanyl-D-alan-
yl-N-methyl-L-leucyl-N-methyl-L-leucyl-N-methyl-L-valyl]
##STR00472##
[1426] A mixture of
cyclo-[[(2S,3R,4R,6E)-7-(4-(dihydroxyphosphorylmethoxy)phenyl)-4-methyl-3-
-hydroxy-2-(methylamino)-6-heptenoyl]-L-2-aminobutyryl-sarcosyl-N-methyl-L-
-leucyl-L-valyl-N-methyl-L-leucyl-L-alanyl-D-alanyl-N-methyl-L-leucyl-N-me-
thyl-L-leucyl-N-methyl-L-valyl] (34 mg, 0.023 mmol), phenol (22 mg,
0.23 mmol), dicyclohexylcarbodiimide (47 mg, 0.23 mmol) and
4-(N,N-dimethylamino)pyridine (5.6 mg, 0.046 mmol) in DMF (2 mL)
was stirred at 140.degree. C. for 20 min. After cooling, the
monophenyl mono-phosphonic acid product was purified by RP HPLC
using a Phenomenex Synergi 5.mu. Hydro RP 80A column (50.times.21.2
mm) with eluents of 0.1% TFA H.sub.2O--0.1% TFA CH.sub.3CN. MS
(m/z) 1450.9 [M+H].sup.+, 1449.1 [M-H].sup.-; .sup.31P (121.4 MHz,
CDCl.sub.3) .delta. 14.9. This intermediate was mixed with ethyl
(S)-(-)-lactate (40 mg, 0.34 mmol), PyBOP (80 mg, 0.15 mmol),
diisopropylethylamine (45 .mu.L, 0.26 mmol) and DMF (1.7 mL). The
resulting mixture was stirred at room temperature for 2 hours.
After removal of insoluble impurities, the crude product was
purified by RP HPLC using a Phenomenex Synergi 5.mu. Hydro RP 80A
column (50.times.21.2 mm) with eluents of 0.1% TFA H.sub.2O--0.1%
TFA CH.sub.3CN. The desired fractions were pooled and partitioned
between acetonitrile and saturated aqueous sodium bicarbonate. The
organic layer was concentrated to afford the product as a solid (12
mg, 34%).
[1427] MS (m/z) 1573.1 [M+Na].sup.+, 1548.8 [M-H].sup.-; .sup.31P
(121.4 MHz, CDCl.sub.3) .delta. 15.3 and 17.4.
Example 257
cyclo-[[(2S,3R,4R,6E)-7-(4-(1-(S)-Hydroxycarbonylethoxy)-hydroxyphosphoryl-
methoxy)phenyl)-4-methyl-3-hydroxy-2-(methylamino)-6-heptenoyl]-L-2-aminob-
utyryl-sarcosyl-N-methyl-L-leucyl-L-valyl-N-methyl-L-leucyl-L-alanyl-D-ala-
nyl-N-methyl-L-leucyl-N-methyl-L-leucyl-N-methyl-L-valyl]
##STR00473##
[1429] To a solution of
cyclo-[[(2S,3R,4R,6E)-7-(4-(1-(S)-ethoxycarbonylethoxy)phenoxyphosphorylm-
ethoxy)phenyl)-4-methyl-3-hydroxy-2-(methyl-amino)-6-heptenoyl]-L-2-aminob-
utyryl-sarcosyl-N-methyl-L-leucyl-L-valyl-N-methyl-L-leucyl-L-alanyl-D-ala-
nyl-N-methyl-L-leucyl-N-methyl-L-leucyl-N-methyl-L-valyl] (5 mg,
3.2 .mu.mol) in a mixed solvent of water and acetonitrile (0.5 mL
and 4.5 mL) was added 1 N NaOH (40 .mu.L). The solution was stirred
at room temperature for 2 hours. The resulting reaction mixture was
concentrated and purified by RP HPLC using a Phenomenex Synergi
5.mu. Hydro RP 80A column (50.times.21.2 mm) with eluents of 0.1%
TFA H.sub.2O--0.1% TFA CH.sub.3CN. The desired fraction was
concentrated to dryness affording the product as a solid (1.5 mg,
32%).
[1430] MS (m/z) 1446.9 [M+H].sup.+, 1444.9 [M-H].sup.-; HPLC
retention time 0.2 min. (relative to 4.0 min. of cyclosporin A;
Phenominex Synergi 4 micron hydro-RP 80A 50.times.4.6 mm; solvents,
35% water and 65% acetonitrile; flow rate 2 mL/min.; column
temperature 60.degree. C.).
Example 258
[1431] The synthesis of compounds of the invention that are analogs
of BCX-1777 is shown herein.
##STR00474##
[1432] Compounds of the invention, such as, for example, 258.1 can
be made according to the general route outlined herein.
##STR00475##
Example 259
##STR00476##
[1434] The Boc-protected
(1S)-1-(9-deazaguanin-9-yl)-1,4-dideoxy-1,4-imino-D-ribitol,
compound, 259.1, is prepared by stirring the
(1S)-1-(9-deazaguanin-9-yl)-1,4-dideoxy-1,4-imino-D-ribitol (WO
9,919,338 and Evans, G. B. et al., Tetrahedron, 2000, 56, 3053,
also reported in Evans, G. B. et al., J. Med. Chem. 2003, 46, 3412)
with BOC anhydride as described in Greene, T., "Protective Groups
in Organic Synthesis," Wiley-Interscience, 1999. Compound, 259.1,
is then treated in a solvent such as tetrahydrofuran or
dimethylformamide with a base such as sodium hydride. When bubbling
ceases, diethyl phosphonomethyl-triflate (prepared according to
Tetrahedron Lett., 1986, 27, 1477) is added, yielding the desired
phosphonate, 259.2, after deprotection of the BOC group using
trifluoroacetic acid (TFA).
Example 260
##STR00477##
[1436] Compounds such as 260.1 and 260.2 can be made according to
the general route outlined herein.
Example 261
##STR00478##
[1438] The Boc-protected
(1S)-1-(9-deazaguanin-9-yl)-1,4-dideoxy-1,4-imino-D-ribitol,
compound, 259.1, is prepared by stirring the
(1S)-1-(9-deazaguanin-9-yl)-1,4-dideoxy-1,4-imino-D-ribitol (WO
9,919,338 and Evans, G. B. et al., Tetrahedron, 2000, 56, 3053,
also reported in Evans, G. B. et al., J. Med. Chem. 2003, 46, 3412)
with BOC anhydride as described in Greene, T., "Protective Groups
in Organic Synthesis," Wiley-Interscience, 1999. Subsequent
protection of the primary alcohol using a TBS group can be achieved
using TBSCl and imidazole in solvents such as CH.sub.2Cl.sub.2 as
described in Greene, T., "Protective Groups in Organic Synthesis,"
Wiley-Interscience, 1999 to provide compound, 261.1. Compound,
261.1, is then treated in a solvent such as tetrahydrofuran or
dimethylformamide with a base such as sodium hydride. When bubbling
ceases, diethyl phosphonomethyltriflate (prepared according to
Tetrahedron Lett., 1986, 27, 1477) is added, yielding a mixture of
the desired phosphonate diester, 261.2, and 261.3, after
deprotection of the BOC group using trifluoroacetic acid (TFA).
Compounds, 261.2, and 261.3, can be also prepared via a more
complicated 2' OH protected analog of compound 261.1 followed by
alkylation using the diethyl phosphonomethyltriflate to provide
compound 261.2, exclusively. Compound 261.3 can also be prepared by
installation of a different protecting group at the 3' OH position,
followed by deprotection of 2' OH and alkylation with diethyl
phosphonomethyltriflate at the 2' center followed by global
deprotection.
Example 262
##STR00479##
[1440] Representative compounds of the invention can be prepared as
illustrated above. Derivatization at the C-11 hydroxy group is
accomplished through alkylation of methylprednisolone aceponate
262.1 with the appropriate phosphonate, furnishing analogs of
formula 262.2. A specific compound of the invention can be prepared
as follows.
##STR00480##
[1441] After sodium hydride extraction of the hydroxy proton in
262.1, diethyl phosphonate triflate is added to afford ether
262.3.
Example 263
##STR00481##
[1443] Representative compounds of the invention can be prepared as
illustrated above by exploiting the reactivity differences among
the three hydroxy groups available when methylprednisolone
aceponate, 262.1, is fully hydrolized. Following protection of the
only exposed hydroxy group in 262.1, intermediate, 263.1 is
saponified to give diol, 263.2. Alkylation at the primary hydroxy
group with the appropriate phosphonate and subsequent acylation
provides the propionate ester, 263.4. The desired product, 263.5,
is achieved after deprotection.
Example 264
##STR00482##
[1445] Methylprednisolone aceponate, 262.1, is protected as its
silyl ether using the standard TBSCl and imidazole conditions. (J.
Am. Chem. Soc., 1972, 94, 6190). Saponification of both ester
moieties using aqueous sodium hydroxide provides the diol, 264.2.
The less sterically hindered primary hydroxy group is alkylated by
the addition of sodium hydroxide and the phosphonate triflate.
After treating intermediate, 264.3, with propionic anhydride in
pyridine, the previously hydrolized C-17 propionic ester is
replaced. (J. Med. Chem., 1980, 23, 430-437). TBAF deprotection of
the silyl ether furnishes diethyl phosphonate 264.5.
Example 265
##STR00483##
[1447] Representative compounds of the invention can be prepared as
illustrated above. The two hydroxy groups of diol, 263.2, are
regioselectively differentiated by protection at the primary site,
thus allowing alkylation at the tertiary hydroxy group. The
resulting phosphonate intermediate, 265.2, is then deprotected to
afford the diol 265.3. Again the more accessible primary hydroxy
group is acylated to produce the desired analog 265.4.
Example 266
##STR00484##
[1449] Diol, 264.2 (see example 264), is protected at the primary
site as its silyl ether, 266.1. Following alkylation with the
diethyl phosphonate triflate, the resulting intermediate, 266.2, is
treated with TBAF to give diol, 266.3. Acetic anhydride and
pyridine are used to generate the final product 266.4. (J. Mol.
Biol., 1972, 72, 219).
Example 267
##STR00485##
[1451] Representative compounds of the invention can be prepared as
illustrated above. The phosphorus containing merimepodib analog
267.2 is synthesized from parent compounds by alkylation.
Merimepodib 267.1 is obtained by the procedure as described in U.S.
Pat. No. 6,054,472 and U.S. Pat. No. 6,344,465. The methoxy group
of merimepodib 267.1 is demethylated to phenolic OH using a
suitable reagent, such as boron tribromide. The phosphonate moiety
is introduced to the phenolic OH in a suitable aprotic solvent such
as, DMF and is then treated with the phosphonate reagent bearing a
leaving group, for example, bromine, mesyl, tosyl, or
trifluoromethanesulfonyl, in the presence of a suitable organic or
inorganic base. A specific compound of the invention can be
prepared as follows.
##STR00486##
[1452] A solution of 267.1 in dichloromethane is treated with boron
tribromide to obtain the demethylated compound 267.8. Compound
267.8 is then treated with cesium carbonate and one equivalent of
(trifluoromethanesulfonyloxy)-methylphosphonic acid diethyl ester
267.9 to give merimepodib-phosphonate 267.10. Using the above
procedure but employing different phosphonate reagents, the
corresponding products 267.2 bearing different linking group can be
obtained.
Example 268
##STR00487##
[1454] Representative compounds of the invention can be prepared as
illustrated above. The imidazole containing intermediate 268.13 is
synthesized from an aldehyde 268.12 by the procedure of Shih in
Tetrahedron Lett. 1993, 34, 595. Compound 268.12 is prepared by a
two-step procedure described in U.S. Pat. No. 5,807,876, U.S. Pat.
No. 6,054,472, and U.S. Pat. No. 6,344,465. The imidazole is
protected using suitable reagent, for example,
2-(trimethylsilyl)-ethyoxymethyl (SEM) chloride, and the compound
268.14 is converted to 268.15 by the similar procedure described
for the synthesis of 197.1 in U.S. Pat. No. 6,054,472 and U.S. Pat.
No. 6,344,465. After the protecting group on the imidazole of
268.15 is removed, the phosphonate containing moiety is introduced
to the imidazole to provide compounds of the invention. A specific
compound of the invention can be prepared as follows.
##STR00488##
[1455] Compound 268.15 is treated with tetrabutylammonium fluoride
in THF in reflux condition and the resulting 268.16 is alkylated
with 268.9 using sodium hydride as a base to obtain two isomers
268.17 and 268.18, which are separated by chromatography.
Example 269
##STR00489##
[1457] Representative compounds of the invention can be prepared as
illustrated above. Tetrasubstituted benzene derivatives are
obtained by literature procedures (Ichikawa and Ichibagase Yakugaku
Zasshi 1963, 83, 103; Norio, A. et al. Tetrahedron Lett. 1992,
33(37), 5403). After the phenolic OH is protected with a suitable
protecting group, for example benzyl group, the compound 269.21 is
synthesized by the same procedure described in U.S. Pat. No.
6,054,472, and U.S. Pat. No. 6,344,465. After the protecting group
is removed, the phosphonate containing moiety is introduced to the
phenolic OH using the phosphonate reagent 269.7, bearing a suitable
leaving group. A specific compound of the invention can be prepared
as follows.
##STR00490##
[1458] For example, a solution of 269.22, which is obtained by the
procedure of Norio et al. (Tetrahedron Lett. 1992, 33(37), 5403),
is treated with sodium hydride and one equivalent of benzyl bromide
in DMF to get 269.23. Compound 269.23 is converted to 269.24 by a
series of steps such as those reported in U.S. Pat. No. 6,054,472,
and U.S. Pat. No. 6,344,465. After the benzyl protecting group of
269.24 is removed by catalytic hydrogenation, a phosphonate bearing
moiety is attached by alkylation of the resulting phenol in DMF
using sodium hydride and one equivalent of
(trifluoromethanesulfonyl-oxy)methylphosphonic acid diethyl ester
269.9 to give 269.25.
Example 270
##STR00491##
[1460] Representative compounds of the invention can be prepared as
illustrated above. Compound 270.26 is treated with
carbonyldiimidazole or triphosgene followed by the compound 270.27,
which has a handle to attach phosphonate moiety. Compound 270.27
bearing an extra substituent is synthesized from the tri
substituted phenol with a cyano and a nitro groups, which is either
commercially available or by literature procedures (Zolfigol, M. A.
et. al. Indian J. Chem. Sect. B 2001, 40, 1191; De Jongh, R. O. et
al. Recl. Trav. Chim. Pays-Bas 1968, 87, 1327). The resulting
270.28 is converted to 270.29 using procedures similar to those
described in U.S. Pat. No. 6,054,472, and U.S. Pat. No. 6,344,465.
The phosphonate moiety of 270.6 is attached after deprotection of
the benzyl group of 270.29.
##STR00492##
[1461] For example, the bromine substituent of compound 270.30 is
substituted with cyano group by the procedure of De Jongh, R. O. et
al. (Recl. Trav. Chim. Pays-Bas 1968, 87, 1327) and the methoxy
group is converted to benzyloxy group as a protecting group, which
affords compound 270.31. After selective reduction of cyano to
aminomethyl group by borane, the amino group is protected with Boc
group and then the reduction of the nitro group using tin (II)
chloride generates compound 270.32. This substituted aniline 270.32
is then treated with a reaction mixture of the compound 270.26 and
carbonyldiimidazole, as described in U.S. Pat. No. 6,054,472, and
U.S. Pat. No. 6,344,465, to form the urea 270.33. Compound 270.33
is converted to 270.34. Deprotection of the benzyl group using
catalytic hydrogenation followed by attachment of a phosphonate
moiety using 270.9 in the presence of cesium carbonate produces
compound 270.35.
Example 271
[1462] The syntheses of phosphonate compounds of the invention and
of intermediate compounds necessary for their synthesis are
illustrated herein. Derivatization at the C-21 hydroxy group is
accomplished through alkylation of dexamethasone 271A with the
appropriate phosphonate, furnishing analogs shown herein.
##STR00493##
[1463] Derivatization at the C-21 hydroxy group is accomplished
through alkylation of dexamethasone 271A with the appropriate
phosphonate, furnishing analogs of the type 271.2.
##STR00494##
[1464] After sodium hydride extraction of the primary hydroxy
proton in 271A, diethyl phosphonate triflate is added to afford
ether 271.5.
Example 272
##STR00495##
[1466] Synthesis of C-21 phosphonate analogs having formula, 271.4,
is shown herein. Protection this time of dexamehtasone 271A at the
less hindered site furnishes alcohol, 271.5, which is alkylated at
the only exposed hydroxy group with the appropriate phosphonate.
Removal of the protecting groups completes the construction of
analog, 271.4.
Example 272
##STR00496##
[1468] Dexamethasone, 271A, is protected as its silyl ether using
the standard TBSCl and imidazole conditions. (J. Am. Chem. Soc.,
1972, 94, 6190; however, harsher conditions should allow for
bis-protection. After alkylating with the diethyl phosphonate
triflate, the resulting intermediate, 271.9, is treated with TBAF
to give the desired phosphonate, 271.10.
Example 273
[1469] A number of compounds of the general structure 273A can
either be prepared using procedures described in the literature, or
be purchased from commercial sources. The following are good
sources for information on the art of preparing a variety of
compounds, of the general structure 273A, Townsend, Chemistry of
Nucleosides and Nucleotides, Plenum Press, 1994; and Vorbruggen and
Ruh-Pohlenz, Handbook of Nucleoside Synthesis, John Wiley &
Sons, Inc., 2001.
[1470] In the examples the compounds of the invention, described
herein, the substituents have the following general formula
273A:
##STR00497##
[1471] wherein one or more of the Z substituents have been
substituted with an A.sup.0 group; and wherein:
[1472] Z.sub.1 and Z.sub.2 are independently selected from
hydrogen, or a C.sub.1-C.sub.18 acyl, and Z.sub.3 is H, a
C.sub.1-C.sub.18 acyl, or
##STR00498##
[1473] or Z.sub.1 is hydrogen, and together Z.sub.2 and Z.sub.3
are
##STR00499##
[1474] base is
##STR00500##
[1475] wherein X and Y are independently O or S; Z.sup.4 is
hydrogen, amino, hydroxy, or a halogen selected from Cl and Br.
##STR00501##
[1476] More specifically, the preparation of generic structure,
273A are described in Nagahara, et al J. Med. Chem.; 33; 1990;
407-415. The structure 273.2 is described in Kini, et al J. Med.
Chem.; 34; 1991; 3006-3010. The two patents cited above also
provided examples of the synthesis of compound, 273A.
[1477] The core components of this reaction sequence are the
transformation of compound from 273.3 to 273.6. Appropriate
oxidant(s) can convert the primary alcohol (5'-hydroxy) shown in
273.3 to a carboxylic acid or its corresponding ester. In the case
of an ester, an additional deprotection step will give the
carboxylic acid, 273.4. A variety of oxidation procedures exist in
the literature and can be utilized here. These include but are not
limited to the following methods: (i) pyridinium dichromate in
Ac.sub.2O, t-BuOH, and dichloromethane producing the t-butyl ester,
followed by a deprotection using reagent such as trifluoroacetic
acid to convert the ester to the corresponding carboxylic acid (see
Classon, et al., Acta Chem. Scand. Ser. B; 1985, 39, 501-504.
Cristalli, et al., J. Med. Chem., 1988, 31, 1179-1183.); (ii)
iodobenzene diacetate and 2,2,6,6-tetramethyl-1-piperidinyloxy,
free radical (TEMPO) in acetonitrile, producing the carboxylic acid
(See Epp, et al; J. Org. Chem. 64; 1999; 293-295. Jung et al; J.
Org. Chem.; 66; 2001; 2624-2635.); (iii) sodium periodate,
ruthenium(III) chloride in chloroform producing the carboxylic acid
(see Kim, et al, J Med. Chem. 37; 1994; 4020-4030. Homma, et al; J.
Med. Chem., 35; 1992; 2881-2890); (iv) chromium trioxide in acetic
acid producing the carboxylic acid (see Olsson et al; J. Med.
Chem.; 29; 1986; 1683-1689. Gallo-Rodriguez et al; J. Med. Chem.;
37; 1994; 636-646); (v) potassium permanganate in aqueous potassium
hydroxide producing the carboxylic acid (see Ha, et al; J. Med.
Chem.; 29; 1986; 1683-1689. Franchetti, et al; J. Med. Chem.; 41;
1998; 1708-1715.) (vi) nucleoside oxidase from S. maltophilia to
give the carboxylic acid (see Mahmoudian, et al; Tetrahedron; 54;
1998; 8171-8182.)
[1478] The preparation of compound 273.5 starting with compound
273.4 using lead(IV) tetraacetate (Lv=OAc) was described by Teng et
al; J. Org. Chem., 59; 1994; 278-280 and Schultz, et al; J. Org.
Chem.; 48; 1983; 3408-3412. When lead(IV) tetraacetate is used
together with lithium chloride (see Kochi, et al; J. Am. Chem.
Soc.; 87; 1965; 2052), the corresponding chloride is obtained
(273.5, Lv=Cl). Lead(IV) tetraacetate in combination with
N-chlorosuccinimide can produce the same product (273.5, Lv=Cl)
(see Wang, et al; Tet. Asym.; 1; 1990; 527 and Wilson et al; Tet.
Asym.; 1; 1990; 525). Alternatively, the acetate leaving group (Lv)
can also be converted to other leaving group such as bromide by
treatment of trimethylsilyl bromide to give 273.5 ((see Spencer, et
al; J. Org. Chem.; 64; 1999; 3987-3995).
[1479] The coupling of 273.5 (Lv=OAc) with a variety of
nucleophiles were described by Teng et al; Synlett; 1996; 346-348
and U.S. Pat. No. 6,087,482; Column 54 line 64 to Column 55 line
20. Specifically, the coupling between 273.5 and diethyl
hydroxymethylphosphonate in the presence of trimethylsilyl
trifluoromethanesulfonate (TMS-OTf) was described. It can be
envisioned that other compounds with the general structure of
HO-linker-POR.sup.P1R.sup.P2 can also be used so long as the
functional groups in these compounds are compatible with the
coupling reaction conditions. There are many examples in the
published literature describing the coupling of 273.5 (Lv=halogen)
with a variety of alcohols. The reactions can be facilitated with a
number of reagents, such as silver(I) salts (see Kim et al; J. Org.
Chem.; 56; 1991; 2642-2647, Toikka et al; J. Chem. Soc. Perkins
Trans. 1; 13; 1999; 1877-1884), mercury(II) salts (see Veeneman et
al; Recl. Trav. Chim. Pays-Bas; 106; 1987; 129-131), boron
trifluoride diethyl etherate (see Kunz et al; Hel. Chim Acta; 68;
1985; 283-287), Tin(II) chloride (see O'Leary et al; J. Org. Chem.;
59; 1994; 6629-6636), alkoxide (see Shortnacy-Fowler et al;
Nucleosides Nucleotides; 20; 2001; 1583-1598), and iodine (see
Kartha et al; J. Chem. Soc. Perkins Trans. 1; 2001; 770-772). These
methods can be selectively used in conjunction with different
methods in forming 273.5 with various leaving groups (Lv) to
produce 273.6.
[1480] The transformations from 273.1 to 273.2, from 273.2 to
273.3, and from 273.6 to 273.7 are intended to allow the core
components of the transformations (from 273.3 to 273.6) to occur
while preserving the functional groups already exist in the
compound structures. Thus, the syntheses may require the
introduction and removal of protecting groups from a compound is a
commonly practiced art in organic synthesis. It should be
understood that in the transformation 273.6 to 273.7, R.sup.P1 and
R.sup.P2 do not need to remain unchanged. The final form of
R.sup.P1 and R.sup.P2 can be selected from a variety of possible
structures.
Example 274
##STR00502## ##STR00503##
[1482] Compound 274.1 is prepared using the method described in the
patent application WO 01/90121 (table at page 115). The 5'-hydroxyl
in 274.1 is protected as a tert-butyldimethylsilyl (TBDMS) ether.
The 2'- and 3'-hydroxyl groups can be protected as bezoyl (Bz)
esters to give 274.2. The 5'-hydroxyl can then be deprotected to
give 274.3. Oxidation using iodobenzene diacetate and
2,2,6,6-tetramethyl-1-piperidinyloxy, free radical (TEMPO) convert
the primary alcohol to the corresponding acid 274.4. Further
oxidation of 274.4 using lead tetraacetate can produce 274.5.
Coupling between 274.5 and diethyl hydroxy-methyl-phosphonate
(available from Sigma-Aldrich, Cat. No. 39, 262-6) effected by
TMS-OTf can afford 274.6. Treating 274.6 with TMS-Br converts the
phosphodiester to the corresponding phosphonic acid 274.7.
Deprotection of the 2'- and 3'-hydroxyl gives 274.8 as an example
of the generic structure A, where Base is an
7-thia-8-oxo-guanosine, R.sup.1, R.sup.2, R.sup.P1 and R.sup.P2 are
hydrogen, linker is a methylene group.
[1483] The phosphonic acids in 274.7 and 274.8 are used as examples
for illustration purpose. Other forms of phosphonates can be access
via the phosphonic acid, or other forms, such as the corresponding
diesters as described herein.
Example 275
[1484] Leflunomide (structure below, together with its active
metabolite) (see U.S. Pat. No. 4,284,786) is a derivative of
isoxazole. Representative compounds of the invention can be
prepared as illustrated above using procedures similar to those
described in J. Med. Chem. 1996, 39, 4608. Their structures are
shown below.
##STR00504##
[1485] Synthetic methodology towards compounds such as these is
described by Westwood et al, J. Med. Chem., 1996, 39, 4608-4621,
according to the general routes outlined below.
##STR00505##
Example 275A
[1486] The synthesis of suitable phosphonate-containing anilines
are shown below.
##STR00506##
Example 275B
##STR00507##
[1487] Example 276
##STR00508##
[1489] Representative compounds of the invention can be prepared as
illustrated above using procedures similar to those described in J.
Med. Chem. 1996, 39, 4608. Treatment of compound of the invention
276.1 with base provides compound 276.2 which is also a compound of
the invention.
Example 277
##STR00509##
[1491] Representative compounds of the invention can be prepared as
illustrated above. Treatment of compound of the invention 277.1
with base provides compound 277.2 which is also a compound of the
invention.
Example 278
##STR00510##
[1492] Example 278A Synthesis of K-105-44
[1493] 2-Methyl-5-nitrophenol (2.00 g, 13.05 mmol) was dissolved in
dry DMF (10 mL) under argon atmosphere and cooled to 0.degree. C.
Diethylphosphonomethyl-O-triflate (4.70 gm, 15.66 mmol) and cesium
carbonate (6.38 gm, 19.58 mmol) were added sequentially. The
reaction mixture was stirred at 0.degree. C. for 4 hrs. TLC
(cyclohexane/EtOAc, 1:1) showed completion of reaction. Deionized
water (15 mL) was added and the mixture was extracted with EtOAC
(2.times.50 mL). The organic layer was washed with 1N HCl (20 mL)
followed by water (2.times.20 mL), dried over Na.sub.2SO.sub.4 and
concentrated to a semi-solid. Purification by silica gel column
chromatography (cyclohexane/EtOAc, 1:1) afforded pure compound
K-105-44 as an oil (3.86 g, 97%).
[1494] ESI-MS m/z 304 [M+H].sup.+.
Example 278B
Synthesis of K-105-48
[1495] Compound K-105-44 (2.8 g, 9.24 mmol) was dissolved in 15 mL
of absolute ethanol (15 mL) and 6N HCl (2 mL) under an argon
atmosphere. Following the addition of SnCl.sub.2.2H.sub.2O (5.26 g,
27.72 mmol), the reaction mixture was stirred overnight at room
temperature. TLC (CHCl.sub.3/MeOH, 9:1) showed completion of
reaction. The mixture was concentrated to a semi-solid and
dissolved in ethyl acetate (30 mL). The ethyl acetate layer was
washed with deionized water (10 mL) and satd. NaHCO.sub.3 (10 mL)
and dried over Na.sub.2SO.sub.4. Concentration gave a solid that
was used without purification.
[1496] ESI-MS m/z 274 [M+H].sup.+.
Example 278C
Synthesis of K-105-49-3
[1497] Crude compound K-105-48 (900 mg, 3.38 mmol) was dissolved in
15 mL of dry THF (15 mL) under an argon atmosphere. Following the
addition of 5-methylisoxazole-4-carboxylic acid (381 mg, 3.00 mmol)
and diisopropyl carbodiimide (511 .mu.L, 3.30 mmol), the reaction
mixture was stirred 6 h at room temperature. TLC (CHCl.sub.3/MeOH,
9:1) showed completion of reaction. The reaction mixture was
filtered and the filtrate concentrated to give a solid, which was
dissolved in ethyl acetate (25 mL). The solution was washed with
deionized water (2.times.10 mL) and dried over Na.sub.2SO.sub.4.
Concentration gave a solid that was purified by silica gel column
chromatography (CHCl.sub.3/MeOH, 95:5) to afford pure compound
K-105-49-3 as light yellow solid (680 mg, 55%).
[1498] ESI-MS m/z 383 [M+H].sup.+.
[1499] .sup.1H NMR (300 MHz, CDCl.sub.3): .delta. 7.11 (1H, s,
ArH), 7.06 (2H, s, ArH), 4.29-4.20 (4H, m, OCH.sub.2), 4.14 (2H, d,
J=10.4 Hz, OCH.sub.2), 2.76 (3H, s, CH.sub.3), 2.14 (3H, s,
CH.sub.3), 1.37 (6H, t, J=7.0 Hz, CH.sub.3).
[1500] .sup.31P NMR (121.7 MHz, DMSO-d.sub.6/external
H.sub.3PO.sub.4) .delta. ppm 19.7-20.0 (m)
[1501] HPLC: 98% pure (Sphereclone 5 .mu.L, H.sub.2O: MeCN, 20 min
linear from 10-90% MeCN, 1.0 mL/min)
Example 278D
Synthesis of K-105-54-1
[1502] Compound K-105-54-1 (250 mg, 0.65 mmol) was dissolved in 10
mL of absolute ethanol (15 mL) under an argon atmosphere. Following
the addition of NaOH (29 mg, 0.72 mmol), the reaction mixture was
stirred overnight at room temperature. TLC (CHCl.sub.3/MeOH, 9:1)
showed completion of reaction. The reaction mixture was
concentrated to a solid and dissolved in ethyl acetate (20 mL). The
solution was washed with deionized water (2.times.10 mL) and dried
over Na.sub.2SO.sub.4. Concentration gave a solid that was purified
by silica gel column chromatography (CHCl.sub.3/MeOH, 4:1),
affording pure compound K-105-54-1 as a solid (188 mg, 75%).
[1503] ESI-MS m/z 383 [M+H].sup.+.
[1504] .sup.1H NMR (300 MHz, DMSO-d.sub.6): .delta. 7.32 (1H, s,
ArH), 6.96 (2H, s, ArH), 4.31 (2H, d, J=9.9 Hz, OCH.sub.2),
4.18-4.08 (4H, m, 2.times.OCH.sub.2), 2.08 (3H, s, CH.sub.3), 2.00
(3H, s, CH.sub.3), 1.26 (6H, t, J=7.0 Hz, CH.sub.3). .sup.31P NMR
(121.7 MHz, DMSO-d.sub.6/external H.sub.3PO.sub.4) .delta. ppm
20.0-20.4 (m)
[1505] HPLC: 93% pure (Sphereclone 5 .mu.L, H.sub.2O: MeCN, 20 min
linear from 10-90% MeCN, 1.0 mL/min)
Example 279
##STR00511##
[1507] Representative compounds of the invention can be prepared as
illustrated above. Specific compounds of the invention can be
prepared as illustrated below.
##STR00512## ##STR00513##
Example 280
##STR00514## ##STR00515##
[1509] Representative macrolide compounds of the invention, wherein
the structure 280.1 is understood to be the compound tacrolimus,
ascomycin or sirolimus, can be prepared as illustrated above, for
example, using an aryl bismuth reagent such as that shown is
described in Bioorg. Med. Chem. Lett, 1995, 5, 1035. Additionally,
silver salts have been used to mediate alkylations on
immunosuppresive macrolides such as these: see J. Med. Chem., 1998,
41, 1764. Specific compounds of the invention can be prepared as
illustrated below.
Example 281
##STR00516##
[1511] Representative macrolide compounds of the invention, wherein
the structure 212.1 is understood to be the compound tacrolimus,
ascomycin or sirolimus, can be prepared as illustrated above, for
example, using an aryl bismuth reagent such as that shown is
described in Bioorg. Med. Chem. Lett, 1995, 5, 1035. Additionally,
silver salts have been used to mediate alkylations on
immunosuppresive macrolides such as these: see J. Med. Chem., 1998,
41, 1764. Specific compounds of the invention can be prepared as
illustrated below.
##STR00517##
Example 282
##STR00518##
[1513] Representative compounds of the invention can be prepared as
illustrated above. Derivatization at the C-21 hydroxy group is
accomplished through alkylation of prednisone 282.1 with the
appropriate phosphonate to provide compounds of the invention
282.2. A specific compound of the invention can be prepared as
follows.
##STR00519##
[1514] After sodium hydride extraction of the primary hydroxy
proton in 282.1, diethyl phosphonate triflate is added to afford
ether 282.4.
Example 283
##STR00520##
[1516] Representative compounds of the invention 283.3 can be
prepared as illustrated above. Protection of prednisone 283.1 at
the less hindered primary site furnishes alcohol 283.5, which is
alkylated at the exposed hydroxy group with the appropriate
phosphonate to provide 283.6. Removal of the protecting group
completes the construction of analog 283.3. A specific compound can
be prepared as follows.
##STR00521##
[1517] Prednisone 283.1 is mono-protected as its TBS ether 283.7.
After alkylating with the diethyl phosphonate triflate, the
resulting intermediate 283.8 is treated with TBAF to give the
desired phosphonate 283.9.
[1518] The syntheses of phosphonate compounds of the invention and
of intermediate compounds necessary for their synthesis are
illustrated herein. Derivatization at the C-21 hydroxy group is
accomplished through alkylation of dexamethasone 1 with the
appropriate phosphonate, furnishing analogs shown herein.
Example 284
[1519] Representative compounds of the invention can be prepared as
illustrated above. Derivatization at the C-11 hydroxy group is
accomplished through alkylation of rimexolone 284.1 with the
appropriate phosphonate, furnishing analogs of formula 284.2. A
specific compound of the invention can be prepared as illustrated
below.
##STR00522##
[1520] After sodium hydride extraction of the hydroxy proton in
284.1, diethyl phosphonate triflate is added to afford ether
284.5.
##STR00523##
Example 285
##STR00524##
[1522] The diacid (100 mg, 0.304 mmol), amino acid (100 mg, 0.651
mmol), phenol (145 mg, 1.54 mmol), and triethylamine (510 .mu.L,
3.66 mmol) were dissolved in pyridine (5 mL). The mixture was
heated to 60.degree. C. for 5 minutes. To this reaction mixture was
added a solution of triphenylphosphine (560 mg, 2.14 mmol) and
Aldrithiol(2) (470 mg, 2.13 mmol) dissolved in pyridine (5 mL). The
reaction was then heated at 60.degree. C. for 12 hours. The
reaction mixture was diluted in EtOAc, washed with H.sub.2O, sat'd
NaHCO.sub.3(aq), and brine. The organic layer was dried
(MgSO.sub.4), concentrated and purified by chromatography on silica
gel (1% MeOH/CH.sub.2Cl.sub.2.fwdarw.10% MeOH/CH.sub.2Cl.sub.2) to
give monoamidate 130-1 (5 mg, 3%) and bisamidate 130-2 (5 mg,
3%).
[1523] For 130-1: .sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 7.78
(1H, m), 7.35 (2H, m), 7.20 (3H, m), 4.18-3.95 (5H, m), 2.24-1.90
(2H, m), 1.87-1.62 (4H, m), 1.38-1.18 (6H, m), 1.02 (6H, m);
.sup.31P NMR (121 MHz, CD.sub.3OD) .delta. 36.3, 35.3; LC-MS
(method: 0.5 min 95% H.sub.2O/5% MeCN 5 min 0% H.sub.2O/100% MeCN,
rt=2.18 min. MS calc'd for C.sub.23H.sub.34N.sub.6O.sub.5P
(MH.sup.+): 505.2. Found 505.2.
[1524] For 130-2: .sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 7.77
(1H, s), 4.23-3.92 (8H, m), 2.04-1.50 (6H, m), 1.42 (3H, d), 1.40
(3H, d), 1.28 (3H, t), 1.22 (3H, t), 1.02 (3H, s), 1.01 (3H, s);
.sup.31P NMR (121 MHz, CD.sub.3OD) .delta. 33.9; LC-MS (method: 0.5
min 95% H.sub.2O/5% MeCN 5 min 0% H.sub.2O/100% MeCN, rt=1.79 min.
MS calc'd for C.sub.22H.sub.39N.sub.7O.sub.6P (MH.sup.+): 528.3.
Found 528.3.
Example 286
##STR00525##
[1526] The diacid (25 mg, 0.072 mmol), amino acid (25 mg, 0.16
mmol), phenol (38 mg, 0.40 mmol), and triethylamine (127 .mu.L,
0.911 mmol) were dissolved in pyridine (1.25 mL). The mixture was
heated to 60.degree. C. for 5 minutes. To this reaction mixture was
added a solution of triphenylphosphine (140 mg, 0.534 mmol) and
Aldrithiol(2) (119 mg, 0.540 mmol) dissolved in pyridine (1.25 mL).
The reaction was then heated at 60.degree. C. for 12 hours. Another
batch of diacid (12 mg, 0.035 mmol) was treated as described above.
The reaction mixtures from both batches were combined and diluted
in EtOAc, washed with H.sub.2O, sat'd NaHCO.sub.3(aq) and brine.
The organic layer was dried (MgSO.sub.4), concentrated and purified
by chromatography on silica gel (1% MeOH/CH.sub.2Cl.sub.2 10%
MeOH/CH.sub.2Cl.sub.2). to give monoamidate 133-1 (3 mg, 8%) and
bisamidate 133-2 (8 mg, 20%).
[1527] For 133-1: .sup.1H NMR (300 MHz, CD.sub.3OD) .delta.
8.38-8.08 (1H, m), 7.78-7.60 (2H, m), 7.50-7.18 (8H, m), 6.67-6.05
(1H, m), 5.60-5.30 (2H, m), 4.63 (1H, bs), 4.25-3.95 (3H, m), 1.37
(3H, m), 1.18 (3H, m); .sup.31P NMR (121 MHz, CD.sub.3OD) .delta.
21.5, 20.2; LC-MS (method: 0.5 min 95% H.sub.2O/5% MeCN.fwdarw.5
min 0% H.sub.2O/100% MeCN, rt=1.98 min. MS calc'd for
C.sub.25H.sub.28N.sub.6O.sub.5P (MH.sup.+): 523.2. Found 523.2.
[1528] For 133-2: .sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 8.15
(1H, dd), 7.72 (1H, s), 7.67 (1H, m), 7.39 (2H, m), 7.28 (1H, m),
6.44 (1H, dd), 5.40 (2H, s), 4.23-3.90 (6H, m), 1.42 (6H, m), 1.27
(3H, t), 1.18 (3H, t); .sup.31P NMR (121 MHz, CD.sub.3OD) .delta.
19.7; LC-MS (method: 0.5 min 95% H.sub.2O/5% MeCN 5 min 0%
H.sub.2O/100% MeCN, rt=1.86 min. MS calc'd for
C.sub.24H.sub.33N.sub.7O.sub.6P (MH.sup.+): 546.2. Found 546.2.
Example 287
Pro-Drug Cleavage Assays
Isolation of PBMC Extracts:
[1529] Fresh human PBMCs were obtained from patients undergoing
leukophoresis; cells were shipped in plasma and processed within 26
h of draw. Purification was achieved using the Ficoll-Paque method:
PBMC cells were harvested by centrifugation at 1200.times.g for 5
minutes and washed three times by re-suspension in RBC lysis buffer
(155 mM NH.sub.4Cl, 0.1 mM EDTA, 10 mM KHCO.sub.3). Washed cells
were suspended in lysis buffer (0.2.times.10.sup.9 cells in 1 ml of
10 mM Tris, pH 7.4, 150 mM NaCl, 20 mM CaCl.sub.2, 1 mM DTT and 1%
NP40) and incubated on ice for 20 minutes. The PBMC crude extract
was centrifuged at 1000.times.g for 30 min to remove unlysed cells
and the supernatant at 100,000 X g for 1 h. The 100,000.times.g
supernatant (PBMC Extract: P0) was harvested, snap frozen in liquid
nitrogen and stored at -70.degree. C.
Protocol for Measurement of Cleavage of Prodrugs by PBMC
Extracts:
[1530] Reaction mixtures contained 25 mM MesNa (pH 6.5), 100 mM
NaCl, 1 mM DTT, 0.1% NP-40, 30 .mu.M substrate, and varying amounts
of enzyme in a final volume of 100 .mu.l. The enzymatic reaction is
performed at 37.degree. C. for 10-120 minutes and stopped at 3-4
individual time points by adding 180 .mu.l of ice cold methanol.
Samples are incubated @ -20.degree. C. for 30 min, and centrifuged
13,000 RPM for 30 min (@ 4.degree. C.). The supernatant is
transferred to a 96 well plate and evaporated under vacuum using a
speedvac. The precipitate is dissolved in 100 .mu.l of 20 mM
CH.sub.3COONH.sub.4+5% AcCN. The disappearance of pro-drug is
measured by HPLC, monitoring at 260 nm. The specific activity of
the PBMC Extract against the prodrugs tested is defined as: v
(cleavage rate)/.mu.g protein=pmoles/min/.mu.g.
TABLE-US-00003 Results Human PBMC extract specific Compound
activity (pmol/min/.mu.g) 130-1 3.48 130-2 0.65 133-1 4.9 133-2
0.38
Example 288
[1531] Representative compounds of the invention having the
following formulae can be prepared as described herein.
##STR00526##
[1532] For example, three regions of mycophenolate mofetil can be
utilized for the attachment of the phosphonate prodrug as
demonstrated by compounds D, E, and G shown above. Also, the
carboxylic acid can be replaced with a phosphonic acid as in
compound F.
Example 288A
##STR00527##
[1534] Representative compounds of the invention can be prepared as
illustrated above. The morpholino ethyl moiety can serve as a
prodrug functionality to improve bioavailability and can be
replaced with the phosphonate prodrug handle as shown above.
Mycophenolic acid is commercially available, e.g., from Sigma
Chemical Company, St. Louis, Mo. Activation of the carboxylic acid
288.1 in the presence of the free phenol, followed by addition of
an alcohol carrying the phosphonate group, results in the formation
of the desired product 288.3 (U.S. Pat. No. 4,786,637). A specific
compound of the invention can be prepared as follows.
##STR00528##
[1535] Mycophenolic acid 288.1 is dissolved in dichloromethane.
Thionyl chloride is added followed by a catalytic amount of DMF.
The reaction mixture is stirred at room temperature for 3 hours,
after which the volatile components are removed under vacuum. The
phosphonate-alcohol is dissolved in dichloromethane and chilled to
about 4.degree. C. on an ice bath. The mycophenolic acid chloride
288.2 is dissolved in dichloromethane and added to the chilled
solution. After stirring for 90 minutes at about 4.degree. C., the
reaction mixture is washed with water and then with aqueous sodium
bicarbonate. The organic solution is dried and evaporated to yield
the phosphonate 288.4.
Example 289
##STR00529##
[1537] Representative compounds of the invention can be prepared as
illustrated above. The C-4 phenol position provides a reactive
handle for further analogs as illustrated above. Once the
carboxylic acid of 289.1 is blocked by morpholino ethyl, such as in
compound 289.2 the phenol can be alkylated under basic conditions.
Bases such as pyridine, potassium carbonate, or triethylamine are
utilized. Leaving groups such as trifluoromethylsulfonate,
mesylate, bromide, or iodide are attached to the phosphonate
prodrug subunit and reacted, in the presence of base, with compound
289.2. Compound 289.3 can either be used directly, or in the form
of a salt, compound 289.4. Among the large number of salts that can
be prepared, chloride and bisulfate salts are one particular
embodiment of the invention. A specific compound of the invention
can be prepared as follows.
##STR00530##
[1538] Compound 289.5 is prepared similar to compound 289.2
(described in Example 288). A solution of morpholino ethanol in
dichloromethane is cooled to about 4.degree. C. The mycophenolic
acid chloride 289.5 is dissolved in dichloromethane and added to
the cooled solution. Stirring this solution for about 90 minutes
gives compound 289.2. The reaction mixture is washed with water and
dried with sodium sulfate. Removal of the solvent provides isolated
compound 289.2. Alkylation at the phenolic position of 289.2 is
achieved by suspending the compound in pyridine. Triflate 289.6 is
added to the solution and the mixture is stirred at room
temperature for about 90 minutes. The reaction mixture is poured
into water and the product is extracted with ethyl acetate. Removal
of the organic layer provides compound 289.7. Hydrochloride salt of
289.7 can optionally be prepared. Compound 289.7 is dissolved in
isopropanol and the solution is added to a mixture of hydrogen
chloride in isopropanol. The hydrochloride salt 289.8 is collected
by filtration and dried under vacuum.
Example 290
##STR00531##
[1540] Representative compounds of the invention can be prepared as
illustrated above. The carboxylic acid of mycophenolic acid can be
replaced with a phosphonic acid that may also serves as a prodrug
handle. In order to remove the carboxylic acid containing side
chain, the acid chloride 290.5 (prepared in Example 289) is
converted to ester 290.1. Protection of the phenol with a silyl
group, followed by dihydroxylation and cleavage of the diol
generates aldehyde 290.3 (Pankiewicz, et al., J. Med. Chem., 2002,
45, 703), (Patterson et al., U.S. Pat. No. 5,444,072). A Wittig
reaction with ylide 290.4 carrying an appropriately protected
phosphonate provides the desired compound 290.5. Final deprotection
yields compound 290.6. A specific compound of the invention can be
prepared as follows.
##STR00532##
[1541] Mycophenolate ester 290.8 can simply be prepared by stirring
the acid chloride 290.7 with MeOH. Then, the phenol position of
mycophenolate ester is protected by a silyl group such as TBS to
provide compound 290.9. Once the phenol position is protected,
dihydroxylation using osmium tetraoxide followed by periodinate
cleavage provides aldehyde 290.10. Aldehyde 290.10 and excess of
the ylide 290.11 are heated in benzene at reflux for about 24
hours. The reaction mixture is concentrated and the residue is
purified by column chromatography to provide olefin 290.12
(Pankiewics et al., J. Med. Chem., 2002, 45, 703). A final
deprotection using HF-pyridine yields the final product 290.13.
Example 291
##STR00533##
[1543] Representative compounds of the invention can be prepared as
illustrated above. Another attachment point of the compound can be
unmasked after demethylation of mycophenolate ester 291.2 as
illustrated above. For this purpose, the 4-OH needs to be masked
with a protecting group (P) such as a silyl group. Once the 6-MeO
is demethylated and alkylated, the protecting group at position 4
is removed to reveal the final product 291.4. The morphonyl ethanol
group is installed early and carried through the alkylation steps.
A different protecting group may be installed initially and removed
later. In such the latter type of synthesis, the last step is the
formation of the morpholinoethyl ester prodrug. A specific compound
of the invention can be prepared as described below.
##STR00534##
[1544] Phenol 291.5 is protected with TBS group in CH.sub.2Cl.sub.2
using imidazole as base to yield 291.6. Demethylation is performed
using thiolate nucleophiles to generate compound 291.7. A variety
of other methods are also available in literature as described in
Protective Groups in Organic Synthesis by Greene and Wuts.
Alklation of the 6-OH using a triflate of the phosphonate proceeds
well using K.sub.2CO.sub.3 or TEA to provide 291.8. Final
deprotection to remove the TBS group provides product 291.9.
Example 292
##STR00535##
[1546] Representative compounds of the invention can be prepared as
illustrated above.
[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2-m-
ethyl-but-2-enyloxymethyl]-phosphonic acid diisopropyl ester
[1547] A mixture of
7-hydroxy-6-(4-hydroxy-3-methyl-but-2-enyl)-5-methoxy-4-methyl-3H-isobenz-
ofuran-1-one 1A (50 mg, 0.18 mmol, Pankiewicz et al., J. Med.
Chem., 45, 703), diisopropyl bromomethylphosphonate (93 mg, 0.36
mmol) and lithium t-butoxide (1M in THF, 0.54 mL) in DMF (3 mL) was
heated at 70.degree. C. for 5 hours. The reaction was quenched with
1N HCl. The mixture was poured into 5% aqueous lithium chloride,
extracted with ethyl acetate, and concentrated. The residue was
purified by chromatography on silica gel, affording
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid diisopropyl ester 1B
(25 mg, 32%); .sup.1H NMR (300 MHz, CDCl.sub.3) .delta.1.25 (m,
12H), 1.79 (s, 3H), 2.05 (s, 3H), 3.37 (d, J=6.6 Hz, 2H), 3.58 (d,
2H), 3.77 (s, 3H), 3.97 (m, 2H), 4.68 (m, 2H), 5.19 (s, 2H), 5.45
(t, J=6.6 Hz, 1H), 7.83 (s, 1H) ppm.
[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2-m-
ethyl-but-2-enyloxymethyl]-phosphonic acid and
[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid monoisopropyl ester
[1548] To a solution of
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid diisopropyl ester 1B
(25 mg, 0.055 mmol) and 2,6-lutidine (0.18 mL, 1.65 mmol) in
acetonitrile was added trimethylsilyl bromide (0.126 mL, 1.1 mmol)
at 0.degree. C. The mixture was allowed to warm to room temperature
and stirred for 4 hours. The reaction was quenched with methanol at
0.degree. C., and the resulting mixture was concentrated. The
residue was purified by preparative reverse-phase HPLC to afford,
after removal of the solvent,
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid 1C as an oil (17 mg,
83%); .sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.81 (s, 3H), 2.06
(s, 3H), 3.40 (d, J=6.6 Hz, 2H), 3.50 (d, 2H), 3.77 (s, 3H), 3.97
(s, 2H), 5.20 (s, 2H), 5.47 (t, J=6.6 Hz, 1H) and
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid monoisopropyl ester 1D
as an oil (2 mg, 7%); .sup.1H NMR (300 MHz, CD.sub.3OD) .delta.
1.23 (d, 6H), 1.81 (s, 3H), 2.08 (s, 3H), 3.40 (d, J=6.6 Hz, 2H),
3.50 (d, 2H), 3.77 (s, 3H), 3.90 (s, 2H), 4.50 (m, 1H), 5.20 (s,
2H), 5.47 (t, J=6.6 Hz, 1H) ppm.
Example 293
[1549] Representative compounds of the invention can be prepared as
illustrated below.
##STR00536##
[5-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3--
methyl-penta-1,3-dienyl]-phosphonic acid dimethyl ester
[1550] To a solution of tetramethylmethylene diphosphonate (102 mg,
0.44 mmol) in THF (2.5 mL) was added a THF solution of sodium
bis(trimethyl-silyl)amide (1.0 M, 0.44 mL). After stirring for 30
minutes, a solution of
4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2-m-
ethyl-but-2-enal 2A (30 mg, 0.11 mmol, Pankiewicz et al., J. Med.
Chem., 45, 703) in THF (2.5 mL) was added, and stirring was
continued for an additional 15 minutes. The reaction was quenched
with saturated aqueous ammonium chloride. The mixture was extracted
with ethyl acetate. After evaporation of solvent, the residue was
purified by chromatography on silica gel eluting with ethyl acetate
(50% to 100%)/hexanes, affording
[5-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3--
methyl-penta-1,3-dienyl]-phosphonic acid dimethyl ester 2B (30 mg,
71%) as an oil; .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 1.80 (s,
3H), 2.04 (s, 3H), 3.45 (d, J=6.6 Hz, 2H), 3.76 (s, 3H), 3.88 (d,
6H), 5.20 (s, 3H), 5.55 (m, 1H), 5.95 (m, 1H), 7.05 (m, 1H), 7.65
(s, 1H) ppm.
[5-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3-m-
ethyl-penta-1,3-dienyl]-phosphonic acid
[1551] To a solution of
[5-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3--
methyl-penta-1,3-dienyl]-phosphonic acid dimethyl ester 2B (22 mg,
0.057 mmol) and 2,6-lutidine (0.22 mL, 1.71 mmol) in acetonitrile
was added trimethylsilyl bromide (0.183 mL, 1.71 mmol) at 0.degree.
C. The mixture was allowed to warm to room temperature and stirred
for 1 hour. The reaction was quenched with methanol at 0.degree.
C., and the resulting mixture was concentrated. The residue was
purified by preparative reverse-phase HPLC to afford, after removal
of the solvent,
[5-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3--
methyl-penta-1,3-dienyl]-phosphonic acid 2C as a solid (13 mg,
65%); .sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.91 (s, 3H), 2.10
(s, 3H), 3.55 (d, J=6.6 Hz, 2H), 3.75 (s, 3H), 5.2 (s, 2H), 5.6-5.8
(m, 2H), 6.9 (m, 1H) ppm.
Example 294
[1552] Representative compounds of the invention can be prepared as
illustrated below.
##STR00537##
6-(4-Bromo-3-methyl-but-2-enyl)-7-hydroxy-5-methoxy-4-methyl-3H-isobenzof-
uran-1-one
[1553] Polymer-supported triphenylphosphine (3 mmol/g, 0.5 g) was
soaked in dichloromethane (10 mL) for 1 hour
7-Hydroxy-6-(4-hydroxy-3-methyl-but-2-enyl)-5-methoxy-4-methyl-3H-isobenz-
ofuran-1-one 1A (100 mg, 0.36 mmol) and carbon tetrabromide (143
mg, 0.43 mmol) were sequentially added and the mixture was shaken
for 1 hour at room temperature. More carbon tetrabromide (143 mg,
0.43 mmol) was added and the mixture was shaken further for 1 hour.
The mixture was filtered and the filtrate was concentrated. The
residue was chromatographed on silica gel (0% to 60% ethyl
acetate/hexanes) to afford
6-(4-bromo-3-methyl-but-2-enyl)-7-hydroxy-5-methoxy-4-methyl-3H-isobenzof-
uran-1-one 3B as an oil (52 mg, 42%); .sup.1H NMR (300 MHz,
CDCl.sub.3) .delta. 1.95 (s, 3H), 2.16 (s, 3H), 3.44 (d, J=7.2 Hz,
2H), 3.78 (s, 3H), 3.98 (s, 2H), 5.21 (s, 2H), 5.68 (t, J=7.2 Hz,
1H), 7.71 (brs, 1H) ppm.
[5-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3-m-
ethyl-pent-3-enyl]-phosphonic acid diethyl ester
[1554] n-Butyl lithium (1.6 M in hexanes, 1 mL) was added to an
equal volume of THF at -20.degree. C. A solution of diethyl
methylphosphonate (220 mg, 1.45 mmol) in THF (1 mL) was then added
dropwise and the solution was stirred for 30 minutes. After cooling
at 60.degree. C., the solution was transferred via a cannula to a
vial containing copper (I) iodide (276 mg, 1.45 mmol), and the
resulting mixture was stirred for 1 hour at -30.degree. C. A
solution of
6-(4-bromo-3-methyl-but-2-enyl)-7-hydroxy-5-methoxy-4-methyl-3H-isobenzof-
uran-1-one 3B (50 mg, 0.15 mmol) in THF (1 mL) was added and the
mixture was allowed to warm to 0.degree. C. for 2 hours before
saturated aqueous ammonium chloride was added. The reaction mixture
was acidified with 2 N HCl and extracted with ethyl acetate. The
ethyl acetate extract was concentrated and the residue was
chromatographed on silica gel (40% to 100% ethyl acetate/hexanes),
affording
[5-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3--
methyl-pent-3-enyl]-phosphonic acid diethyl ester 3C as an oil (27
mg, contaminated with the starting diethyl methylphosphonate);
.sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 1.32 (m, 6H), 1.8-1.9 (m,
5H), 2.18 (s, 3H), 2.25 (m, 2H), 3.42 (d, J=7.2 Hz, 2H), 3.78 (s,
3H), 4.15 (m, 4H), 5.21 (s, 2H), 5.24 (t, J=7.2 Hz, 1H), 7.65 (s,
1H) ppm.
[5-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3-m-
ethyl-pent-3-enyl]-phosphonic acid monoethyl ester
[1555] A mixture of
[5-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3--
methyl-pent-3-enyl]-phosphonic acid diethyl ester 3C (27 mg, 0.066
mmol), LiOH (200 mg), MeOH (3 mL) and water (1 mL) was stirred at
70.degree. C. for 4 hours. After cooling, the reaction solution was
acidified with 2 N HCl, mixed with brine, and extracted with ethyl
acetate/acetonitrile. The organic extract was concentrated and the
residue was purified by preparative reverse-phase HPLC
(acetonitrile and 0.1% aqueous CF.sub.3COOH), affording
[5-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3--
methyl-pent-3-enyl]-phosphonic acid monoethyl ester 3D (7 mg, 28%);
.sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.28 (t, J=6.9 Hz, 3H),
1.7-1.9 (m, 5H), 2.20 (s, 3H), 2.2-2.3 (m, 2H), 3.41 (d, J=6.6 Hz,
2H), 3.80 (s, 3H), 4.02 (m, 2H), 5.2-5.3 (m, 3H) ppm.
##STR00538##
[5-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3--
methyl-pent-3-enyl]-phosphonic acid
[1556] To a solution of
{5-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-is-
obenzofuran-5-yl]-3-methyl-pent-3-enyl}-phosphonic acid diethyl
ester (20 mg, 0.039 mmol) in DMF (0.5 mL) and DCM (0.5 mL) was
added TMSBr (50.5 .mu.L, 0.39 mmol) followed by 2,6-lutidine (45.3
.mu.L, 0.39 mmol). The reaction was allowed to proceed for one hour
when it was complete, as judged by LCMS. The reaction mixture was
quenched with MeOH and concentrated to dryness. The residue was
purified by preparative reverse-phase HPLC. The fraction containing
the desired product was concentrated and treated with 10% TFA/DCM
for 5 minutes. After concentration, the residue was purified by
preparative reverse-phase HPLC to provide 7 mg (50%) of
[5-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-3--
methyl-pent-3-enyl]-phosphonic acid as a solid. .sup.1H NMR (300
MHz, CD.sub.3OD) .delta. 1.66-1.78 (m, 5H), 2.10 (s, 3H), 2.16-2.22
(m, 2H), 3.34 (d, J=7.2 Hz, 2H), 3.72 (s, 3H), 5.16 (s, 2H), 5.20
(t, J=7.2 Hz, 1H) ppm; .sup.31P (121.4 MHz, CD.sub.3OD) .delta.
31.57 ppm; MS (m/z) 355 [M-H].sup.-, 357 [M+H].sup.+.
Example 295
[1557] Representative compounds of the invention can be prepared as
illustrated below.
##STR00539##
2-(4-Bromo-but-2-enyl)-6-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro--
isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid methyl ester
[1558] To a cooled (-78.degree. C.) solution of mycophenolic acid
methyl ester 4A (138 mg, 0.41 mmol) in THF (2.5 mL) was added a THF
solution of sodium bis(trimethysilyl)amide (1.0 M, 0.98 mL). After
stirring for 30 minutes, a solution of 1,4-dibromo-2-butene (950
mg, 4.1 mmol) in THF (2.5 mL) was added and stirring was continued
for 10 minutes. The resulting mixture was warmed to -30.degree. C.
and stored at this temperature for 16 hours. The reaction was
quenched with saturated aqueous ammonium chloride. The mixture was
extracted with ethyl acetate to give, after evaporation of the
solvent, a residue that was purified by chromatography on silica
gel eluting with ethyl acetate (0% to 40%)/hexanes, affording
2-(4-bromo-but-2-enyl)-6-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro--
isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid methyl ester 4B (150
mg, 78%) as an oil; .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 1.75
(s, 3H), 2.0-2.4 (m, 8H), 2.62 (m, 1H), 3.37 (d, J=6.6 Hz, 2H),
3.58 (s, 3H), 3.76 (s, 3H), 3.88 (d, J=4.8 Hz, 2H), 5.1-5.3 (m,
3H), 5.67 (brs, 2H), 7.67 (s, 1H) ppm.
2-[4-(Diethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-methyl-3-o-
xo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid methyl
ester
[1559] A solution of
2-(4-bromo-but-2-enyl)-6-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro--
isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid methyl ester 4B (140
mg, 0.30 mmol) and triethylphosphite (600 mg, 3.6 mmol) in toluene
(30 mL) was stirred at reflux for 20 hours. The mixture was
concentrated and chromatographed on silica gel eluting with ethyl
acetate (60% to 100%)/hexanes, affording
2-[4-(diethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-methyl-3--
oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid
methyl ester 4C as an oil (70 mg, 43%); .sup.1H NMR (300 MHz,
CDCl.sub.3) .delta. 1.27 (m, 6H), 1.79 (s, 3H), 2.0-2.7 (m, 8H),
3.37 (d, J=6.6 Hz), 3.52 (s, 3H), 3.75 (s, 3H), 4.08 (m, 4H), 5.20
m, 3H), 5.45 (m, 2H) ppm.
2-[4-(Diethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-methyl-3-o-
xo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid
[1560] A mixture of
2-[4-(diethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-methyl-3--
oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid
methyl ester 4C (33 mg, 0.063 mmol) and lithium hydroxide (44 mg)
in a mixture of THF (6 mL) and water (1 mL) was stirred at room
temperature for 6 hours. The organic solvent was removed and the
residue was partitioned between ethyl acetate and 5% aqueous sodium
bicarbonate. The aqueous layer was acidified with 2 N HCl and
extracted with ethyl acetate. The ethyl acetate extract was
concentrated, affording
2-[4-(diethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-methyl-3--
oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid 4D as
an oil (30 mg, 100%); .sup.1H NMR (300 MHz, CDCl.sub.3) .delta.
1.27 (m, 6H), 1.79 (s, 3H), 2.0-2.7 (m, 8H), 3.37 (d, J=6.6 Hz),
3.75 (s, 3H), 4.08 (m, 4H), 5.19 (s, 2H), 5.25 (m, 1H), 5.44 (m,
1H), 5.55 (m, 1H), 5.45 (m, 2H) ppm.
2-[4-(Ethoxy-hydroxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-meth-
yl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-h ex-4-enoic
acid
[1561] A mixture of
2-[4-(diethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-methyl-3--
oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid
methyl ester 4C (25 mg, 0.048 mmol) and lithium hydroxide (200 mg)
in a mixture of methanol (3 mL) and water (1 mL) was stirred at
70.degree. C. for 2 hours. The organic solvent was evaporated and
the residue acidified with 2N HCl and extracted with ethyl
acetate/acetonitrile. The organic extract was concentrated, and the
residue was purified by preparative reverse-phase HPLC
(acetonitrile and 0.1% aqueous CF.sub.3COOH), affording
2-[4-(ethoxy-hydroxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-met-
hoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic
acid 4E as an oil (15 mg, 89%); .sup.1H NMR (300 MHz, CD.sub.3OD)
.delta. 1.25 (t, J=6.9 Hz, 3H), 1.81 (s, 3H), 2.1-2.6 (m, 8H), 3.40
(d, J=6.6 Hz, 2H), 3.77 (s, 3H), 3.97 (m, 2H), 5.1-5.3 (m, 3H),
5.67 (brs, 2H) ppm.
##STR00540##
2-[4-(Dimethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-methyl-3-
-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid
methyl ester
[1562] Under a N.sub.2 atmosphere, a solution of
2-(4-bromo-but-2-enyl)-6-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro--
isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid methyl ester (490 mg,
1.05 mmol) in trimethylphosphite (2.5 mL, 21.1 mmol) was heated at
120.degree. C. for 1 hour. The reaction was allowed to cool to room
temperature. The reaction mixture was worked up by removal of the
solvent in vacuo followed by chromatography using EtOAc-hexanes to
provide 460 mg (88%) of the product as an oil. .sup.1H NMR (300
MHz, CDCl.sub.3) .delta. 1.77 (s, 3H), 2.081-2.31 (m, 4H), 2.15 (s,
3H), 2.52 (d, 1H, J=22 Hz), 2.54 (d, 1H, J=22 Hz), 2.55-2.63 (m,
1H), 3.36 (d, 2H, J=7 Hz), 3.57 (s, 3H), 3.72 (d, 6H, J=11 Hz),
3.76 (s, 3H), 5.20 (s, 2H), 5.20-5.26 (m, 1H), 5.36-5.56 (m, 2H),
7.69 (s, 1H) ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta. 30.1
ppm; MS (m/z) 497.2 [M+H].sup.+, 519.2 [M+Na].sup.+.
##STR00541##
2-[4-(Dimethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-methyl-3-
-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid
[1563]
2-[4-(Dimethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-me-
thyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic
acid methyl ester (460 mg, 0.927 mmol) in a solution of 1:1:2 of
H.sub.2O, MeOH, THF (8 mL) was stirred with LiOH.H.sub.2O (78 mg,
1.86 mmol) at ambient temperature for 12 hours. A second batch of
LiOH.H.sub.2O (40 mg, 0.952 mmol) was added. The reaction mixture
was stirred at room temperature for another 16 hours, after which
no further progress was observed. The reaction was quenched by
addition of a saturated aqueous solution of NH.sub.4Cl. The organic
layer was removed in vacuo and the product was extracted with EtOAc
from the aqueous layer, which had been acidified by addition of 5
drops of 2 N HCl. The product was further purified by
chromatography to provide the desired product. .sup.1H NMR (300
MHz, CDCl.sub.3) .delta. 1.79 (s, 3H), 2.08-2.38 (m, 4H), 2.15 (s,
3H), 2.53 (d, 1H, J=22 Hz), 2.60 (d, 1H, J=22 Hz), 2.57-2.64 (m,
1H), 3.38 (d, 2H, J=7 Hz), 3.72 (d, 6H, J=11 Hz) 3.76 (s, 3H), 5.20
(s, 2H), 5.27 (t, 1H, J=6 Hz), 5.36-5.63 (m, 2H) ppm; .sup.31P
(121.4 MHz, CDCl.sub.3) .delta. 30.5 ppm; MS (m/z) 481.2
[M-H].sup.-.
##STR00542##
2-[4-(2-[4-(Dimethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-me-
thyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic
acid
[1564] To a solution of
2-[4-(dimethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-methyl-3-
-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid (25
mg, 0.052 mmol) in acetonitrile (2 mL) was added 2,6-lutidine (60
.mu.L, 0.52 mmol) and TMSBr (67 .mu.L, 0.52 mmol). The reaction was
allowed to proceed for 45 minutes when it was completed as judged
by LCMS. The reaction mixture was concentrated under reduced
pressure and quenched with an aqueous NaOH solution (1 mL). The
product was purified by RP HPLC (using a C18 column with a gradient
of H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA) to provide 14.2 mg
(60%) of the product as a solid. .sup.1H NMR (300 MHz, CD.sub.3OD)
.delta. 1.81 (s, 3H), 2.081-2.31 (m, 4H), 2.16 (s, 3H), 2.45 (d,
1H, J=22 Hz), 2.47 (d, 1H, J=22 Hz), 2.55-2.63 (m, 1H), 3.38 (d,
2H, J=7 Hz), 3.77 (s, 3H), 5.25 (s, 2H), 5.20-5.36 (m, 1H),
5.36-5.56 (m, 2H) ppm; .sup.31P (121.4 MHz, CD.sub.3OD) .delta.
25.4 ppm; MS (m/z) 453 [M-H].sup.-.
##STR00543##
2-[4-(Dimethoxy-phosphoryl)-but-2-enyl]-6-[6-methoxy-7-methyl-3-oxo-4-(2--
trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-hex-4-en-
oic acid 2-trimethylsilanyl-ethyl ester
[1565] A solution of
2-[4-(dimethoxy-phosphoryl)-but-2-enyl]-6-(4-hydroxy-6-methoxy-7-methyl-3-
-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic acid (160
mg, 0.332 mmol) and trimethylsilylethanol (160 mg, 1.36 mmol) in
THF (8.00 mL) was stirred with triphenylphosphine (345 mg, 1.33
mmol). To this solution was added diethyl azodicarboxylate (230
.mu.L, 1.33 mmol) at 0.degree. C. The mixture was allowed to warm
to room temperature and stirred for 16 hours. Additional
triphenylphosphine (180 mg, 0.692 mmol), trimethylsilylethanol (160
mg, 1.36 mmol), and diethyl azodicarboxylate (115 .mu.L, 0.665
mmol) were added and the reaction mixture was stirred for another 1
day at room temperature. The reaction was worked up by removing the
solvents in vacuo and purifying the residue by silica gel
chromatography to provide 192 mg (85%) of the product as a clear
oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.03 (s, 9H), 0.05
(s, 9H), 0.93-0.96 (m, 2H), 1.20-1.29 (m, 2H), 1.78 (s, 3H),
2.01-2.32 (m, 4H), 2.17 (s, 3H), 2.51 (d, 1H, J=22 Hz), 2.58 (d,
1H, J=22 Hz), 2.50-2.60 (m, 1H), 3.37 (d, 2H, J=7 Hz), 3.72 (d, 6H,
J=11 Hz), 3.76 (s, 3H), 4.08 (appt t, 2H, J=8 Hz), 4.30 (appt t,
2H, J=8 Hz), 5.12 (s, 2H), 5.15-5.25 (m, 1H), 5.36-5.63 (m, 2H)
ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta. 29.3 ppm; MS (m/z)
705.3 [M+Na].sup.+.
##STR00544##
2-[4-(Hydroxy-methoxy-phosphoryl)-but-2-enyl]-6-[6-methoxy-7-methyl-3-oxo-
-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-he-
x-4-enoic acid 2-trimethylsilanyl-ethyl ester
[1566] A mixture of
2-[4-(dimethoxy-phosphoryl)-but-2-enyl]-6-[6-methoxy-7-methyl-3-oxo-4-(2--
trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-hex-4-en-
oic acid 2-trimethylsilanyl-ethyl ester (184 mg, 0.270 mmol) in
tert-butylamine (2.8 mL, 27 mmol) was heated at 60.degree. C. for
24 hours. The solution was allowed to cool to room temperature and
concentrated. The residue was purified by silica gel column
chromatography using MeOH/CH.sub.2Cl.sub.2 (0-30%) to provide 75 mg
of the product as a clear oil. .sup.1H NMR (300 MHz, CDCl.sub.3)
.delta. 0.01 (s, 9H), 0.04 (s, 9H), 0.89 (appt t, 2H, J=9 Hz), 1.23
(appt t, 2H, J=9 Hz), 1.77 (s, 3H), 2.01-2.31 (m, 4H), 2.17 (s,
3H), 2.36 (d, 1H, J=22 Hz), 2.38 (d, 1H, J=22 Hz), 2.52 (septet,
1H, J=9 Hz), 3.39 (d, 2H, J=7 Hz), 3.51 (d, 3H, J=11 Hz), 4.01-4.08
(m, 2H), 4.30 (dd, 2H, J=8, 9 Hz), 5.11 (s, 2H), 5.19 (br t, 1H,
J=6 Hz), 5.33-5.56 (m, 2H), 8.49 (br s, 1H) ppm; .sup.31P (121.4
MHz, CDCl.sub.3) .delta. 22.1 ppm; MS (m/z) 667.4 [M+Na].sup.+.
##STR00545##
2-{4-[(1-Ethoxycarbonyl-ethoxy)-methoxy-phosphoryl]-but-2-enyl}-6-[6-meth-
oxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-
-5-yl]-4-methyl-h ex-4-enoic acid 2-trimethylsilanyl-ethyl
ester
[1567] A solution of
2-[4-(hydroxy-methoxy-phosphoryl)-but-2-enyl]-6-[6-methoxy-7-methyl-3-oxo-
-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-he-
x-4-enoic acid 2-trimethylsilanyl-ethyl ester (67 mg, 0.10 mmol)
and PyBOP (234 mg, 0.450 mmol) in DMF (1.5 mL) was stirred with
ethyl (S)-(-)-lactate (53 mg, 0.45 mmol) and DIEA (174 .mu.L, 1.00
mmol) at ambient temperature for 1 hour, when complete consumption
of the starting materials was observed. The reaction was worked up
by addition of saturated aqueous sodium chloride and ethyl acetate.
The organic layer was separated and washed with 5% aqueous solution
of lithium chloride. The organic layer was dried in vacuo and the
residue was purified by silica gel chromatography using
MeOH--CH.sub.2Cl.sub.2 (0-20%) to provide 57 mg (74%) of the
desired product as a clear oil. .sup.1H NMR (300 MHz, CDCl.sub.3)
.delta. 0.02 (s, 9H), 0.05 (s, 9H), 0.88-0.94 (m, 2H), 1.20-1.30
(m, 2H), 1.29 (t, 3H, J=7 Hz), 1.45 (d, 3H, J=7 Hz), 1.78 (s, 3H),
2.01-2.31 (m, 4H), 2.17 (s, 3H), 2.50-2.58 (m, 1H), 2.65 (d, 1H,
J=22 Hz), 2.67 (d, 1H, J=22 Hz), 3.39 (d, 2H, J=7 Hz), 3.69 and
3.77 (d, 3H, J=11 Hz), 3.76 (s, 3H), 4.07 (appt t, 2H, J=7 Hz),
4.20 (dq, 2H, J=3, 7 Hz), 4.29 (appt t, 2H, J=9 Hz), 4.85-4.99 (m,
1H), 5.12 (s, 2H), 5.19 (br t, 1H, J=6 Hz), 5.33-5.61 (m, 2H) ppm;
.sup.31P (121.4 MHz, CDCl.sub.3) .delta. 28.9, 29.9 ppm; MS (m/z)
791.4 [M+Na].sup.+.
##STR00546##
2-{4-[(1-Ethoxycarbonyl-ethoxy)-methoxy-phosphoryl]-but-2-enyl}-6-(4-hydr-
oxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex--
4-enoic acid
[1568] A solution of
2-{4-[(1-ethoxycarbonyl-ethoxy)-methoxy-phosphoryl]-but-2-enyl}-6-[6-meth-
oxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-
-5-yl]-4-methyl-hex-4-enoic acid 2-trimethylsilanyl-ethyl ester (14
mg, 0.018 mmol) in THF (1 mL) was stirred with a 1M solution of
TBAF in THF (55 .mu.L, 0.055 mmol) for 1 hour. The reaction mixture
was concentrated, acidified with 1N HCl and extracted with EtOAc.
The organic layer was washed with brine and dried. The product was
purified by silica gel column chromatography EtOH-EtOAc (0-10%).
Further purification was performed by dissolving the product in
CH.sub.2Cl.sub.2 and passing the compound through a 13 mm Acrodisc
syringe filter with a 0.45 .mu.m Nylon membrane to provide 8 mg
(77%) of the product. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta.
0.92 (t, 3H, J=7 Hz), 1.30 (d, 3H, J=8 Hz), 1.79 (s, 3H), 2.10-2.39
(m, 4H), 2.15 (s, 3H), 2.53 (d, 1H, J=8 Hz), 2.65 (d, 1H, J=22 Hz),
2.68 (d, 1H, J=22 Hz), 3.38 (d, 2H, J=7 Hz), 3.70 and 3.74 (d, 3H,
J=11 Hz), 3.76 (s, 3H), 4.07 (m, 2H), 4.96 (dq, 1H, J=7 Hz), 5.20
(s, 2H), 5.27 (br t, 1H, J=7 Hz), 5.33-5.55 (m, 2H), 7.51-7.56 (m,
1H), 7.68-7.74 (m, 1H) ppm; .sup.31P (121.4 MHz, CDCl.sub.3)
.delta. 29.0, 30.1 ppm; MS (m/z) 569.2 [M+H].sup.+, 591.3
[M+Na].sup.+.
##STR00547##
2-{4-[(1-Carboxy-ethoxy)-hydroxy-phosphoryl]-but-2-enyl}-6-[6-methoxy-7-m-
ethyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]--
4-methyl-hex-4-enoic acid 2-trimethylsilanyl-ethyl ester
[1569] A solution of
2-{4-[(1-ethoxycarbonyl-ethoxy)-methoxy-phosphoryl]-but-2-enyl}-6-[6-meth-
oxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-
-5-yl]-4-methyl-hex-4-enoic acid 2-trimethylsilanylethyl ester (12
mg, 0.016 mmol) in tert-butylamine (1 mL, 9.6 mmol) was heated at
65.degree. C. for 16 hours. The solution was allowed to cool to
room temperature and concentrated to provide the crude product as
an oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.03 (s, 9H),
0.04 (s, 9H), 0.86-0.98 (m, 2H), 1.22-1.33 (m, 2H), 1.50 (d, 3H,
J=7 Hz), 1.78 (s, 3H), 2.05-2.30 (m, 4H), 2.10 (s, 3H), 2.48-2.63
(m, 3H), 3.40 (d, 2H, J=7 Hz), 3.76 (s, 3H), 4.08 (appt t, 2H, J=9
Hz), 4.25-4.33 (m, 2H), 4.75-4.84 (m, 1H), 5.13 (s, 2H), 5.15-5.23
(m, 1H), 5.33-5.55 (m, 2H) ppm; .sup.31P (121.4 MHz, CDCl.sub.3)
.delta. 28.9 ppm; MS (m/z) 725.3 [M-H].sup.-.
##STR00548##
2-{4-[(1-Carboxy-ethoxy)-hydroxy-phosphoryl]-but-2-enyl}-6-(4-hydroxy-6-m-
ethoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl-hex-4-enoic
acid
[1570] A solution of crude
2-{4-[(1-carboxy-ethoxy)-hydroxy-phosphoryl]-but-2-enyl}-6-[6-methoxy-7-m-
ethyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]--
4-methyl-hex-4-enoic acid 2-trimethylsilanyl-ethyl ester
(AC-2101-59) and tetrabutylammonium fluoride in THF (1M, 54 .mu.L,
0.054 mmol) was stirred with THF (1 mL) for 2 hours at ambient
temperature, when more tetrabutylammonium fluoride in THF (54
.mu.L, 0.054 mmol) was added. The reaction was stirred for an
additional 16 hours, by which time the reaction was complete. The
reaction mixture was concentrated in vacuo and the product was
purified by RP HPLC using a Phenomenex Synergi 5.mu. Hydro RP 80A
column (50.times.21.2 mm) with eluents of H.sub.2O, 0.1%
TFA-CH.sub.3CN, 0.1% TFA to provide the product (8.0 mg) as a clear
oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 1.51 (d, 3H, J=7
Hz), 1.79 (s, 3H), 2.05-2.40 (m, 4H), 2.11 (s, 3H), 2.49-2.71 (m,
3H), 3.38 (d, 2H, J=6 Hz), 3.76 (s, 3H), 4.85 (br s, 1H), 5.20 (s,
2H), 5.21-5.30 (m, 1H), 5.33-5.63 (m, 2H) ppm; .sup.31P (121.4 MHz,
CDCl.sub.3) .delta. 27.7 ppm; MS (m/z) 525.2 [M-H].sup.-.
##STR00549##
2-{4-[(1-Ethoxycarbonyl-ethylamine)-methoxy-phosphoryl]-but-2-enyl}-6-[6--
methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzof-
uran-5-yl]-4-methyl-hex-4-enoic acid 2-trimethylsilanyl-ethyl
ester
[1571] A solution of
2-[4-(hydroxy-methoxy-phosphoryl)-but-2-enyl]-6-[6-methoxy-7-methyl-3-oxo-
-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-he-
x-4-enoic acid 2-trimethylsilanyl-ethyl ester (20 mg, 0.030 mmol),
PyBOP (62.4 mg, 0.120 mmol) in DMF (1.0 mL) was stirred with
L-alanine ethyl ester hydrochloride (18 mg, 0.12 mmol) and DIEA (26
.mu.L, 0.15 mmol) at ambient temperature for 1 hour, when complete
consumption of the starting materials was observed. The reaction
was worked up by addition of water until the reaction solution
became cloudy. DMF was added dropwise until the mixture became
clear again. The reaction mixture was filtered through Acrodisc (13
mm syringe filter with a 0.45 .mu.m Nylon membrane) and purified by
RP HPLC using a Phenomenex Synergi 5.mu. Hydro RP 80A column
(50.times.21.2 mm), eluting with water and acetonitrile. The
fractions containing the product were pooled together and
concentrated in vacuo to remove the acetonitrile. The remaining
solution was saturated with sodium chloride and extracted with
EtOAc and acetonitrile to provide 7.2 mg of the product. .sup.1H
NMR (300 MHz, CDCl.sub.3) .delta. 0.03 (s, 9H), 0.05 (s, 9H), 0.923
(appt t, 2H, J=8 Hz), 1.18-1.31 (m, 5H), 1.41 (t, 3H, J=7 Hz), 1.78
(s, 3H), 2.03-2.36 (m, 4H), 2.18 (s, 3H), 2.43-2.63 (m, 3H),
3.10-3.30 (m, 1H), 3.40 (d, 2H, J=7 Hz), 3.62 and 3.65 (d, 3H, J=11
Hz), 3.76 (s, 3H), 4.03-4.12 (m, 2H), 4.20 (dq, 2H, J=2, 7 Hz),
4.29 (appt t, 2H, J=8 Hz), 5.12 (s, 2H), 5.18-5.28 (m, 1H),
5.33-5.67 (m, 2H) ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta.
30.4, 31.2 ppm; MS (m/z) 790.4 [M+Na].sup.+.
##STR00550##
2-{4-[(1-Ethoxycarbonyl-ethylamine)-methoxy-phosphoryl]-but-2-enyl}-6-(4--
hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-methyl--
hex-4-enoic acid
[1572] To a solution of
2-{4-[(1-ethoxycarbonyl-ethylamine)-methoxy-phosphoryl]-but-2-enyl}-6-[6--
methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzof-
uran-5-yl]-4-methyl-hex-4-enoic acid 2-trimethylsilanyl-ethyl ester
(7.2 mg, 9.38 mmol) in THF (1 mL) was added TBAF (40 .mu.L, 1M
solution in THF) at room temperature. The reaction mixture was
stirred for 20 minutes, when the starting material was completely
converted to the desired product as judged by LCMS. The reaction
mixture was dried in vacuo and re-dissolved in DMF. The product was
purified by RP HPLC using a Phenomenex Synergi 5.mu. Hydro RP 80A
column (50.times.21.2 mm) with eluents of H.sub.2O--CH.sub.3CN. The
fractions containing the desired product were pooled and further
purified on Dowex 50WX8-400 packed on a 4.5 cm.times.2 cm column to
elute the sodium salt at H.sub.2O-- MeOH (1:1), providing 3.2 mg of
the desired product. .sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.26
(dd, 3H, J=4, 7 Hz), 1.37 (t, 3H, J=8 Hz), 1.80 (s, 3H), 2.00-2.22
(m, 4H), 2.10 (s, 3H), 2.25-2.60 (m, 3H), 3.37 (d, 2H, J=7 Hz),
3.60 and 3.65 (d, 3H, J=11 Hz), 3.74 (s, 3H), 3.83-3.96 (m, 1H),
4.18 (q, 2H, J=8 Hz), 5.15 (s, 2H), 5.25-5.42 (m, 2H), 5.55-5.69
(m, 1H) ppm; .sup.31P (121.4 MHz, CD.sub.3OD) .delta. 33.8, 34.2
ppm; MS (m/z) 568.2 [M+H].sup.+, 590.3 [M+Na].sup.+.
##STR00551##
6-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2-[-
4-(hydroxy-methoxy-phosphoryl)-but-2-enyl]-4-methyl-hex-4-enoic
acid
[1573] To a solution of
2-[4-(hydroxy-methoxy-phosphoryl)-but-2-enyl]-6-[6-methoxy-7-methyl-3-oxo-
-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-he-
x-4-enoic acid 2-trimethylsilanylethyl ester (11 mg, 0.016 mmol) in
THF (1 mL) was added TBAF (50 .mu.L, 1M solution in THF) at room
temperature. The solution was stirred for 16 hours and
concentrated. The solution was dried under reduced pressure and
re-suspended in DMF (0.8 mL) and water (0.25 mL). The solution was
filtered through Acrodisc (13 mm syringe filter with a 0.45 .mu.m
Nylon membrane) and purified by RP HPLC using a Phenomenex Synergi
5.mu. Hydro RP 80A column (50.times.21.2 mm) with eluents of
H.sub.2O, 0.1% TFA-CH.sub.3CN, 0.1% TFA. The product from the
column was subjected to ion exchange chromatography (Sodium salt
form of Dowex 50WX8-400) using a 2.times.4.5 cm column eluting with
H.sub.2O-MeOH (1:1) to provide 7.5 mg of the desired product as an
oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 1.80 (s, 3H),
2.01-2.29 (m, 5H), 2.11 (s, 3H), 2.35 (d, 2H, J=22 Hz), 3.38 (d,
2H, J=7 Hz), 3.53 (d, 3H, J=11 Hz), 3.75 (s, 3H), 5.19 (s, 2H),
5.26 (t, 1H, J=6 Hz), 5.43-5.54 (m, 2H) ppm; .sup.31P (121.4 MHz,
CDCl.sub.3) .delta. 23.5 ppm; MS (m/z) 469.2 [M+H].sup.+, 491.3
[M+Na].sup.+.
##STR00552## ##STR00553##
6-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-4-methyl-hex-4-enoic acid methyl ester
[1574] To a solution of
6-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-m-
ethyl-hex-4-enoic acid methyl ester (222 mg, 0.66 mmol),
triphenylphosphine (260 mg, 0.996 mmol), and diethyl
azodicarboxylate (173 mg, 0.996 mmol) in THF (3 mL) at 0.degree. C.
was added a solution of 2-trimethylsilylethanol (142 .mu.L, 0.996
mmol) in THF (3 mL). The resulting yellow solution was allowed to
warm to room temperature and stirred overnight. The reaction was
concentrated to dryness and ether and hexanes were added.
Triphenylphosphine oxide was removed by filtration and the filtrate
was concentrated and purified by silica gel chromatography to
provide 248 mg of the desired product as a colorless oil. .sup.1H
NMR (300 MHz, CDCl.sub.3) .delta. 0.03 (s, 9H), 1.18-1.30 (m, 2H),
1.81 (s, 3H), 2.18 (s, 3H), 2.25-2.33 (m, 2H), 2.37-2.45 (m, 2H),
3.42 (d, 2H, J=7 Hz), 3.62 (s, 3H), 3.77 (s, 3H), 4.25-4.35 (m,
2H), 5.13 (s, 2H), 5.12-5.22 (m, 1H) ppm.
##STR00554##
[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobe-
nzofuran-5-yl]-acetaldehyde
[1575] A solution of
6-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-4-methyl-hex-4-enoic acid methyl ester (618 mg,
1.42 mmol) in MeOH (10 mL), CH.sub.2Cl.sub.2 (10 mL) and pyridine
(50 .mu.L, 0.618 mmol) was cooled to -70.degree. C. using a dry
ice/acetone bath according to the procedure of Smith, D. B. et al.,
J. Org. Chem., 1996, 61, 6, 2236. A stream of ozone was bubbled
through the reaction via a gas dispersion tube until the reaction
became blue in color (15 minutes). The ozone line was replaced with
a stream of nitrogen and bubbling continued for another 15 minutes,
by which time the blue color had disappeared. To this solution,
thiourea (75.7 mg, 0.994 mmol) was added in one portion at
-70.degree. C., and the cooling bath was removed. The reaction was
allowed to warm to room temperature and stirred for 15 hours. The
reaction was worked up by filtration to remove solid thiourea
S-dioxide, and then partitioned between CH.sub.2Cl.sub.2 and water.
The organic layer was removed. The aqueous layer was washed with
CH.sub.2Cl.sub.2 one more time, and the organic extracts were
combined. The organic layer was washed with aqueous 1N HCl,
saturated NaHCO.sub.3 and brine. The organic extracts were dried in
vacuo and the residue was purified to by silica gel chromatography
to afford 357 mg (75%) of the product as a white solid. .sup.1H NMR
(300 MHz, CDCl.sub.3) .delta. -0.01 (s, 9H), 1.05-1.15 (m, 2H),
2.15 (s, 3H), 3.69 (s, 3H), 3.78 (d, 2H, J=1 Hz), 4.27-4.39 (m,
2H), 5.11 (s, 2H), 9.72 (d, 1H, J=1 Hz) ppm.
##STR00555##
4-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-2-methyl-but-2-enal
[1576]
[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-acetaldehyde (70 mg, 0.21 mmol) in toluene (2
mL) was heated at 100.degree. C. with
2-(triphenyl-phosphanylidene)-propionaldehyde (72.9 mg, 0.23 mmol)
overnight. A second portion of
2-(triphenyl-phosphanylidene)-propionaldehyde (33 mg, 0.11 mmol)
was added and the reaction mixture was heated for an additional
day. After concentration, the residue was purified by silica gel
chromatography to provide 54 mg (83%) of the desired product as a
pale yellow oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.00 (s,
9H), 1.10-1.21 (m, 2H), 1.87 (s, 3H), 2.16 (s, 3H), 3.67-3.76 (m,
2H), 3.74 (s, 3H), 4.27-4.39 (m, 2H), 5.11 (s, 2H), 6.40-6.48 (m,
1H), 9.2 (s, 1H) ppm.
##STR00556##
6-(4-Hydroxy-3-methyl-but-2-enyl)-5-methoxy-4-methyl-7-(2-trimethylsilany-
l-ethoxy)-3H-isobenzofuran-1-one
[1577] A solution of
4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-2-methyl-but-2-enal (103 mg, 0.27 mmol) in
methanol (5 mL) was cooled to 0.degree. C. A solution of CeCl.sub.3
(0.68 mL, MeOH: H.sub.2O, 9:1) was added, followed by LiBH.sub.4
(0.14 mL, 0.28 mmol of a 2M solution in THF). The ice bath was
removed and the reaction mixture was allowed to warm to room
temperature. The reaction mixture was stirred for an additional 40
minutes whereupon TLC indicated complete consumption of starting
aldehyde. The reaction was worked up by addition of aqueous 1N HCl
(0.5 mL) and the product was extracted with CH.sub.2Cl.sub.2. The
organic layer was washed with saturated aqueous sodium bicarbonate
solution and brine. The organic layer was concentrated under
reduced pressure and the residue was purified by silica gel
chromatography to provide 100 mg (97%) of the product as a clear
liquid. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.00 (s, 9H),
1.20 (dd, 2H, J=7, 8 Hz), 1.81 (s, 3H), 2.13 (s, 3H), 3.38-3.50 (m,
2H), 3.74 (s, 3H), 3.95 (s, 2H), 4.27 (dd, 2H, J=7, 8 Hz), 5.08 (s,
2H), 5.17-5.44 (m, 1H) ppm.
##STR00557##
6-(2-Hydroxy-ethyl)-5-methoxy-4-methyl-7-(2-trimethylsilanyl-ethoxy)-3H-i-
sobenzofuran-1-one
[1578] To a solution of
[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobe-
nzofuran-5-yl]-acetaldehyde (97 mg, 0.29 mmol) in THF (5 mL) was
added an aliquot of a 2 M LiBH.sub.4 in THF (150 .mu.L, 0.300
mmol). The reaction mixture was stirred at room temperature for 1
hour when complete consumption of the starting materials was
observed by TLC. The reaction mixture was worked up by addition of
an aqueous 1N HCl solution and extraction with EtOAc. The organic
layer was dried in vacuo and the residue was purified by silica gel
chromatography to provide the product. .sup.1H NMR (300 MHz,
CDCl.sub.3) .delta. 0.00 (s, 9H), 1.20 (dd, 2H, J=7, 9 Hz), 2.07
(br s, 1H), 2.14 (s, 3H), 2.97 (t, 2H, J=6 Hz), 3.76 (t, 2H, J=6
Hz), 3.77 (s, 3H), 4.32 (dd, 2H, J=7, 8 Hz), 5.08 (s, 2H) ppm.
##STR00558##
{2-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-is-
obenzofuran-5-yl]-ethoxymethyl}-phosphonic acid diisopropyl
ester
[1579] A mixture of
6-(2-hydroxy-ethyl)-5-methoxy-4-methyl-7-(2-trimethylsilanyl-ethoxy)-3H-i-
sobenzofuran-1-one (79 mg, 0.23 mmol) was heated with
bromomethylphosphonic acid diisopropyl ester (120 mg, 0.46 mmol) in
the presence of lithium t-butoxide (22 mg, 0.27 mmol) in DMF (2 mL)
at 70.degree. C. overnight. The reaction mixture was purified by RP
HPLC (acetonitrile and 0.1% aqueous CF.sub.3COOH) to provide the
desired product. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.00 (s,
9H), 1.13-1.25 (m, 2H), 1.26 (t, 12H, J=6 Hz), 2.12 (s, 3H), 2.98
(t, 2H, J=7 Hz), 3.60-3.73 (m, 4H), 3.77 (s, 3H), 4.05-4.16 (m,
2H), 4.62-4.74 (m, 2H), 5.07 (s, 2H) ppm; MS (m/z) 539
[M+Na].sup.+.
Example 296
[1580] Representative compounds of the invention can be prepared as
illustrated below.
##STR00559##
[2-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-et-
hoxymethyl]-phosphonic acid
[1581] To a solution of
{2-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-is-
obenzofuran-5-yl]-ethoxymethyl}-phosphonic acid diisopropyl ester
(7.5 mg, 0.014 mmol) in acetonitrile (2 mL) and 2,6-lutidine (25
.mu.L, 0.21 mmol) was added trimethylsilyl bromide (27 .mu.L, 0.21
mmol) at room temperature. The reaction was allowed to proceed for
18 hours when completion of the reaction was indicated by LCMS. The
reaction was quenched by addition of MeOH and concentration. The
residue was purified by RP-HPLC using a C18 column. The collected
product was dissolved in a solution of 10% TFA/CH.sub.2Cl.sub.2 to
assure complete deprotection. The reaction mixture was lyophilized
to provide the desired product. .sup.1H NMR (300 MHz, CD.sub.3OD)
.delta. 2.12 (s, 3H), 2.98 (t, 2H, J=7 Hz), 3.66-3.76 (m, 4H), 3.78
(s, 3H), 5.21 (s, 2H) ppm; MS (m/z) 331 [M-H].sup.-.
##STR00560##
Example 297
[1582] Representative compounds of the invention can be prepared as
illustrated below.
##STR00561##
6-(4-Bromo-3-methyl-but-2-enyl)-7-hydroxy-5-methoxy-4-methyl-3H-isobenzof-
uran-1-one
[1583] Polymer-supported triphenylphosphine (3 mmol/g, 0.5 g) was
soaked in dichloromethane (10 mL) for 1 hour
7-Hydroxy-6-(4-hydroxy-3-methyl-but-2-enyl)-5-methoxy-4-methyl-3H-isobenz-
ofuran-1-one (100 mg, 0.36 mmol) and carbon tetrabromide (143 mg,
0.43 mmol) were added sequentially and the mixture was shaken for 1
hour at room temperature. More carbon tetrabromide (143 mg, 0.43
mmol) was added and the mixture was shaken further for 1 hour The
mixture was filtered and the filtrate was concentrated. The residue
was chromatographed on silica gel (0% to 60% ethyl acetate/hexanes)
to afford
6-(4-bromo-3-methyl-but-2-enyl)-7-hydroxy-5-methoxy-4-methyl-3H-isobenzof-
uran-1-one as an oil (52 mg, 42%); .sup.1H NMR (300 MHz,
CDCl.sub.3) .delta. 1.95 (s, 3H), 2.16 (s, 3H), 3.44 (d, J=7.2,
2H), 3.78 (s, 3H), 3.98 (s, 2H), 5.21 (s, 2H), 5.68 (t, J=7.2 Hz,
1H), 7.71 (brs, 1H) ppm.
##STR00562##
[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyl]-phosphonic acid dimethyl ester
[1584] A solution of
6-(4-bromo-3-methyl-but-2-enyl)-7-hydroxy-5-methoxy-4-methyl-3H-isobenzof-
uran-1-one (33 mg, 0.097 mmol) in trimethylphosphite (1.0 mL, 8.5
mmol) was heated to 100.degree. C. for 1 hour, whereupon complete
reaction was indicated by LCMS. The reaction was worked up by
removal of the excess reagent under reduced pressure and the
residue was purified by silica gel chromatography using
EtOAc-hexanes (20-100%) to provide 20 mg (60%) of the desired
product. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 1.90 (s, 3H),
2.09 (s, 3H), 2.48 (d, 2H, J=22 Hz), 3.38 (t, 2H, J=6 Hz), 3.64 (d,
6H, J=11 Hz), 3.72 (s, 3H), 5.14 (s, 2H), 5.33 (q, 1H, J=6 Hz),
7.65 (br s, 1H) ppm; MS (m/z) 371 [M+H].sup.+.
Example 298
[1585] Representative compounds of the invention can be prepared as
illustrated below.
##STR00563##
[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyl]-phosphonic acid
[1586] To a solution of
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyl]-phosphonic acid dimethyl ester (18 mg, 0.049
mmol) in acetonitrile (2 mL) was added TMSBr (63 .mu.L, 0.49 mmol)
and 2,6-lutidine (85 .mu.L, 0.73 mmol) at 0.degree. C. The reaction
solution was allowed to warm to room temperature and stirred for 2
hours when completion of the reaction was observed by LCMS. The
reaction was cooled to 0.degree. C. and quenched by the addition of
MeOH. The reaction mixture was concentrated under reduced pressure
and the residue was purified by RP HPLC using a C18 column with a
gradient of H.sub.2O-acetonitrile (5-0%) over 20 minutes to provide
12.2 mg (73%) of the product. .sup.1H NMR (300 MHz, CD.sub.3OD)
.delta. 1.95 (s, 3H), 2.15 (s, 3H), 2.48 (d, 2H, J=22 Hz), 3.44 (t,
2H, J=6 Hz), 3.79 (s, 3H), 5.24 (s, 2H), 5.38 (q, 1H, J=7 Hz), 6.87
(br s, 1H) ppm; MS (m/z) 341 [M-H].sup.-.
Example 299
[1587] Representative compounds of the invention can be prepared as
illustrated below.
##STR00564##
[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid monophenyl ester and
[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid diphenyl ester
[1588] To a solution of
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid (49 mg, 0.13 mmol) in
DMF (0.4 mL) and phenol (62 mg, 0.65 mmol) was added dicyclohexyl
carbodiimide (107 mg, 0.52 mmol) and DMAP (8 mg, 0.065 mmol) in DMF
(0.6 mL), slowly at 0.degree. C. The reaction was allowed to warm
to room temperature and heated to 140.degree. C. for 10 hours.
After cooling to room temperature the mixture was filtered and
extracted with aqueous 1N NaOH solution. The aqueous layer was
acidified with aqueous 1N HCl and extracted with EtOAc. The organic
layer was dried over Na.sub.2SO.sub.4 and concentrated to dryness.
The residue was purified by RP HPLC to provide 18.5 mg of
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid monophenyl ester, as a
pale yellow solid and 4.1 mg of
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid diphenyl ester (minor
product) also as a pale yellow solid. Major product: .sup.1H NMR
(300 MHz, CD.sub.3OD) .delta. 1.82 (s, 3H), 2.16 (s, 3H), 3.46 (d,
2H, J=7 Hz), 3.70 (d, 2H, J=8 Hz), 3.77 (s, 3H), 3.96 (s, 2H), 5.25
(s, 2H), 5.52 (t, 1H, J=8 Hz), 7.10-7.21 (m, 3H), 7.30 (t, 2H, J=8
Hz) ppm; .sup.31P (121.4 MHz, CD.sub.3OD) .delta. 17.3 ppm; MS
(m/z) 449.0 [M+H].sup.+, 471.2 [M+Na].sup.+. Minor product: .sup.1H
NMR (300 MHz, CD.sub.3OD) .delta. 1.82 (s, 3H), 2.15 (s, 3H), 3.47
(d, 2H, J=7 Hz), 3.77 (s, 3H), 3.98-4.06 (m, 4H), 5.25 (s, 2H),
5.50-5.61 (m, 1H), 7.10-7.25 (m, 6H), 7.30-7.41 (m, 4H) ppm;
.sup.31P (121.4 MHz, CD.sub.3OD) .delta. 16.3 ppm; MS (m/z) 525.2
[M+H].sup.+, 547.2 [M+Na].sup.+.
Example 300
[1589] Representative compounds of the invention can be prepared as
illustrated below.
##STR00565##
2-{[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-
-2-methyl-but-2-enyloxymethyl]-phenoxy-phosphinoyloxy}-propionic
acid ethyl ester
[1590] To a solution of
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid monophenyl ester (18.5
mg, 0.040 mmol) and ethyl (S)-(-)-lactate (47 .mu.L, 0.400 mmol) in
pyridine (0.5 mL) was added PyBOP (32 mg, 0.060 mmol). The solution
was stirred at room temperature for 1 hour, when an additional
portion of PyBOP (21 mg, 0.040 mmol) was added. The solution was
stirred for another hour and concentrated. The residue was purified
by HPLC to provide 7.5 mg of the desired product as a clear oil.
.sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.22 and 1.25 (t, 3H, J=7
Hz), 1.42 and 1.50 (d, 3H, J=7 Hz), 1.82 and 1.83 (s, 3H), 2.16 (s,
3H), 3.47 (d, 2H, J=7 Hz), 3.78 (s, 3H), 3.89 (d, 1H, J=8 Hz),
3.93-4.02 (m, 3H), 4.10-4.22 (m, 2H), 4.94-5.08 (m, 1H), 5.25 (s,
2H), 5.50-5.60 (m, 1H), 7.15-7.27 (m, 3H), 7.33-7.41 (m, 2H) ppm;
.sup.31P (121.4 MHz, CD.sub.3OD) .delta. 18.9, 20.3 ppm
(diastereomers at phosphorus); MS (m/z) 549.2 [M+H].sup.+, 571.3
[M+Na].sup.+.
Example 301
[1591] Representative compounds of the invention can be prepared as
illustrated below.
##STR00566##
2-{[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-
-2-methyl-but-2-enyloxymethyl]-phenoxy-phosphinoylamino}-propionic
acid ethyl ester
[1592] To a solution of
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid monophenyl ester (20
mg, 0.045 mmol) and L-alanine ethyl ester hydrochloride (68.5 mg,
0.45 mmol) in pyridine (1.0 mL) was added PyBOP (70 mg, 0.14 mmol).
After stirring overnight, the mixture was concentrated and the
residue purified by RP HPLC using a C18 column with a gradient of
H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA to provide 3.6 mg of the
product as a colorless gel. .sup.1H NMR (300 MHz, CD.sub.3OD)
.delta. 1.17-1.3 (m, 6H), 1.8-1.9 (m, 3H), 2.16 (s, 3H), 3.17 (m,
1H), 3.47 (d, 2H), 3.72-3.8 (m, 5H), 3.92-4.2 (m, 4H), 5.25 (s,
2H), 5.54 (m, 1H), 7.18 (m, 3H), 7.33 (m, 2H) ppm; .sup.31P (121.4
MHz, CD.sub.3OD) .delta. 24.1, 25.0 ppm (diastereomers at
phosphorus); MS (m/z) 546.2 [M-H].sup.+.
Example 302
[1593] Representative compounds of the invention can be prepared as
illustrated below.
##STR00567##
[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid monomethyl ester
[1594] To a solution of
[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2--
methyl-but-2-enyloxymethyl]-phosphonic acid diphenyl ester (53 mg,
0.1 mmol) in methanol (0.5 mL) was added an aqueous solution of 1N
NaOH (300 .mu.L). After stirring overnight, the mixture was
concentrated and the residue purified by RP HPLC using a C18 column
with a gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA to
provide 5 mg of the product as a colorless gel, together with the
phosphonic acid monophenyl ester (7 mg) and the phosphonic acid
dimethyl ester (14.5 mg). .sup.1H NMR (300 MHz, CD.sub.3OD) .delta.
1.84 (s, 3H), 2.16 (s, 3H), 3.47 (d, 2H, J=7 Hz), 3.6 (d, 2H, J=12
Hz), 3.75 (d, 3H, J=11 Hz), 3.79 (s, 3H), 3.94 (s, 2H), 5.26 (s,
2H), 5.53 (t, 1H, J=7 Hz) ppm; .sup.31P (121.4 MHz, CD.sub.3OD)
.delta. 21.5 ppm; MS (m/z) 385.2 [M-H].sup.+, 387.1
[M+H].sup.+.
Example 303
[1595] Representative compounds of the invention can be prepared as
illustrated below.
##STR00568##
(2-{4-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphonic
acid diethyl ester
[1596] To a solution of
4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-2-methyl-but-2-enal (84 mg, 0.22 mmol),
(2-amino-ethyl)-phosphonic acid diethyl ester oxalate (91 mg, 0.33
mmol), and sodium triacetoxyborohydride (93 mg, 0.44 mmol) in DMF
(1.5 mL) was added acetic acid (60 .mu.L, 1.0 mmol) at room
temperature. The solution was stirred for 2 days when it was
quenched by addition of saturated aqueous sodium bicarbonate
solution and EtOAc. The organic layer was separated and
concentrated under reduced pressure. The residue was purified by RP
HPLC using a C18 column with a gradient of H.sub.2O, 0.1%
TFA-acetonitrile, 0.1% TFA to provide 115 mg (96%) of the product
as an oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.04 (s, 9H),
1.16-1.27 (m, 2H), 1.34 (t, 6H, J=7 Hz), 1.94 (s, 3H), 2.18 (s,
3H), 2.20-2.31 (m, 2H), 3.13-3.31 (m, 2H), 3.48 (d, 2H, J=7 Hz),
3.54 (s, 2H), 3.78 (s, 3H), 4.14 (pent, 4H, J=7 Hz), 4.30-4.37 (m,
2H), 5.13 (s, 2H), 5.65 (t, 1H, J=7 Hz), 6.23 (br s, 2H) ppm;
.sup.31P (121.4 MHz, CDCl.sub.3) .delta. 27.8 ppm; MS (m/z) 542.3
[M+H].sup.+, 564.2 [M+Na].sup.+.
##STR00569##
{2-[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-
-2-methyl-but-2-enylamino]-ethyl}-phosphonic acid
[1597] A solution of
(2-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphonic
acid diethyl ester (30 mg, 0.055 mmol), TMSBr (72 .mu.L, 0.55
mmol), and 2,6-lutidine (64 .mu.L, 0.55 mmol) was stirred in
CH.sub.2Cl.sub.2 (1 mL) and DMF (0.5 mL) for 1 hour at ambient
temperature. The reaction mixture was purified by RP HPLC using a
C18 column with a gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1%
TFA to provide 7.8 mg of the product as a white solid. .sup.1H NMR
(300 MHz, CD.sub.3OD) .delta. 1.96 (s, 3H), 1.95-2.07 (m, 2H), 2.16
(s, 3H), 3.10-3.24 (m, 2H), 3.51 (d, 2H, J=7 Hz), 3.57 (s, 2H),
3.81 (s, 3H), 5.25 (s, 2H), 5.73 (t, 1H, J=7 Hz) ppm; .sup.31P
(121.4 MHz, CD.sub.3OD) .delta. 20.2 ppm; .sup.19F NMR (282.6 MHz,
CD.sub.3OD) .delta. -74.0 ppm; MS (m/z) 386.3 [M+H].sup.+.
Example 304
[1598] Representative compounds of the invention can be prepared as
illustrated below.
##STR00570##
[2-(Methanesulfonyl-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-et-
hoxy)-1,3-dihydro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-amino)-ethyl]-p-
hosphonic acid diethyl ester
[1599] A solution of
(2-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphonic
acid diethyl ester (45 mg, 0.092 mmol) in CH.sub.2Cl.sub.2 (0.5 mL)
was stirred with methanesulfonyl chloride (21 .mu.L, 0.28 mmol) and
pyridine (45 .mu.L, 0.55 mmol) at ambient temperature overnight.
The reaction was quenched by addition of 2 drops of water. The
reaction mixture was concentrated and purified by RP HPLC using a
C18 column with a gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1%
TFA to provide 36 mg of the product (63%) as a clear gel. .sup.1H
NMR (300 MHz, CDCl.sub.3) .delta. 0.05 (s, 9H), 1.18-1.29 (m, 2H),
1.29 (t, 6H, J=7 Hz), 1.85 (s, 3H), 2.00-2.13 (m, 2H), 2.19 (s,
3H), 2.85 (s, 3H), 3.32-3.43 (m, 2H), 3.47 (d, 2H, J=7 Hz), 3.69
(s, 2H), 3.79 (s, 3H), 4.05 (pent, 4H, J=7 Hz), 4.30-4.37 (m, 2H),
5.13 (s, 2H), 5.45 (t, 1H, J=7 Hz) ppm; .sup.31P (121.4 MHz,
CD.sub.3Cl) .delta. 27.5 ppm; MS (m/z) 642.2 [M+Na].sup.+.
##STR00571##
(2-{[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl-
)-2-methyl-but-2-enyl]-methanesulfonyl-amino}-ethyl)-phosphonic
acid
[1600] A solution of
[2-(methanesulfonyl-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-et-
hoxy)-1,3-dihydro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-amino)-ethyl]-p-
hosphonic acid diethyl ester (18 mg, 0.029 mmol) in acetonitrile
(0.5 mL) was stirred with TMSBr (38 .mu.L, 0.29 mmol) and
2,6-lutidine (34 .mu.L, 0.29 mmol) for 2 hours at room temperature.
The reaction was worked up by addition of EtOAc and aqueous 1N HCl.
The organic layer was washed with brine and the solvent was removed
in vacuo. The residue was suspended in a solution of 10%
TFA-CH.sub.2Cl.sub.2 for 10 minutes before it was dried to provide
9.9 mg of the desired product (73%) as a white solid. .sup.1H NMR
(300 MHz, DMSO-d6) .delta. 1.76 (s, 3H), 1.76-1.88 (m, 2H), 2.10
(s, 3H), 2.87 (s, 3H), 3.24-3.35 (m, 2H), 3.39 (d, 2H, J=7 Hz),
3.65 (s, 2H), 3.75 (s, 3H), 5.22 (s, 2H), 5.41-5.48 (m, 1H) ppm;
.sup.31P (121.4 MHz, DMSO-d6) .delta. 21.4 ppm; MS (m/z) 464.1
[M+H].sup.+.
Example 305
[1601] Representative compounds of the invention can be prepared as
illustrated below.
##STR00572##
[2-(Acetyl-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-
-dihydro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-amino)-ethyl]-phosphonic
acid diethyl ester
[1602] To a solution of
(2-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphonic
acid diethyl ester (32 mg, 0.059 mmol) in acetic acid (0.5 mL) was
added acetic anhydride (0.5 mL). The solution was stirred at room
temperature for 90 minutes when it was quenched by addition of 2
drops of water. The solution was dried in vacuo and the residue was
purified by RP HPLC using a C18 column with a gradient of H.sub.2O,
0.1% TFA-acetonitrile, 0.1% TFA to provide 28 mg of the product
(81%) as a clear gel. The NMR data of this compound shows two
rotamers in a ratio of 70:30. .sup.1H NMR (300 MHz, CDCl.sub.3)
.delta. 0.05 (s, 9H), 1.17-1.27 (m, 2H), 1.30 and 1.31 (t, 6H, J=7
Hz), 1.70-1.79 (m, 2H), 1.76 (s, 3H), 2.00 (s, 3H), 2.18 (s, 3H),
3.40-3.52 (m, 2H), 3.46 (d, 2H, J=7 Hz), 3.77 (s, 3H), 3.79 and
3.93 (s, 3H), 4.07 (pent, 4H, J=7 Hz), 4.27-4.35 (m, 2H), 5.13 (s,
2H), 5.22-5.30 (m, 1H) ppm; .sup.31P (121.4 MHz, CDCl.sub.3)
.delta. 27.5 and 28.9 ppm; MS (m/z) 584.1 [M+H].sup.+, 606.2
[M+Na].sup.+.
##STR00573##
(2-{Acetyl-[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofur-
an-5-yl)-2-methyl-but-2-enyl]-amino}-ethyl)-phosphonic acid
[1603] To a solution of
[2-(acetyl-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-
-dihydro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-amino)-ethyl]-phosphonic
acid diethyl ester (14 mg, 0.024 mmol) in acetonitrile (0.5 mL) was
added TMSBr (31 .mu.L, 0.24 mmol) and 2,6-lutidine (28 .mu.L, 0.24
mmol). The solution was stirred at room temperature for 1 hour. The
reaction was quenched by addition of methanol and aqueous 1N HCl.
The product was extracted with EtOAc. The combined organic extracts
were dried over Na.sub.2SO.sub.4 and concentrated in vacuo. The
product was purified by RP HPLC using a C18 column with a gradient
of H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA to provide 5.4 mg of
the product (53%) as a white solid. The NMR data of this compound
shows two rotamers. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 1.67
and 1.73 (s, 3H), 1.85-2.12 (m, 5H), 2.13 (s, 3H), 3.30-3.61 (m,
4H), 3.75 (s, 3H), 3.76 (br s, 2H), 5.17 (s, 2H), 5.31 (br s, 1H)
ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta. 27.5 and 28.8 ppm; MS
(m/z) 428.2 [M+H].sup.+, 450.2 [M+Na].sup.+.
Example 306
[1604] Representative compounds of the invention can be prepared as
illustrated below.
##STR00574##
[2-(Benzyl-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-
-dihydro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-amino)-ethyl]-phosphonic
acid diethyl ester
[1605] A solution of
(2-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphonic
acid diethyl ester (30 mg, 0.055 mmol), benzaldehyde (5.6 .mu.L,
0.055 mmol), and sodium triacetoxyborohydride (23 mg, 0.11 mmol)
was stirred with acetic acid (15.7 .mu.L, 0.28 mmol) in DMF (0.5
mL) at room temperature over night. The reaction was quenched with
a 10% aqueous Na.sub.2CO.sub.3 solution and the product was
extracted with EtOAc. The organic layer was dried and concentrated
under reduced pressure. The product was purified by RP HPLC using a
C18 column with a gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1%
TFA to provide 15 mg of the product (43%) as a clear gel. .sup.1H
NMR (300 MHz, CDCl.sub.3) .delta. 0.02 (s, 9H), 1.18-1.25 (m, 2H),
1.24 (t, 6H, J=7 Hz), 1.86 (s, 3H), 1.88-2.02 (m, 2H), 2.16 (s,
3H), 2.65-2.74 (m, 2H), 3.93 (s, 2H), 3.46 (br d, 4H, J=7 Hz), 3.76
(s, 3H), 4.00 (pent, 4H, J=7 Hz), 4.25-4.34 (m, 2H), 5.11 (s, 2H),
5.34-5.43 (m, 1H), 7.18-7.33 (m, 5H) ppm; .sup.31P (121.4 MHz,
CDCl.sub.3) .delta. 30.9 ppm; MS (m/z) 632.4 [M+H].sup.+, 654.3
[M+Na].sup.+.
##STR00575##
(2-{Benzyl-[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofur-
an-5-yl)-2-methyl-but-2-enyl]-amino}-ethyl)-phosphonic acid
[1606] A solution of
(2-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphonic
acid diethyl ester (15 mg, 0.024 mmol) in acetonitrile (0.5 mL) was
treated with TMSBr (31 .mu.L, 0.24 mmol) and 2,6-lutidine (28
.mu.L, 0.24 mmol). The solution was stirred at ambient temperature
for 1 hour, when it was quenched with methanol. The solvent was
removed under reduced pressure and the residue was purified by RP
HPLC using a C18 column with a gradient of H.sub.2O, 0.1%
TFA-acetonitrile, 0.1% TFA to provide 11 mg of the product (93%) as
a white solid. .sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.89 (s,
3H), 2.03-2.15 (m, 2H), 2.14 (s, 3H), 3.30-3.47 (m, 2H), 3.50 (br
s, 2H), 3.62 (br s, 2H), 3.79 (s, 3H), 4.28 (s, 2H), 5.23 (s, 2H),
5.76 (br s, 1H), 7.46 (br s, 5H) ppm; .sup.31P (121.4 MHz,
CDCl.sub.3) .delta. 20.1 ppm; MS (m/z) 476.3 [M+H].sup.+, 498.3
[M+Na].sup.+.
Example 307
[1607] Representative compounds of the invention can be prepared as
illustrated below.
##STR00576##
[2-(Formyl-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-
-dihydro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-amino)-ethyl]-phosphonic
acid diethyl ester
[1608] To a solution of
(2-{4-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphonic
acid diethyl ester (74 mg, 0.14 mmol) in formic acid (1 mL) was
added formic anhydride (1 mL) and the solution was stirred at room
temperature for 1 hour. The reaction mixture was concentrated and
the crude product carried onto the next step. The NMR data of this
compound shows two rotamers with the ratio of 70:30. .sup.1H NMR
(300 MHz, CDCl.sub.3) .delta. 0.05 (s, 9H), 1.18-1.28 (m, 2H), 1.28
and 1.30 (t, 6H, J=7 Hz), 1.74 (s, 3H), 1.84-2.08 (m, 2H), 2.19 (s,
3H), 3.34-3.45 (m, 2H), 3.47 (d, 2H, J=7 Hz), 3.72 and 3.87 (s,
2H), 3.78 and 3.79 (s, 3H), 4.06 and 4.07 (pent, 4H, J=7 Hz),
4.26-4.37 (m, 2H), 5.13 (s, 2H), 5.30-5.46 (m, 1H), 8.03 and 8.19
(s, 1H) ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta. 27.5 and 28.1
ppm; MS (m/z) 570.1 [M+H].sup.+, 592.2 [M+Na].sup.+.
##STR00577##
(2-{Formyl-[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofur-
an-5-yl)-2-methyl-but-2-enyl]-amino}-ethyl)-phosphonic acid
[1609] To a solution of crude
[2-(formyl-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-
-dihydro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-amino)-ethyl]-phosphonic
acid diethyl ester (78 mg, 0.14 mmol) in acetonitrile (1 mL) was
added TMSBr (177 .mu.L, 1.4 mmol) and 2,6-lutidine (163 .mu.L, 1.4
mmol). The solution was stirred at room temperature for 1 hour when
it was quenched by addition of methanol and 1N aqueous HCl. The
product was extracted with EtOAc and purified by RP HPLC using a
C18 column with a gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1%
TFA to provide 29 mg of the product as a white solid. The NMR data
of this compound shows two rotamers with the ratio of approximately
70:30. .sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.62 and 1.64 (s,
3H), 1.83-1.98 (m, 2H), 2.16 (s, 3H), 3.38-3.55 (m, 4H), 3.78 (s,
3H), 3.80 and 3.91 (s, 2H), 5.22 (s, 2H), 5.39-5.52 (m, 1H), 8.03
and 8.18 (s, 1H) ppm; MS (m/z) 414.2 [M+H].sup.+, 436.2
[M+Na].sup.+.
Example 308
[1610] Representative compounds of the invention can be prepared as
illustrated below.
##STR00578##
({4-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-i-
sobenzofuran-5-yl]-2-methyl-but-2-enylamino}-methyl)-phosphonic
acid diethyl ester
[1611] To a solution of
4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-2-methyl-but-2-enal (500 mg, 1.33 mmol),
(2-aminomethyl)phosphonic acid diethyl ester oxalate (376 mg, 1.46
mmol), sodium triacetoxyborohydride (563 mg, 2.66 mmol) in DMF (10
mL) was added acetic acid (380 .mu.L, 6.65 mmol) at room
temperature. The solution was stirred overnight when it was
quenched by addition of saturated aqueous sodium bicarbonate
solution and EtOAc. The organic layer was separated and
concentrated under reduced pressure. The residue was purified by
silica gel chromatography to provide 500 mg (71%) of the product as
an oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.00 (s, 9H),
1.13-1.23 (m, 2H), 1.25 and 1.27 (t, 6H, J=7 Hz), 1.65-1.75 (m,
2H), 1.77 (s, 3H), 2.13 (s, 3H), 2.80 (s, 1H), 3.14 (s, 2H), 3.41
(d, 2H, J=7 Hz), 3.73 (s, 3H), 4.08 and 4.09 (pent, 4H, J=7 Hz),
4.20-4.30 (m, 2H), 5.08 (s, 2H), 5.30 (t, 1H, J=7 Hz) ppm; .sup.31P
(121.4 MHz, CDCl.sub.3) .delta. 26.5 ppm; MS (m/z) 528.1
[M+H].sup.+, 550.2 [M+Na].sup.+.
##STR00579##
{[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2-
-methyl-but-2-enylamino]-methyl}-phosphonic acid
[1612] To a solution of
({4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-i-
sobenzofuran-5-yl]-2-methyl-but-2-enylamino}-methyl)-phosphonic
acid diethyl ester (20 mg, 0.038 mmol) in DMF (0.5 mL) was added
TMSBr (49 .mu.L, 0.38 mmol) and 2,6-lutidine (44 .mu.L, 0.38 mmol).
The solution was stirred at room temperature for 1 hour when it was
quenched by addition of methanol. The product was purified by RP
HPLC using a C18 column with a gradient of H.sub.2O, 0.1%
TFA-acetonitrile, 0.1% TFA to provide 5.6 mg of the product as a
white solid. .sup.1H NMR (300 MHz, CD.sub.3OD and CDCl.sub.3)
.delta. 1.93 (s, 3H), 2.13 (s, 3H), 2.94 (br d, 2H, J=11 Hz),
3.42-3.53 (m, 2H), 3.60 (s, 2H), 3.78 (s, 3H), 5.22 (s, 2H), 5.71
(br s, 1H) ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta. 8.5 ppm;
MS (m/z) 372.2 [M+H].sup.+, 743.2 [2M+H].sup.+.
Example 309
[1613] Representative compounds of the invention can be prepared as
illustrated below.
##STR00580##
2-({2-[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5--
yl)-2-methyl-but-2-enylamino]-ethyl}-phenoxy-phosphinoyloxy)-propionic
acid ethyl ester
[1614] A solution of
4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-2-methyl-but-2-enal (188 mg, 0.5 mmol) was stirred
with 2-[(2-aminoethyl)phenoxy-phosphinoyloxy]-propionic acid ethyl
ester acetic acid salt (315.8 mg, 0.75 mmol) in CH.sub.2Cl.sub.2 (3
mL) for 2 hours at ambient temperature. Sodium
triacetoxyborohydride (159 mg, 0.75 mmol) was added to the solution
and the reaction was allowed to proceed for 1 hour. The reaction
was quenched by addition of a saturated aqueous solution of
NaHCO.sub.3 and the product was extracted with EtOAc. The organic
layer was removed under reduced pressure and the residue was
resuspended in a 10% TFA/CH.sub.2Cl.sub.2 for 1 hour. The reaction
mixture was concentrated and the product was purified by RP HPLC
using a C18 column with a gradient of H.sub.2O, 0.1%
TFA-acetonitrile, 0.1% TFA to provide 198 mg of the product as a
white solid. The NMR data of this compound shows two diastereomers
at phosphorus in a ratio of approximately 45:55. .sup.1H NMR (300
MHz, CD.sub.3OD) .delta. 1.23 and 1.24 (t, 3H, J=7 Hz), 1.38 and
1.52 (d, 3H, J=7 Hz), 1.97 and 1.98 (s, 3H), 2.14 (s, 3H),
2.44-2.66 (m, 2H), 3.31-3.48 (m, 2H), 3.51 (d, 2H, J=7 Hz), 3.66
(d, 2H, J=5 Hz), 3.80 (s, 3H), 4.10-4.27 (m, 2H), 4.90-5.10 (m,
1H), 5.20 (s, 2H), 5.73-5.82 (m, 1H), 7:15-7.27 (m, 3H), 7.35-7.45
(m, 2H) ppm; .sup.31P (121.4 MHz, CD.sub.3OD) .delta. 22.6, 24.3
ppm; MS (m/z) 561.9 [M+H].sup.+.
Example 310
[1615] Representative compounds of the invention can be prepared as
illustrated below.
##STR00581##
2-[Hydroxy-(2-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)--
1,3-dihydro-isobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphino-
yloxy]-propionic acid ethyl ester
[1616] A solution of
4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-2-methyl-but-2-enal (38 mg, 0.1 mmol) was stirred
with 2-[(2-aminoethyl)-phenoxy-phosphinoyloxy]-propionic acid ethyl
ester acetic acid (63 mg, 0.15 mmol) in CH.sub.2Cl.sub.2 (1 mL) for
2 hours at ambient temperature. Sodium triacetoxyborohydride (32
mg, 0.15 mmol) was added to the solution and the reaction was
allowed to proceed for 1 hour. The reaction was quenched by
addition of a saturated aqueous solution of NaHCO.sub.3 and the
product was extracted with EtOAc. The organic layer was removed
under reduced pressure and the residue was re-suspended in 10%
TFA/CH.sub.2Cl.sub.2 for 1 hour. The reaction mixture was
concentrated and the product was purified by RP HPLC using a C18
column with a gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA
to provide 15 mg of the product (154-2). .sup.1H NMR (300 MHz,
CDCl.sub.3) .delta. 0.04 (s, 9H), 1.15-1.24 (m, 2H), 1.26 (t, 3H,
J=7 Hz), 1.48 (d, 3H, J=7 Hz), 1.93 (s, 3H), 2.10-2.25 (m, 2H),
2.18 (s, 3H), 3.10-3.31 (m, 2H), 3.48 (d, 2H, J=7 Hz), 3.48-3.61
(m, 2H), 3.77 (s, 3H), 4.04-4.21 (m, 2H), 4.29-4.40 (m, 2H),
4.81-4.92 (m, 1H), 5.13 (s, 2H), 5.64 (t, 1H, J=7 Hz), 8.70-9.11
(m, 3H) ppm; 31P (121.4 MHz, CDCl.sub.3) .delta. 21.9 ppm; MS (m/z)
586.3 [M+H].sup.+, 1171.4 [2M+H].sup.+.
##STR00582##
2-(Hydroxy-{2-[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzo-
furan-5-yl)-2-methyl-but-2-enylamino]-ethyl}-phosphinoyloxy)-propionic
acid
[1617] A solution of
2-[hydroxy-(2-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)--
1,3-dihydro-isobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphino-
yloxy]-propionic acid ethyl ester (15 mg, 0.026 mmol) in 10%
TFA-CH.sub.2Cl.sub.2 (1 mL) was stirred at ambient temperature for
10 minutes. The reaction was worked up by removal of the solvent.
The residue was dissolved in THF (0.5 mL) and water (0.4 mL) and 1N
aqueous NaOH solution (0.1 mL) was added. The solution was stirred
at room temperature for 20 minutes when it was acidified with 1N
aqueous HCl solution. The resulting solution was purified by RP
HPLC using a C18 column with a gradient of H.sub.2O, 0.1%
TFA-acetonitrile, 0.1% TFA to provide 6.8 mg of the product as a
white solid. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 1.38 (d, 3H,
J=7 Hz), 1.91 (s, 3H), 2.13 (s, 3H), 2.12-2.28 (m, 2H), 3.12-3.33
(m, 2H), 3.41 (d, 2H, J=6 Hz), 3.56 (br s, 2H), 3.75 (s, 3H),
4.71-4.88 (m, 1H), 5.16 (s, 2H), 5.58-5.71 (m, 1H), 7.88 (br s,
3H), 8.60 (br s, 1H), 8.78 (br s, 1H) ppm; .sup.31P (121.4 MHz,
CDCl.sub.3) .delta. 22.0 ppm; MS (m/z) 458.3 [M+H].sup.+, 480.3
[M+Na].sup.+.
##STR00583##
Example 311
[1618] Representative compounds of the invention can be prepared as
illustrated below.
##STR00584##
{1-Cyano-5-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-di-
hydro-isobenzofuran-5-yl]-3-methyl-pent-3-enyl}-phosphonic acid
diethyl ester
[1619] To a solution of diethyl cyanomethylphosphonate (241 mg,
1.38 mmol) in THF (1 mL) was added a THF solution of sodium
bis(trimethysilyl)amide (1.0 M, 1.13 mL, 1.15 mmol). After stirring
for 30 minutes, the solution was added dropwise to a solution of
6-(4-bromo-3-methyl-but-2-enyl)-7-hydroxy-5-methoxy-4-methyl-3H-isobenzof-
uran-1-one (100 mg, 0.23 mmol) in THF (1 mL). The resulting mixture
was allowed to stir at room temperature for one hour before
saturated aqueous ammonium chloride was added. The reaction mixture
was extracted with ethyl acetate. The organic layer was dried over
sodium sulfate and concentrated to dryness. The residue was
purified by silica gel column chromatography, affording 110 mg
(90%) of the desired product. .sup.1H NMR (300 MHz, CDCl.sub.3)
.delta. 0.04 (s, 9H), 1.24 (dd, J=7, 8 Hz, 2H), 1.36 (t, 6H), 1.86
(s, 3H), 2.17 (s, 3H), 2.43-2.57 (m, 2H), 3.04-3.17 (m, 1H), 3.47
(d, J=7.2 Hz, 2H), 3.79 (s, 3H), 4.12-4.37 (m, 6H), 5.13 (s, 2H),
5.44 (t, J=7.2 Hz, 1H) ppm; .sup.31P (121.4 MHz, CDCl.sub.3)
.delta. 18.18 ppm; MS (m/z) 560 [M+Na].sup.+.
##STR00585##
[1-Cyano-5-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran--
5-yl)-3-methyl-pent-3-enyl]-phosphonic acid diethyl ester
[1620]
{1-Cyano-5-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)--
1,3-dihydro-isobenzofuran-5-yl]-3-methyl-pent-3-enyl}-phosphonic
acid diethyl ester (25 mg, 0.047 mmol) was dissolved in a solution
of 10% TFA/CH.sub.2Cl.sub.2 (5 mL) and stirred at room temperature
for 2 hours. The reaction mixture was dried under reduced pressure
and the product was purified by RP-HPLC to provide 16 mg (80%) of
the desired product as a white solid. .sup.1H NMR (300 MHz,
CDCl.sub.3) .delta. 1.38 (t, 6H), 1.86 (s, 3H), 2.15 (s, 3H),
2.40-2.58 (m, 2H), 3.01-3.14 (m, 1H), 3.45 (d, J=7.2 Hz, 2H), 3.79
(s, 3H), 4.18-4.30 (m, 4H), 5.21 (s, 2H), 5.48 (t, J=7.2 Hz, 1H)
ppm; 31P (121.4 MHz, CDCl.sub.3) .delta. 18.09 ppm; MS (m/z) 436
[M-H]-, 438 [M+H]+.
Example 312
[1621] Representative compounds of the invention can be prepared as
illustrated below.
##STR00586##
[1-Cyano-5-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran--
5-yl)-3-methyl-pent-3-enyl]-phosphonic acid
[1622] To a solution of
{1-cyano-5-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-di-
hydro-isobenzofuran-5-yl]-3-methyl-pent-3-enyl}-phosphonic acid
diethyl ester (35 mg, 0.065 mmol) in acetonitrile (2 mL) was added
TMSBr (180 .mu.L, 1.38 mmol) and 2,6-lutidine (160 .mu.L, 1.38
mmol). The reaction solution was allowed stir at room temperature
for one hour before quenching with MeOH. The reaction mixture was
dried under reduced pressure and the residue was purified by RP
HPLC using a C18 column with a gradient of H.sub.2O, 0.1%
TFA-acetonitrile, 0.1% TFA to provide 15 mg (60%) of the desired
product. .sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.86 (s, 3H),
2.15 (s, 3H), 2.38-2.57 (m, 2H), 3.17-3.28 (m, 1H), 3.44 (d, J=7.2
Hz, 2H), 3.80 (s, 3H), 5.25 (s, 2H), 5.47 (t, J=7.2 Hz, 1H) ppm;
.sup.31P (121.4 MHz, CD.sub.3OD) .delta. 15.28 ppm; MS (m/z) 380
[M-H].sup.-, 382 [M+H].sup.+.
Example 313
[1623] Representative compounds of the invention can be prepared as
illustrated below.
##STR00587##
{1-Cyano-5-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-di-
hydro-isobenzofuran-5-yl]-1,3-dimethyl-pent-3-enyl}-phosphonic acid
diethyl ester
[1624] To a solution of
{1-cyano-5-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-di-
hydro-isobenzofuran-5-yl]-3-methyl-pent-3-enyl}-phosphonic acid
diethyl ester (45 mg, 0.084 mmol) in THF (0.5 mL) was added sodium
bis(trimethysilyl)amide (1.0 M, 1.13 mL, 1.15 mmol). After stirring
for 20 minutes, iodomethane (52 .mu.L, 0.84 mmol) was added
dropwise and the resulting mixture was allowed to stir at room
temperature for 2 hours. The reaction mixture was quenched with
saturated aqueous ammonium chloride and extracted with ethyl
acetate. The organic layer was dried over sodium sulfate and
concentrated to dryness. The residue was purified by RP HPLC using
a C18 column with a gradient of H.sub.2O, 0.1% TFA-acetonitrile,
0.1% TFA to afford 6.6 mg (23%) of the desired product. .sup.1H NMR
(300 MHz, CDCl.sub.3) .delta. 0.00 (s, 9H), 1.16 (dd, J=7, 8 Hz,
2H), 1.31 (t, 6H), 1.38 (d, 3H), 1.92 (s, 3H), 2.17 (s, 3H), 2.23
(m, 1H), 2.65 (m, 1H), 3.30-3.42 (m, 2H), 3.73 (s, 3H), 4.14-4.27
(m, 6H), 5.08 (s, 2H), 5.28 (t, J=7.2 Hz, 1H) ppm; .sup.31P (121.4
MHz, CDCl.sub.3) .delta. 22.26 ppm; MS (m/z) 574 [M+Na].sup.+.
##STR00588##
[1-Cyano-5-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran--
5-yl)-1,3-dimethyl-pent-3-enyl]-phosphonic acid
[1625] To a solution of
{1-cyano-5-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-di-
hydro-isobenzofuran-5-yl]-1,3-dimethyl-pent-3-enyl}-phosphonic acid
diethyl ester (18 mg, 0.04 mmol) in DMF (0.5 mL) and DCM (0.5 mL)
was added TMSBr (51 .mu.L, 0.4 mmol) and 2,6-lutidine (46 .mu.L,
0.4 mmol). The reaction solution was allowed stir at room
temperature overnight before quenching with MeOH. The reaction
mixture was dried under reduced pressure and the residue was
purified by RP HPLC using a C18 column with a gradient of H.sub.2O,
0.1% TFA-acetonitrile, 0.1% TFA to provide 4.5 mg (33%) of the
desired product. .sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.37 (d,
3H), 1.87 (s, 3H), 2.13 (s, 3H), 2.26 (m, 1H), 2.64 (m, 1H), 3.39
(m, 2H), 3.75 (s, 3H), 5.18 (s, 2H), 5.34 (m, 1H) ppm; .sup.31P
(121.4 MHz, CD.sub.3OD) .delta. 21.47 ppm; MS (m/z) 422
[M-H].sup.-, 424 [M+H].sup.+.
##STR00589##
Example 314
[1626] Representative compounds of the invention can be prepared as
illustrated below.
##STR00590##
2-Ethyl-4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dih-
ydro-isobenzofuran-5-yl]-but-2-enal
[1627] A solution of
[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobe-
nzofuran-5-yl]-acetaldehyde (1.5 g, 4.46 mmol) in toluene (14 mL)
was heated at 100.degree. C. with
2-(triphenyl-phosphanylidene)-butyraldehyde (1.68 g, 5.35 mmol)
overnight. A second portion of
2-(triphenyl-phosphanylidene)-butyraldehyde (495 mg, 1.49 mmol) was
added and the reaction mixture was heated for an additional day.
After concentration, the residue was purified by silica gel
chromatography to provide 1.3 g (83%) of the desired product as
oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.01 (s, 9H), 1.03
(t, 3H), 1.10-1.21 (m, 2H), 2.15 (s, 3H), 2.15-2.44 (m, 2H),
3.67-3.76 (m, 2H), 3.74 (s, 3H), 4.31-4.36 (m, 2H), 5.10 (s, 2H),
6.34-6.38 (m, 1H), 9.28 (s, 1H) ppm.
##STR00591##
6-(3-Hydroxymethyl-pent-2-enyl)-5-methoxy-4-methyl-7-(2-trimethylsilanyl--
ethoxy)-3H-isobenzofuran-1-one
[1628] A solution of
2-ethyl-4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dih-
ydro-isobenzofuran-5-yl]-but-2-enal (1.3 g, 3.30 mmol) in methanol
(10 mL) and THF (10 mL) was cooled to 0.degree. C. A solution of
CeCl.sub.3 (8.25 mL, 0.4M, MeOH: H.sub.2O, 9:1) was added, followed
by LiBH.sub.4 (1.66 mL, 3.30 mmol of a 2M solution in THF). The ice
bath was removed and the reaction mixture was allowed to warm to
room temperature. The reaction mixture was stirred for an
additional 40 minutes, whereupon TLC indicated complete consumption
of starting aldehyde. The reaction was worked up by addition of
aqueous 1N HCl and the product was extracted with EtOAc. The
organic layer was washed with saturated aqueous sodium bicarbonate
solution and brine. The organic layer was concentrated under
reduced pressure and the residue was purified by silica gel
chromatography to provide 948 mg (73%) of the product as colorless
oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.00 (s, 9H), 1.07
(t, 3H), 1.20 (dd, 2H, J=7, 8 Hz), 2.13 (s, 3H), 2.38-2.50 (m, 2H),
3.77 (s, 3H), 3.99 (s, 2H), 4.27 (dd, 2H, J=0.7, 8 Hz), 5.08 (s,
2H), 5.34 (t, J=7.2 Hz, 1H) ppm.
##STR00592##
6-(3-Bromomethyl-pent-2-enyl)-5-methoxy-4-methyl-7-(2-trimethylsilanyl-et-
hoxy)-3H-isobenzofuran-1-one
[1629] Polymer-supported triphenylphosphine (3 mmol/g, 0.66 g) was
soaked in dichloromethane (6 mL) for 1 hour
6-(3-Hydroxymethyl-pent-2-enyl)-5-methoxy-4-methyl-7-(2-trimethylsilanyl--
ethoxy)-3H-isobenzofuran-1-one (260 mg, 0.66 mmol) and carbon
tetrabromide (657 mg, 1.98 mmol) were added sequentially and the
mixture was shaken for 1 hour at room temperature. The mixture was
filtered and the filtrate was concentrated. The residue was
purified by silica gel chromatography to provide 233 mg (77%) of
the product as a white solid. .sup.1H NMR (300 MHz, CDCl.sub.3)
.delta. 0.00 (s, 9H), 1.08 (t, 3H), 1.20 (dd, 2H, J=7, 8 Hz), 2.14
(s, 3H), 2.35-2.43 (m, 2H), 3.44 (d, J=7.2, 2H), 3.73 (s, 3H), 3.95
(s, 2H), 4.27 (dd, 2H, J=7, 8 Hz), 5.08 (s, 2H), 5.53 (t, J=7.2 Hz,
1H) ppm.
##STR00593##
[2-Ethyl-4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran--
5-yl)-but-2-enyl]-phosphonic acid
[1630] A solution of
6-(3-bromomethyl-pent-2-enyl)-5-methoxy-4-methyl-7-(2-trimethylsilanyl-et-
hoxy)-3H-isobenzofuran-1-one (230 mg, 0.5 mmol) in
trimethylphosphite (1.5 mL, 12.75 mmol) was heated to 100.degree.
C. for 4 hours. The reaction was worked up by removal of excess
trimethylphosphite under reduced pressure. The residue was
dissolved in acetonitrile (1 mL) and TMSBr (646 .mu.L, 5.0 mmol)
and 2,6-lutidine (580 .mu.L, 5.0 mmol) were added at 0.degree. C.
The reaction solution was allowed to warm to room temperature and
stirred for 4 hours. The reaction was cooled to 0.degree. C. and
quenched with addition of MeOH. The reaction mixture was dried
under reduced pressure and the residue was purified by RP HPLC
using a C18 column with a gradient of H.sub.2O, 0.1%
TFA-acetonitrile, 0.1% TFA to provide 77 mg (58%) of the product.
.sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.08 (t, 3H), 2.16 (s,
3H), 2.43 (m, 2H), 2.48 (d, 2H, J=22 Hz), 3.46 (t, 2H, J=6 Hz),
3.79 (s, 3H), 5.25 (s, 2H), 5.38 (q, 1H, J=7 Hz) ppm.; .sup.31P
(121.4 MHz, CD.sub.3OD) .delta. 25.65 ppm.; MS (m/z) 355
[M-H].sup.-, 357 [M+H].sup.+.
Example 315
[1631] Representative compounds of the invention can be prepared as
illustrated below.
##STR00594##
{1-Cyano-3-ethyl-5-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy-
)-1,3-dihydro-isobenzofuran-5-yl]-pent-3-enyl}-phosphonic acid
diethyl ester
[1632] To a solution of diethyl cyanomethylphosphonate (233 mg,
1.32 mmol) in THF (1 mL) was added a THF solution of sodium
bis(trimethysilyl)amide (1.0 M, 1.21 mL, 1.21 mmol). After stirring
for 30 minutes, the solution was added dropwise to a solution of
6-(3-bromomethyl-pent-2-enyl)-5-methoxy-4-methyl-7-(2-trimethylsilanyl-et-
hoxy)-3H-isobenzofuran-1-one (100 mg, 0.22 mmol) in THF (1 mL). The
resulting mixture was allowed to stir at room temperature overnight
before saturated aqueous ammonium chloride was added. The reaction
mixture was extracted with ethyl acetate. The organic layer was
dried over sodium sulfate and concentrated to dryness. The residue
was purified by preparative reverse-phase HPLC, affording 51 mg
(42%) of the desired product. .sup.1H NMR (300 MHz, CDCl.sub.3)
.delta. 0.04 (s, 9H), 1.07 (t, 3H), 1.24 (dd, 2H, J=7, 8 Hz), 1.36
(t, 6H), 2.12 (m, 1H), 2.18 (s, 3H), 2.35-2.47 (m, 2H), 2.67 (m,
1H), 3.00-3.14 (m, 1H), 3.44 (d, J=7.2, 2H), 3.79 (s, 3H),
4.12-4.37 (m, 6H), 5.13 (s, 2H), 5.38 (t, J=7.2 Hz, 1H) ppm;
.sup.31P (121.4 MHz, CDCl.sub.3) .delta. 18.26 ppm; MS (m/z) 574
[M+Na].sup.+.
##STR00595##
[1-Cyano-3-ethyl-5-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isoben-
zofuran-5-yl)-pent-3-enyl]-phosphonic acid
[1633]
{1-Cyano-3-ethyl-5-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl--
ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-pent-3-enyl}-phosphonic
acid diethyl ester (19.5 mg, 0.035 mmol) was dissolved in a
solution of 10% TFA/CH.sub.2Cl.sub.2 (2 mL) and stirred at room
temperature for 10 minutes. The reaction mixture was dried under
reduced pressure and purified by RP-HPLC to provide 9.5 mg (61%) of
the desired product. This material was dissolved in DMF (0.5 mL)
and DCM (0.5 mL) and TMSBr (27 .mu.L, 0.2 mmol) and 2,6-lutidine
(23 .mu.L, 0.2 mmol) were added. The reaction solution was allowed
stir at room temperature overnight before quenching with MeOH. The
reaction mixture was dried under reduced pressure and the residue
was purified by RP HPLC using a C18 column with a gradient of
H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA to provide 5.1 mg (65%)
of the desired product as a white solid. .sup.1H NMR (300 MHz,
CD.sub.3OD) .delta. 1.10 (t, 3H), 2.16 (s, 3H), 2.23-2.52 (m, 3H),
2.67 (m, 1H), 3.05-3.20 (m, 1H), 3.48 (d, J=7.2, 2H), 3.81 (s, 3H),
5.26 (s, 2H), 5.43 (t, J=7.2 Hz, 1H) ppm; .sup.31P (121.4 MHz,
CD.sub.3OD) .delta. 14.18 ppm; MS (m/z) 394 [M-H].sup.-, 396
[M+H].sup.+.
Example 316
[1634] Representative compounds of the invention can be prepared as
illustrated below.
##STR00596##
{2-Ethyl-4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-di-
hydro-isobenzofuran-5-yl]-but-2-enyloxymethyl}-phosphonic acid
diisopropyl ester
[1635] To a solution of bromomethylphosphonate diisopropyl ester
(680 mg, 2.62 mmol) and
6-(3-hydroxymethyl-pent-2-enyl)-5-methoxy-4-methyl-7-(2-trimethylsilanyl--
ethoxy)-3H-isobenzofuran-1-one (688 mg, 1.75 mmol) in DMF (3 mL)
was added lithium t-butoxide (1.0M in THF; 2.6 mL). The reaction
was heated at 70.degree. C. for 2 hours. After cooling to ambient
temperature, more bromomethylphosphonate diisopropyl ester (680 mg,
2.62 mmol) and lithium t-butoxide (1.0M in THF; 2.6 mL) were added.
The reaction mixture was heated at 70.degree. C. for a further
hour, cooled, poured into a solution of lithium chloride (5%
aqueous) and extracted with ethyl acetate. The organic extract was
dried and the product was purified by chromatography on silica gel,
eluting with hexane-ethyl acetate to provide 347 mg (35%) of the
product as a colorless oil. .sup.1H NMR (300 MHz, CDCl.sub.3)
.delta. 0.04 (s, 9H), 1.09 (t, 3H, J=7.5 Hz), 1.20-1.26 (m, 2H),
1.31 (t, 12H, J=6 Hz), 2.18 (s, 3H), 2.29 (q, 2H, J=7.5 Hz), 3.5
(m, 2H), 3.59 (d, 2H, J=8.7 Hz), 3.78 (s, 3H), 3.98 (s, 2H),
4.28-4.35 (m, 2H), 4.6-4.8 (m, 2H), 5.13 (s, 2H), 5.4 (t, 1H, J=7
Hz) ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta. 20.26 ppm; MS
(m/z) 593.3 [M+Na].sup.+.
##STR00597##
[2-Ethyl-4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran--
5-yl)-but-2-enyloxymethyl]-phosphonic acid
[1636] To a solution of
{2-ethyl-4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-di-
hydro-isobenzofuran-5-yl]-but-2-enyloxymethyl}-phosphonic acid
diisopropyl ester (347 mg, 0.61 mmol) in acetonitrile (5 mL) was
added 2,6-lutidine (0.71 mL, 6.1 mmol) and bromotrimethylsilane
(0.786 mL, 6.1 mmol). The mixture was stirred at room temperature
for 3 hours, quenched with methanol (5 mL), concentrated, and
partitioned between ethyl acetate and 1N HCl (aqueous). The organic
layer was concentrated to give the free phosphonic acid as a
colorless oil (205 mg, 70%). This material (20 mg) was dissolved in
a solution of trifluoroacetic acid (0.3 mL) and dichloromethane
(2.7 mL) and stirred for 30 minutes at ambient temperature. After
concentration, the residue was purified by RP HPLC using a C18
column with a gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA
to provide the product, after lyophilization, as a white solid (10
mg). .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 1.007 (t, 3H, J=7.5
Hz), 2.13 (s, 3H), 2.32 (q, 2H, J=7.5 Hz), 3.41 (d, 2H, J=6.3 Hz),
3.56 (d, 2H, J=9 Hz), 3.75 (s, 3H), 3.95 (s, 2H), 5.16 (s, 2H),
5.43 (t, 1H, J=6.3 Hz) ppm; .sup.31P (121.4 MHz, CDCl.sub.3)
.delta. 22.8 ppm; MS (m/z) 385.2 [M-H].sup.+, 387.1
[M+H].sup.+.
Example 317
[1637] Representative compounds of the invention can be prepared as
illustrated below.
##STR00598## ##STR00599## ##STR00600##
6-Allyloxy-3-methyl-4-trifluoromethanesulfonyloxy-phthalic acid
dimethyl ester
[1638] To a solution of 6-allyloxy-4-hydroxy-3-methyl-phthalic acid
dimethyl ester (8.06 g, 28.8 mmol) [synthesized according to: J. W.
Patterson, Tetrahedron, 1993, 49, 4789-4798] and pyridine (11.4 g,
144.0 mmol) in dichloromethane (DCM) (20 mL) at 0.degree. C. was
added triflic anhydride (12.19 g, 43.2 mmol). The reaction was
stirred at 0.degree. C. for 2 hours after which additional triflic
anhydride (3 mL) was added. Stirring at 0.degree. C. was continued
for an additional hour. The reaction mixture was poured into a
mixture of DCM and HCl (1N). The layers were separated and the
aqueous layer was extracted with DCM. The combined organic layers
were dried over sodium sulfate. Filtration and evaporation of
solvents in vacuo yielded a crude product, which was purified by
silica gel chromatography to provide 8.39 g of the product as an
oil. .sup.1H NMR (300 MHz, CDCl.sub.3): .delta.=2.32 (s, 3H), 3.89
(s, 6H), 4.60 (m, 2H), 5.33 (d, J=9.3 Hz, 1H), 5.41 (d, J=18.6 Hz,
1H), 5.95 (m, 1H), 6.95 (s, 1H) ppm; .sup.19F NMR (282 MHz,
CDCl.sub.3): .delta.=-74 ppm.
##STR00601##
6-Hydroxy-3-methyl-4-trifluoromethanesulfonyloxy-phthalic acid
dimethyl ester
[1639] To a solution of
6-allyloxy-3-methyl-4-trifluoromethanesulfonyloxy-phthalic acid
dimethyl ester (8.39 g, 20.3 mmol) in toluene (20 mL) was added
tetrakistriphenylphosphine palladium (0.47 g, 0.40 mmol) and
diethylamine (2.97 g, 40.86 mmol) at room temperature under an
atmosphere of nitrogen. Stirring at room temperature was continued
until all starting material was consumed. The crude reaction
mixture was partitioned between diethyl ether and HCl (0.1 N). The
organic layer was washed with brine and dried over sodium sulfate.
Filtration and evaporation of solvents in vacuo yielded a crude
material, which was purified by silica gel chromatography to
provide 4.16 g (55%) of the desired product as an off-white solid.
.sup.1H NMR (300 MHz, CDCl.sub.3): .delta.=2.20 (s, 3H), 3.93 (s,
3H), 3.95 (s, 3H), 7.01 (s, 1H) ppm; .sup.19F NMR (282 MHz,
CDCl.sub.3): .delta.=-74 ppm.
##STR00602##
6-Hydroxy-3-methyl-4-vinyl-phthalic acid dimethyl ester
[1640] To a solution of
6-hydroxy-3-methyl-4-trifluoromethanesulfonyloxy-phthalic acid
dimethyl ester (2.17 g, 5.85 mmol) in N-methylpyrrolidinone (15 mL)
was added lithium chloride (743 mg, 17.5 mmol) and triphenylarsine
(179 mg, 0.585 mmol). Tributylvinyltin (2.04 g, 6.43 mmol) was
added followed by
tris(tribenzylideneacetone)dipalladium(0)-chloroform adduct (90 mg,
0.087 mmol). The reaction was placed under an atmosphere of
nitrogen and heated at 60.degree. C. for 18 hours. The reaction was
cooled to room temperature and poured onto a mixture of ice (20 g),
EtOAc (40 mL), and potassium fluoride (1 g). Stirring was continued
for 1 hour. The aqueous layer was extracted with EtOAc and the
organic extracts filtered through Celite. The combined organic
layers were washed with water and dried over sodium sulfate.
Filtration and evaporation of solvents in vacuo yielded a crude
material, which was purified by silica gel chromatography to
provide 1.27 g (87%) of the product as an off-white solid. .sup.1H
NMR (300 MHz, CDCl.sub.3): .delta.=2.16 (s, 3H), 3.91 (s, 3H), 3.92
(s, 3H), 5.46 (dd, J=11.1, 1.2 Hz, 1H), 5.72 (dd, J=17.1, 0.9 Hz,
1H), 6.86 (dd, J=17.1, 11.1 Hz, 1H), 7.14 (s, 1H), 10.79 (s, 1H)
ppm.
##STR00603##
4-Ethyl-6-hydroxy-3-methyl-phthalic acid dimethyl ester
[1641] 6-Hydroxy-3-methyl-4-vinyl-phthalic acid dimethyl ester
(1.27 g, 5.11 mmol) was dissolved in benzene (10 mL) and EtOAc (10
mL). Tristriphenylphosphine rhodium chloride (150 mg) was added and
the reaction was placed under an atmosphere of hydrogen. Stirring
at room temperature was continued. After 14 hours, the solvents
were removed in vacuo and the crude material was purified by silica
gel chromatography to provide 1.14 g (88%) of the desired product
as an off-white solid. .sup.1H NMR (300 MHz, CDCl.sub.3):
.delta.=1.19 (t, J=7.8 Hz, 3H), 2.10 (s, 3H), 2.60 (q, J=7.8 Hz,
2H), 3.89 (s, 6H), 6.87 (s, 1H), 10.79 (s, 1H) ppm.
##STR00604##
1 6-Allyloxy-4-ethyl-3-methyl-phthalic acid dimethyl ester
[1642] 4-Ethyl-6-hydroxy-3-methyl-phthalic acid dimethyl ester
(1.01 g, 4.02 mmol) was dissolved in DMF (5 mL). Potassium
carbonate (3.33 g, 24.14 mmol) was added, followed by allylbromide
(2.92 g, 24.14 mmol). The suspension was heated at 60.degree. C.
After 14 hours, the reaction was cooled to room temperature and
filtered. The solvents were removed in vacuo and the crude material
was purified by silica gel chromatography to provide 0.976 g (83%)
of the desired product as a colorless oil. .sup.1H NMR (300 MHz,
CDCl.sub.3): .delta.=1.16 (t, J=7.2 Hz, 3H), 2.20 (s, 3H), 2.62 (q,
J=7.2 Hz, 2H), 3.83 (s, 3H), 3.84 (s, 3H), 4.57 (m, 2H), 5.26 (dd,
J=9.3, 1.5 Hz, 1H), 5.41 (dd, J=13.5, 1.5 Hz, 1H), 5.98 (m, 1H),
6.82 (s, 1H) ppm.
##STR00605##
4-Allyl-5-ethyl-3-hydroxy-6-methyl-phthalic acid dimethyl ester
[1643] 6-Allyloxy-4-ethyl-3-methyl-phthalic acid dimethyl ester
(1.25 g, 4.28 mmol) was heated at 21.degree. C. under an atmosphere
of nitrogen. After 14 hours, the reaction was cooled to room
temperature. The crude material was purified by silica gel
chromatography to provide 0.971 g (77%) of the desired product as a
colorless oil. .sup.1H NMR (300 MHz, CDCl.sub.3): .delta.=1.14 (t,
J=7.8 Hz, 3H), 2.17 (s, 3H), 2.68 (q, J=7.8 Hz, 2H), 3.49 (m, 2H),
3.86 (s, 3H), 3.89 (s, 3H), 4.89-5.01 (m, 2H), 5.93 (m, 1H), 11.22
(s, 1H) ppm.
##STR00606##
5 6-Allyl-5-ethyl-7-hydroxy-4-methyl-3H-isobenzofuran-1-one
[1644] 4-Allyl-5-ethyl-3-hydroxy-6-methyl-phthalic acid dimethyl
ester (0.971 g, 3.32 mmol) was dissolved in MeOH (8 mL) at room
temperature. A solution of sodium hydroxide (0.798 g, 19.95 mmol)
in water (10 mL) was added and the suspension was heated at
55.degree. C. After 16 hours, the reaction was cooled to room
temperature and washed with diethyl ether. The aqueous layer was
acidified (1N HCl) and the suspension was extracted with EtOAc. The
combined organic layers were dried over sodium sulfate. Filtration
and evaporation of solvents in vacuo yielded the desired bis acid
as a white solid (0.846 g, 98%, M.sup.+=263). The bis acid was
dissolved in acetic acid (6 mL) and HCl (conc., 1.5 mL). The
reaction was heated at 80.degree. C. Zn dust (0.635 g, 9.72 mmol,
each) was added in portions every hour for 7 hours. Stirring at
80.degree. C. was continued for additional 10 hours. The reaction
was cooled to room temperature, and water was added. The resultant
suspension was extracted with EtOAc. The combined organic extracts
were washed with sodium bicarbonate solution and dried over sodium
sulfate. Filtration and evaporation of solvents in vacuo yielded
the crude product, which was purified by silica gel chromatography
to provide 0.375 g (50%) of the product as a white solid. .sup.1H
NMR (300 MHz, CDCl.sub.3): .delta.=1.14 (t, J=7.5 Hz, 3H), 2.18 (s,
3H), 2.71 (q, J=7.5 Hz, 2H), 3.49 (m, 2H), 4.95 (d, J=17.1 Hz, 1H),
5.02 (d, J=10.2 Hz, 1H), 5.23 (s, 2H), 5.98 (m, 1H), 7.66 (s, 1H)
ppm.
##STR00607##
5
6-Allyl-5-ethyl-4-methyl-7-(2-trimethylsilanyl-ethoxy)-3H-isobenzofuran-
-1-one
[1645] To a solution of
6-allyl-5-ethyl-7-hydroxy-4-methyl-3H-isobenzofuran-1-one (199 mg,
0.857 mmol), PPh.sub.3 (337 mg, 1.286 mmol), and
2-trimethylsilylethanol in THF (3 mL) at 0.degree. C. was added
diisopropyl azodicarboxylate (259 mg, 1.286 mmol). The resulting
yellow solution was allowed to warm to room temperature and stirred
for one hour. The solvent was removed in vacuo and the crude
material was dissolved in diethyl ether (3 mL). Hexanes (1.5 mL)
were added. Triphenylphosphine oxide was removed by filtration and
the filtrate was concentrated and purified by silica gel
chromatography to provide the desired product (261 mg, 92%) as a
clear oil. .sup.1H NMR (300 MHz, CDCl.sub.3): .delta.=0.04 (s, 9H),
1.15 (t, J=7.8 Hz, 3H), 1.25 (m, 2H), 2.20 (s, 3H), 2.73 (q, J=7.8
Hz, 2H), 3.54 (m, 2H), 4.28 (m, 2H), 4.95 (d, J=17.1 Hz, 1H), 5.02
(d, J=10.2 Hz, 1H), 5.15 (s, 2H), 5.95 (m, 1H) ppm.
##STR00608##
[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenz-
ofuran-5-yl]-acetaldehyde
[1646] A solution of
6-allyl-5-ethyl-4-methyl-7-(2-trimethylsilanyl-ethoxy)-3H-isobenzofuran-1-
-one (261 mg, 0.788 mmol) in MeOH (5 mL), CH.sub.2Cl.sub.2 (5 mL)
and pyridine (50 .mu.L) was cooled to -78.degree. C. using a dry
ice/acetone bath according to the procedure of Smith, D. B. et al.,
J. Org. Chem., 1996, 61, 6, 2236. A stream of ozone was bubbled
through the reaction via a gas dispersion tube until the reaction
became blue in color (15 minutes). The ozone line was replaced with
a stream of nitrogen and bubbling continued for another 15 minutes,
by which time the blue color had disappeared. To this solution, at
-78.degree. C., was added thiourea (59.9 mg, 0.788 mmol) in one
portion, and the cooling bath was removed. The reaction was allowed
to warn to room temperature and stirred for 15 hours. The reaction
mixture was filtered and then partitioned between CH.sub.2Cl.sub.2
and water. The aqueous layer was extracted with CH.sub.2Cl.sub.2
one more time and the organic extracts were combined, washed with
aqueous 1N HCl, saturated NaHCO.sub.3 and brine and dried over
sodium sulfate. Filtration and evaporation of solvents in vacuo
yielded the crude product, which was purified by silica gel
chromatography to afford 181 mg (69%) of the product as a white
solid. .sup.1H NMR (300 MHz, CDCl.sub.3): .delta.=0.04 (s, 9H),
1.11 (t, J=7.5 Hz, 3H), 1.19 (m, 2H), 2.21 (s, 3H), 2.66 (q, J=7.5
Hz, 2H), 3.90 (s, 2H), 4.36 (m, 2H), 5.18 (s, 2H), 9.71 (s, 1H)
ppm.
##STR00609##
4-[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobe-
nzofuran-5-yl]-2-methyl-but-2-enal
[1647]
[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-i-
sobenzofuran-5-yl]-acetaldehyde (90 mg, 0.269 mmol) and
2-(triphenyl-phosphorylidene)-propionaldehyde (72.9 mg, 0.23 mmol)
in toluene (3 mL) were heated at 100.degree. C. After 15 hours, a
second portion of 2-(triphenyl-phosphanylidene)-propionaldehyde (33
mg, 0.11 mmol) was added and the reaction mixture was heated for
additional 9 hours. The toluene was removed in vacuo, and the
residue was purified by silica gel chromatography to provide 77.6
mg (77%) of the desired product as a pale yellow oil. .sup.1H NMR
(300 MHz, CDCl.sub.3): .delta.=0.03 (s, 9H), 1.15 (t, J=7.5 Hz,
3H), 1.21 (m, 2H), 1.93 (s, 3H), 2.21 (s, 3H), 2.71 (q, J=7.5 Hz,
2H), 3.82 (d, J=6.9 Hz, 2H), 4.34 (m, 2H), 5.18 (s, 2H), 6.38 (m,
1H), 9.35 (s, 1H) ppm.
##STR00610##
5-Ethyl-6-(4-hydroxy-3-methyl-but-2-enyl)-4-methyl-7-(2-trimethylsilanyl--
ethoxy)-3H-isobenzofuran-1-one
[1648]
4-[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enal (77.6 mg, 0.207 mmol) was
dissolved in MeOH (4 mL). A solution of CeCl.sub.3 (51.1 mg, 0.207
mmol) in MeOH/water (9/1, 0.66 mL) was added and the solution was
cooled to 0.degree. C. A solution of lithium borohydride in THF
(2M, 0.105 mL) was added dropwise. After 15 minutes, the reaction
was quenched with 1N HCl (0.5 mL). The MeOH was removed in vacuo
and the crude material was partitioned between DCM and water. The
aqueous layer was extracted with DCM and the combined organic
layers were washed with sodium bicarbonate solution and dried over
sodium sulfate. Filtration and evaporation of solvents yielded a
crude oil, which was purified by silica gel chromatography to
provide 57.2 mg (73%) of the desired product. .sup.1H NMR (300 MHz,
CDCl.sub.3): .delta.=0.04 (s, 9H), 1.15 (t, J=7.8 Hz, 3H), 1.26 (m,
2H), 1.86 (s, 3H), 2.19 (s, 3H), 2.72 (q, J=7.8 Hz, 2H), 3.52 (d,
J=6.3 Hz, 2H), 3.99 (s, 2H), 4.34 (m, 2H), 5.14 (s, 2H), 5.32 (m,
1H) ppm.
##STR00611##
6-(4-Bromo-3-methyl-but-2-enyl)-5-ethyl-4-methyl-7-(2-trimethylsilanyl-et-
hoxy)-3H-isobenzofuran-1-one
[1649]
5-Ethyl-6-(4-hydroxy-3-methyl-but-2-enyl)-4-methyl-7-(2-trimethylsi-
lanyl-ethoxy)-3H-isobenzofuran-1-one (57.2 mg, 0.152 mmol) was
dissolved in DCM (3.5 mL). Polymer-bound triphenylphosphine (3
mmol/g, 152.1 mg) was added and the mixture was mechanically
stirred at room temperature. Carbon tetrabromide (151.3 mg, 0.456
mmol) was added and the solution was stirred at room temperature.
After 2 hours, the reaction was filtered and the solvent was
removed in vacuo. The crude material was purified by silica gel
chromatography to provide 58.0 mg (87%) of the desired product.
.sup.1H NMR (300 MHz, CDCl.sub.3): .delta.=0.04 (s, 9H), 1.15 (t,
J=7.8 Hz, 3H), 1.25 (m, 2H), 1.95 (s, 3H), 2.20 (s, 3H), 2.70 (q,
J=7.8 Hz, 2H), 3.52 (d, J=6.3 Hz, 2H), 3.94 (s, 2H), 4.28 (m, 2H),
5.14 (s, 2H), 5.50 (m, 1H) ppm.
##STR00612##
{4-[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isob-
enzofuran-5-yl]-2-methyl-but-2-enyl}-phosphonic acid
[1650] A solution of
4-[6'-ethyl-7'-methyl-3'-oxo-4'-(2''-trimethylsilanyl-ethoxy)-1',3'-dihyd-
ro-isobenzofuran-5'-yl]-2-methyl-but-2-enyl bromide (58 mg, 0.132
mmol) in trimethylphosphite (0.8 mL) was heated at 110.degree. C.
After 2 hours the reaction was complete. The reaction was cooled to
room temperature and the excess trimethylphosphite was removed in
vacuo. The crude material was used in the next step without further
purification.
[1651] The crude product of the Arbuzov reaction was dissolved in
MeCN (0.8 mL). Trimethylsilyl bromide (202.2 mg, 1.321 mmol) was
added and the reaction was stirred at room temperature. After 15
minutes, lutidine (155.7 mg, 1.453 mmol) was added and stirring at
room temperature was continued. After 2 hours, additional
trimethylsilyl bromide (202.2 mg, 1.321 mmol) was added and
stirring at room temperature was continued. After 4 hours, the
reaction was quenched with MeOH (2 mL). The solvents were
evaporated in vacuo, and the crude material was purified by RP-HPLC
(eluent: water/MeCN). The product-containing fractions were
combined and lyophilized to yield 2.3 mg (5.1%) of the free
phosphonic acid. .sup.1H NMR (300 MHz, DMSO-d6): .delta.=1.07 (t,
J=7.5 Hz, 3H), 1.84 (s, 3H), 2.14 (s, 3H), 2.64 (q, J=7.5 Hz, 2H),
3.34 (m, 4H), 5.06 (m, 1H), 5.25 (s, 2H) ppm; .sup.31P NMR (121
MHz, DMSO-d6): .delta.=22.19 ppm; MS=341 [M.sup.++1].
Example 318
[1652] Representative compounds of the invention can be prepared as
illustrated below.
##STR00613## ##STR00614##
[2-Ethyl-4-[6-ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihy-
dro-isobenzofuran-5-yl]-but-2-enal
[1653]
[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-i-
sobenzofuran-5-yl]-acetaldehyde (90 mg, 0.269 mmol) and
2-(triphenyl-phosphorylidene)-butyraldehyde (98.4 mg, 0.296 mmol)
in toluene (3 mL) were heated at 100.degree. C. After 15 hours, a
second portion of 2-(triphenyl-phosphanylidene)-butyraldehyde (98.4
mg, 0.296 mmol) was added and the reaction mixture was heated for
additional 33 hours. After concentration, the residue was purified
by silica gel chromatography to provide 50.3 mg (48%) of the
desired product as a pale yellow oil.
##STR00615##
5-Ethyl-6-(3-hydroxymethyl-pent-2-enyl)-4-methyl-7-(2-trimethylsilanyl-et-
hoxy)-3H-isobenzofuran-1-one
[1654]
2-Ethyl-4-[6-ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-
-dihydro-isobenzofuran-5-yl]-but-2-enal (50.3 mg, 0.129 mmol) was
dissolved in MeOH (3 mL). A solution of CeCl.sub.3 (31.9 mg, 0.129
mmol) in MeOH/water (9/1, 0.66 mL) was added and the solution was
cooled to 0.degree. C. A solution of lithium borohydride in THF
(2M, 0.065 mL) was added dropwise. After 10 minutes, the reaction
was quenched with 1N HCl (0.5 mL). The methanol was removed in
vacuo and the crude material was partitioned between DCM and water.
The aqueous layer was extracted with DCM and the combined organic
layers were washed with sodium bicarbonate solution and were dried
over sodium sulfate. Filtration and evaporation of solvents in
vacuo yielded a crude oil, which was purified by silica gel
chromatography to provide 35.4 mg (70%) of the desired product.
.sup.1H NMR (300 MHz, CDCl.sub.3): .delta.=0.04 (s, 9H), 1.10-1.19
(m, 6H), 1.26 (m, 2H), 2.19 (s, 3H), 2.32 (q, J=7.5 Hz, 2H), 2.72
(q, J=7.5 Hz, 2H), 3.54 (d, J=6.6 Hz, 2H), 4.05 (s, 2H), 4.26 (m,
2H), 5.14 (s, 2H), 5.27 (m, 1H) ppm.
##STR00616##
6-(3-Bromomethyl-pent-2-enyl)-5-ethyl-4-methyl-7-(2-trimethylsilanyl-etho-
xy)-3H-isobenzofuran-1-one
[1655]
5-Ethyl-6-(3-hydroxymethyl-pent-2-enyl)-4-methyl-7-(2-trimethylsila-
nyl-ethoxy)-3H-isobenzofuran-1-one (35.4 mg, 0.090 mmol) was
dissolved in DCM (3.0 mL). Polymer-bound triphenylphosphine (3
mmol/g, 90.7 mg) was added, and the mixture was mechanically
stirred at room temperature. Carbon tetrabromide (90.2 mg, 0.272
mmol) was added and the solution was stirred at room temperature.
After 2 hours, the reaction was filtered and the solvent was
removed in vacuo. The crude material was purified by silica gel
chromatography to provide 32.0 mg (78%) of the desired product. The
material was used in the next step without further
characterization.
##STR00617##
[2-Ethyl-4-(6-ethyl-4-hydroxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5--
yl)-but-2-enyl]-phosphonic acid
[1656] A solution of
6-(3-bromomethyl-pent-2-enyl)-5-ethyl-4-methyl-7-(2-trimethylsilanyl-etho-
xy)-3H-isobenzofuran-1-one (32 mg, 0.070 mmol) in
trimethylphosphite (0.8 mL) was heated at 110.degree. C. After 2
hours, the reaction was complete. The reaction was cooled to room
temperature and the excess trimethylphosphite was removed in vacuo.
The crude material was used in the next step without further
purification.
[1657] The crude product of the Arbuzov reaction was dissolved in
MeCN (0.8 mL). Trimethylsilyl bromide (108.0 mg, 0.706 mmol) was
added and the reaction was stirred at room temperature. After 2
hours, a second batch of trimethysilyl bromide (108.0 mg, 0.706
mmol) was added. After 3 hours, the reaction was quenched with MeOH
(2 mL). The solvents were evaporated in vacuo and the crude
material was purified by RP-HPLC (eluent: water/MeCN). The
product-containing fractions were combined and lyophilized to yield
15.7 mg (63%) of the product. .sup.1H NMR (300 MHz, DMSO-d6):
.differential.=0.98-1.09 (m, 6H), 2.10 (s, 3H), 2.30 (m, 2H), 2.64
(q, J=7.5 Hz, 2H), 3.38 (m, 4H), 5.03 (m, 1H), 5.25 (s, 2H) ppm;
.sup.31P NMR (121 MHz, DMSO-d6): .delta.=22.26 ppm; MS=355
[M.sup.++1].
Example 319
[1658] Representative compounds of the invention can be prepared as
illustrated below.
##STR00618##
(2-{4-[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-i-
sobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphonic acid
diethyl ester
[1659]
4-[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enal (19.7 mg, 0.052 mmol) and
aminoethylphosphonic acid diethylester oxalate salt (15.6 mg, 0.057
mmol) were dissolved in DMF (0.5 mL). Acetic acid (15.7 mg, 0.263
mmol) was added, followed by sodium triacetoxyborohydride (22.3 mg,
0.105 mmol). After 4 hours, the crude reaction mixture was purified
by RP-HPLC (eluent: water/MeCN) to provide 27.7 mg (97%) of the
desired product after lyophilization. .sup.1H NMR (300 MHz,
CDCl.sub.3): .delta.=0.04 (s, 9H), 1.14 (t, J=7.5 Hz, 3H), 1.26 (m,
2H), 1.30 (t, J=7.2 Hz, 6H), 1.95 (s, 3H), 2.19 (s, 3H), 2.23 (m,
2H), 2.68 (q, J=7.5 Hz, 2H), 3.18 (m, 2H), 3.53 (s, 2H), 4.13 (m,
4H), 4.28 (m, 2H), 5.15 (s, 2H), 5.51 (m, 1H) ppm; .sup.31P NMR
(121 MHz, CDCl.sub.3): .delta.=27.39 ppm; MS=540 [M.sup.++1].
##STR00619##
{2-[4-(6-Ethyl-4-hydroxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2-
-methyl-but-2-enylamino]-ethyl}-phosphonic acid
[1660]
(2-{4-[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dih-
ydro-isobenzofuran-5-yl]-2-methyl-but-2-enylamino}-ethyl)-phosphonic
acid diethyl ester (27.7 mg, 0.051 mmol) was dissolved in DMF (0.5
mL) and DCM (0.5 mL). Trimethylsilyl bromide (78.3 mg, 0.512 mmol)
was added and the reaction was stirred at room temperature. After
20 hours, the reaction was quenched with MeOH (0.3 mL). The
solvents were evaporated in vacuo and the crude material was
purified by RP-HPLC (eluent: water/MeCN). The product-containing
fractions were combined and lyophilized to yield 14.2 mg (57%) of
the free phosphonic acid [MS: 484 M.sup.++1].
[1661] The material was dissolved in DCM (0.5 mL). TFA (0.05 mL)
was added and stirring at room temperature was continued. After 20
minutes, the solvents were removed in vacuo and the crude material
was purified by RP-HPLC (eluent: water/MeCN*0.1% TFA). The
product-containing fractions were combined and lyophilized to yield
7.6 mg (52%) of the product as the TFA salt. .sup.1H NMR (300 MHz,
DMSO-d6): .delta.=1.07 (t, J=7.5 Hz, 3H), 1.84 (s, 3H), 1.90 (m,
2H), 2.11 (s, 3H), 2.63 (q, J=7.5 Hz, 2H), 2.99 (m, 2H), 3.43 (d,
J=6.3 Hz, 2H), 3.51 (s, 2H), 5.26 (s, 2H), 5.45 (m, 1H) ppm;
.sup.31P NMR (121 MHz, DMSO-d6): .delta.=20.02 ppm; MS 384
[M.sup.++1].
##STR00620##
(2-{2-Ethyl-4-[6-ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-d-
ihydro-isobenzofuran-5-yl]-but-2-enylamino}-ethyl)-phosphonic acid
diethyl ester
[1662]
2-Ethyl-4-[6-ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-
-dihydro-isobenzofuran-5-yl]-but-2-enal (26.6 mg, 0.068 mmol) and
aminoethylphosphonic acid diethylester oxalate salt (20.4 mg, 0.075
mmol) were dissolved in DMF (0.8 mL). Acetic acid (20.5 mg, 0.342
mmol) was added, followed by sodium triacetoxyborohydride (27.6 mg,
0.137 mmol). After 8 hours, the crude reaction mixture was purified
by RP-HPLC (eluent: water/MeCN) to provide 24.9 mg (65%) of the
desired product after lyophilization. .sup.1H NMR (300 MHz,
CDCl.sub.3): .delta.=0.05 (s, 9H), 1.10-1.24 (m, 8H), 1.35 (t,
J=7.5 Hz, 6H), 2.19 (s, 3H), 2.23 (m, 2H), 2.35 (q, J=7.8 Hz, 2H),
2.70 (q, J=7.2 Hz, 2H), 3.25 (m, 2H), 3.56 (m, 4H), 4.15 (m, 4H),
4.29 (m, 2H), 5.15 (s, 2H), 5.47 (m, 1H) ppm; .sup.31P NMR (121
MHz, CDCl.sub.3): .delta.=27.71 ppm; MS=554 [M.sup.++1].
##STR00621##
{2-[2-Ethyl-4-(6-ethyl-4-hydroxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-
-5-yl)-but-2-enylamino]-ethyl}-phosphonic acid
[1663]
(2-{2-Ethyl-4-[6-ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-
-1,3-dihydro-isobenzofuran-5-yl]-but-2-enyl
amino}-ethyl)-phosphonic acid diethyl ester (24.9 mg, 0.045 mmol)
was dissolved in DMF (0.5 mL) and DCM (0.5 mL). Trimethylsilyl
bromide (68.7 mg, 0.449 mmol) was added and the reaction was
stirred at room temperature. After 20 hours, the reaction was
quenched with MeOH (0.15 mL). The solvents were evaporated in vacuo
and the crude material was purified by RP-HPLC (eluent:
water/MeCN). The product-containing fractions were combined and
lyophilized to yield 8.0 mg of the free phosphonic acid [MS: 498
M.sup.++1].
[1664] This material was dissolved in DCM (0.5 mL). TFA (0.05 mL)
was added, and stirring at room temperature was continued. After 20
minutes, the solvents were removed in vacuo and the crude material
was purified by RP-HPLC (eluent: water/MeCN*0.1% TFA). The
product-containing fractions were combined and lyophilized to yield
4.4 mg (54%) of the product as the TFA salt. .sup.1H NMR (300 MHz,
DMSO-d6): .delta. 1.05 (m, 6H), 1.60 (m, 2H), 2.10 (s, 3H), 2.67
(q, J=7.5 Hz, 2H), 2.63 (q, J=6.9 Hz, 2H), 2.93 (m, 2H), 3.45 (m,
4H), 5.24 (s, 2H), 5.36 (m, 1H) ppm.; .sup.31P NMR (121 MHz,
DMSO-d6): .delta.=16.93 ppm; MS=398 [M.sup.++1].
Example 320
[1665] Representative compounds of the invention can be prepared as
illustrated below.
##STR00622##
2-({4-[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-i-
sobenzofuran-5-yl]-2-methyl-but-2-enyl}-phenoxy-phosphinoylamino)-propioni-
c acid ethyl ester
[1666]
4-[6'-ethyl-7'-methyl-3'-oxo-4'-(2''-trimethylsilanyl-ethoxy)-1',3'-
-dihydro-isobenzofuran-5'-yl]-2-methyl-but-2-en-phosphonic acid
(44.8 mg, 0.101 mmol), dicyclohexylcarbodiimide (52.6 mg, 0.254
mmol), and phenol (95.8 mg, 1.018 mmol) were dissolved in pyridine
(0.3 mL) and heated at 70.degree. C. for 4 hours. The reaction
mixture was cooled to room temperature and the pyridine was removed
in vacuo. The crude material was partitioned between DCM and HCl
(0.1N). The aqueous layer was extracted with DCM and the combined
organic layers were dried over sodium sulfate. Filtration and
evaporation of solvents in vacuo yielded a crude material, which
was used in the next step without further purification.
[1667] The crude material was dissolved in MeCN (0.8 mL) and water
(0.3 mL). Aqueous sodium hydroxide solution (2N, 0.8 mL) was added
in portions (0.2 mL). After all starting material was consumed, the
organic solvent was removed in vacuo and the crude material was
partitioned between chloroform and aqueous HCl (1N). The aqueous
layer was extracted with chloroform. The combined organic layers
were dried over sodium sulfate. Filtration and evaporation of
solvents yielded the crude product as a mixture of mono phenyl
ester and the symmetrical anhydride.
[1668] The crude material of the previous step and ethyl
(L)-alanine hydrochloride salt (78.1 mg, 0.509 mmol) were dissolved
in DMF (0.4 mL). DMAP (1.2 mg, catalytic) was added, followed by
diisopropylethylamine (131.3 mg, 1.018 mmol). Stirring at room
temperature was continued. After 20 minutes, complete conversion of
the anhydride was observed. After 2 hours, PyBOP (101 mg, 0.202
mmol) was added and stirring at room temperature was continued. The
reaction was filtered and the crude reaction solution was purified
by RP-HPLC (eluent: water/MeCN). The product-containing fractions
were combined and lyophilized to yield the product (15.7 mg, 25%
over three steps) as a white powder. .sup.1H NMR (300 MHz,
CDCl.sub.3): .delta.=0.03 (s, 9H), 1.13-1.28 (m, 8H), 2.03 (s, 3H),
2.19 (s, 3H), 2.62-2.74 (m, 4H), 3.38 (m, 1H), 3.53 (t, J=6.3 Hz,
2H), 4.03 (m, 3H), 4.30 (m, 2H), 5.14 (s, 2H), 5.31 (m, 1H),
7.11-7.17 (m, 3H), 7.25-7.30 (m, 2H) ppm; .sup.31P NMR (121 MHz,
CDCl.sub.3): .delta.=27.04, 27.73 ppm; MS=615 [M.sup.++1].
##STR00623##
2-{[4-(6-Ethyl-4-hydroxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2-
-methyl-but-2-enyl]-phenoxy-phosphinoylamino}-propionic acid ethyl
ester
[1669]
2-({4-[6-Ethyl-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dih-
ydro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-phenoxy-phosphinoylamino)-pr-
opionic acid ethyl ester (7.5 mg, 0.012 mmol) was dissolved in
TFA/DCM (10%, 0.3 mL) at -20.degree. C. The reaction mixture was
warmed to 0.degree. C. and stirred at this temperature for 45
minutes. Pyridine (0.09 mL) was added the solvents were removed in
vacuo. The crude material was purified by RP-HPLC (eluent:
water/MeCN). The product-containing fractions were combined and
lyophilized, yielding a white powder (5.5 mg, 87%). .sup.1H NMR
(300 MHz, CDCl.sub.3): .delta.=1.12-1.29 (m, 6H), 2.03 (s, 3H),
2.17 (s, 3H), 2.65-2.74 (m, 4H), 3.38 (m, 1H), 3.53 (t, J=6.3 Hz,
2H), 4.03 (m, 3H), 5.22 (s, 2H), 5.36 (m, 1H), 7.11-7.16 (m, 3H),
7.24-7.30 (m, 2H), 7.72 (m, 1H) ppm; .sup.31P NMR (121 MHz,
CDCl.sub.3): .delta.=27.11, 27.57 ppm; MS=515 [M.sup.++1].
Example 321
[1670] Representative compounds of the invention can be prepared as
illustrated below.
##STR00624##
6-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-4-methyl-hex-4-enoic acid
[1671] A mixture of
6-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-4-methyl-hex-4-enoic acid methyl ester (1.5 g,
3.45 mmol) and sodium hydroxide (552 mg) in a mixture of methanol
(20 mL) and water (7 mL) was stirred at room temperature for one
hour. The solution was acidified with 1N HCl. The precipitate was
collected by suction filtration and washed with water to give the
desired product (1.2 g, 83%). .sup.1H NMR (300 MHz, CDCl.sub.3)
.delta. 0.02 (s, 9H), 1.15-1.22 (m, 2H), 1.76 (s, 3H), 2.13 (s,
3H), 2.12-2.28 (m, 2H), 2.35-2.41 (m, 2H), 3.37 (d, 2H, J=7 Hz),
3.71 (s, 3H), 4.22-4.28 (m, 2H), 5.07 (s, 2H), 5.13-5.17 (m, 1H)
ppm; MS (m/z) 419.3 [M-H].sup.-, 443.2 [M+Na].sup.+.
##STR00625##
({6-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-i-
sobenzofuran-5-yl]-4-methyl-hex-4-enoylamino}-methyl)-phosphonic
acid diethyl ester
[1672] To a solution of
6-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-4-methyl-hex-4-enoic acid (50 mg, 0.12 mmol) in
THF (1 mL) was added isobutyl chloroformate (17 .mu.L, 0.13 mmol)
and triethylamine (50 .mu.L, 0.36 mmol) at 0.degree. C. After
stirring at 0.degree. C. for 2 hours, diethyl (aminomethyl)
phosphonate oxalate (62 mg, 0.26 mmol) was added and stirring was
continued at room temperature for 20 minutes. After removal of
solvent, the residue was purified by preparative reverse-phase HPLC
to afford 54.8 mg (81%) of the desired product. .sup.1H NMR (300
MHz, CDCl.sub.3) .delta. 0.03 (s, 9H), 1.15-1.22 (m, 2H), 1.31 (t,
6H), 1.81 (s, 3H), 2.18 (s, 3H), 2.30 (m, 4H), 3.41 (d, 2H, J=7
Hz), 3.65 (dd, 2H, J=6, 12 Hz), 3.77 (s, 3H), 3.77-4.16 (m, 4H),
4.26-4.32 (m, 2H), 5.12 (s, 2H), 5.17-5.19 (m, 1H), 5.86 (bs, 1H)
ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta. 23.01 ppm; MS (m/z)
568 [M-H].sup.-, 592 [M+Na].sup.+.
##STR00626##
{[6-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-
-methyl-hex-4-enoylamino]-methyl}-phosphonic acid
[1673] To a solution of
({6-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-i-
sobenzofuran-5-yl]-4-methyl-hex-4-enoyl amino}-methyl)-phosphonic
acid diethyl ester (40 mg, 0.07 mmol) in acetonitrile (1 mL) was
added TMSBr (91 .mu.L, 0.7 mmol) followed by 2,6-lutidine (81.5
.mu.L, 0.7 mmol). The reaction was allowed to proceed overnight
when it was completed as judged by LCMS. The reaction mixture was
quenched with MeOH and concentrated to dryness. The residue was
purified by preparative reverse-phase HPLC to afford 2.6 mg (9%) of
desired product as a white solid. .sup.1H NMR (300 MHz, CD.sub.3OD)
.delta. 1.67 (s, 3H), 2.17 (m, 5H), 2.30-2.46 (m, 2H), 2.80-2.86
(m, 2H), 3.55 (m, 2H), 3.82 (s, 3H), 5.26 (s, 3H) ppm; .sup.31P
(121.4 MHz, CD.sub.3OD) .delta. 10.27 ppm; MS (m/z) 412
[M-H].sup.-, 414 [M+H].sup.+.
Example 322
[1674] Representative compounds of the invention can be prepared as
illustrated below.
##STR00627##
(2-{6-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-4-methyl-hex-4-enoylamino}-ethyl)-phosphonic
acid diethyl ester
[1675] To a solution of
6-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-4-methyl-hex-4-enoic acid (50 mg, 0.12 mmol) in
THF (1 mL) was added isobutyl chloroformate (17 .mu.L, 0.13 mmol)
and triethylamine (50 .mu.L, 0.36 mmol) at 0.degree. C. After
stirring at 0.degree. C. for 2 hours, diethyl (aminoethyl)
phosphonate oxalate (62 mg, 0.26 mmol) was added and stirred at
room temperature was continued for one hour. After removal of
solvent, the residue was purified by preparative reverse-phase HPLC
to afford 37 mg (54%) of the desired product as a white solid.
.sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.03 (s, 9H), 1.15-1.22
(m, 2H), 1.31 (t, 6H), 1.81 (s, 3H), 1.85-1.93 (m, 2H), 2.18 (s,
3H), 2.30 (m, 4H), 3.41 (d, 2H, J=7 Hz), 3.48-3.54 (m, 2H), 3.77
(s, 3H), 3.77-4.16 (m, 4H), 4.26-4.32 (m, 2H), 5.12 (s, 2H),
5.17-5.19 (m, 1H), 6.30 (bs, 1H) ppm; .sup.31P (121.4 MHz,
CDCl.sub.3) .delta. 29.91 ppm; MS (m/z) 584 [M+H].sup.+.
##STR00628##
{2-[6-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-
-4-methyl-hex-4-enoylamino]-ethyl}-phosphonic acid
[1676] To a solution of
(2-{6-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-4-methyl-hex-4-enoylamino}-ethyl)-phosphonic
acid diethyl ester (36.6 mg, 0.063 mmol) in acetonitrile (1 mL) was
added TMSBr (81 .mu.L, 0.63 mmol) followed by 2,6-lutidine (73
.mu.L, 0.63 mmol). The reaction was allowed to proceed overnight,
when it was completed as judged by LCMS. The reaction mixture was
quenched with MeOH and concentrated to dryness. The residue was
purified by preparative reverse-phase HPLC to afford 5.8 mg (29%)
of desired product as a white solid. .sup.1H NMR (300 MHz,
CD.sub.3OD) .delta. 1.80 (s, 3H), 2.14 (m, 5H), 2.25 (m, 4H), 3.35
(m, 2H), 3.38-3.38 (m, 2H), 3.75 (s, 3H), 5.23 (s, 3H) ppm;
.sup.31P (121.4 MHz, CD.sub.3OD) .delta. 26.03 ppm; MS (m/z) 426
[M-H].sup.-, 428 [M+H].sup.+.
Example 323
[1677] Representative compounds of the invention can be prepared as
illustrated below.
##STR00629##
{4-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-is-
obenzofuran-5-yl]-2-methyl-but-2-enyl}-phosphonic acid diphenyl
ester
[1678] To a solution of
[{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-i-
sobenzofuran-5-yl]-2-methyl-but-2-enyl}-phosphonic acid (260 mg,
0.59 mmol) in DMF (6 mL) and phenol (555 mg, 5.9 mmol) was added
dicyclohexyl carbodiimide (1.21 g, 5.9 mmol) and DMAP (36 mg, 0.295
mmol). The reaction mixture was heated to 140.degree. C. for 30
minutes. After cooling to room temperature, the mixture was
partitioned between EtOAc/Hexane (1:1) and 5% aqueous LiCl
solution. The organic layer was washed with 5% aqueous LiCl
solution repeatedly, then dried over Na.sub.2SO.sub.4. After
removal of solvent, the residue was purified by silica gel
chromatography to provide 75 mg (21%) of the desired product. MS
(m/z) 617 [M+Na].sup.+.
##STR00630##
{4-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-is-
obenzofuran-5-yl]-2-methyl-but-2-enyl}-phosphonic acid monophenyl
ester
[1679] To a solution of
{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-is-
obenzofuran-5-yl]-2-methyl-but-2-enyl}-phosphonic acid diphenyl
ester (75 mg, 0.126 mmol) in THF (5 mL) was added 1N NaOH (0.1 mL)
solution. The mixture was allowed to stir at room temperature for
16 hours. EtOAc was added and the resulting mixture was washed with
1H HCl. The organic layer was concentrated to dryness and the
residue was purified by RP HPLC using a C18 column with a gradient
of H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA to provide 24.8 mg
(38%) of the desired product. MS (m/z) 517 [M-H].sup.-, 541
[M+Na].sup.+.
##STR00631##
2-({4-[6-Methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-phenoxy-phosphinoyloxy)-propioni-
c acid ethyl ester
[1680] To a solution of
{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-is-
obenzofuran-5-yl]-2-methyl-but-2-enyl}-phosphonic acid monophenyl
ester (25 mg, 0.048 mmol) and ethyl (S)-(-)-lactate (34 mg, 0.288
mmol) in pyridine (1 mL) was added PyBOP (125 mg, 0.24 mmol). The
solution was stirred at room temperature for 16 hours and
concentrated. The residue was purified by RP HPLC using a C18
column with a gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA
to provide 24 mg (83%) of the desired product. MS (m/z) 641
[M+Na].sup.+.
##STR00632##
2-{[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-
-2-methyl-but-2-enyl]-phenoxy-phosphinoyloxy}-propionic acid ethyl
ester
[1681] To a solution of
2-({4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-
-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-phenoxy-phosphinoyloxy)-propioni-
c acid ethyl ester (24 mg, 0.039 mmol) in DCM (1 mL) was added TFA
(0.5 mL) and the mixture was stirred at room temperature for 10
minutes. The reaction mixture was dried under reduced pressure and
the residue was purified by RP-HPLC to provide 18 mg (90%) of the
desired product as a clear oil. .sup.1H NMR (300 MHz, CDCl.sub.3)
.delta. 1.18-1.34 (m, 3H), 1.36-1.48 (dd, 3H), 2.02 (m, 3H), 2.17
(s, 3H), 2.78-2.98 (dd, 2H), 3.45 (m, 2H), 3.79 (s, 3H), 4.05-4.25
(m, 2H), 4.97 (m, 1H), 5.21 (s, 2H), 5.48 (t, J=7.2 Hz, 1H),
7.05-7.18 (m, 5H) ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta.
24.59, 26.13 ppm; MS (m/z) 517 [M-H].sup.-, 519 [M+H].sup.+.
Example 324
[1682] Representative compounds of the invention can be prepared as
illustrated below.
##STR00633##
2-{[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-
-2-methyl-but-2-enyl]-phenoxy-phosphinoyloxy}-propionic acid
[1683] To a solution of
2-{[4-(4-hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-
-2-methyl-but-2-enyl]-phenoxy-phosphinoyloxy}-propionic acid ethyl
ester (10 mg, 0.019 mmol) in THF (3 mL) was added 1N NaOH (232
.mu.L), and the mixture was stirred at room temperature for 1 hour.
The reaction mixture was dried under reduced pressure and the
residue was purified by RP-HPLC to provide 6 mg (77%) of the
desired product as a clear oil. .sup.1H NMR (300 MHz, CD.sub.3OD)
.delta. 1.41 (d, J=7 Hz, 3H), 1.97 (s, 3H), 2.16 (s, 3H), 2.59 (d,
J=22 Hz, 2H), 3.45 (m, 2H), 3.79 (s, 3H), 4.83 (m, 1H), 5.26 (s,
2H), 5.43 (t, J=7.2 Hz, 1H) ppm; .sup.31P (121.4 MHz, CD.sub.3OD)
.delta. 27.02 ppm; MS (m/z) 413 [M-H].sup.-, 415 [M+H].sup.+.
Example 325
[1684] Representative compounds of the invention can be prepared as
illustrated below.
##STR00634##
2-{[4-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-
-2-methyl-but-2-enyl]-phenoxy-phosphinoylamino}-propionic acid
ethyl ester
[1685]
{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihy-
dro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}-phosphonic acid
monophenyl ester (1 g, .about.1.9 mmol) was combined with pyBOP (2
g, 4 mmol) and DMAP (120 mg, 0.96 mmol). A solution of L-alanine
ethyl ester hydrochloride salt (2.9 g, 19 mmol) and
diisopropylethylamine (6.7 mL, 38 mmol) in pyridine (5 mL) was
added to the monoacid mixture and the reaction was stirred at room
temperature for 12 hours. The reaction mixture was then
concentrated and purified twice by column chromatography (1%
MeOH/CH.sub.2Cl.sub.2 3% MeOH/CH.sub.2Cl.sub.2). The resulting oil
was dissolved in a vigorously-stirred solution of 10%
TFA/CH.sub.2Cl.sub.2 (30 mL) at -40.degree. C. The reaction was
gradually warmed to 0.degree. C. After about 3 hours, the reaction
was complete. Pyridine (4.5 mL) was added, and the reaction mixture
was concentrated. The product was purified by preparative TLC (5%
MeOH/CH.sub.2Cl.sub.2) and concentrated to give 210 mg (21%) of the
desired product as a light yellow oil. .sup.1H NMR (300 MHz,
CDCl.sub.3) .delta. 7.83-7.70 (m, 1H), 7.30-7.20 (m, 2H), 7.18-7.03
(m, 3H), 5.60-5.35 (m, 1H), 5.21 (s, 2H), 4.17-3.95 (m, 3H), 3.79
(s, 3H), 3.60-3.40 (m, 3H), 2.80-2.60 (m, 2H), 2.17 (m, 3H), 2.01
(m, 3H), 1.30-1.10 (m, 6H) ppm; .sup.31P NMR (121 MHz, CDCl.sub.3)
.delta. 28.0, 27.5 ppm; MS (m/z) 516 [M-H].sup.-.
Example 326
[1686] Representative compounds of the invention can be prepared as
illustrated below.
##STR00635##
2-(Dimethoxy-phosphoryl)-6-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilany-
l-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-h ex-4-enoic
acid methyl ester
[1687] To a solution of trimethylphosphonoacetate (63 .mu.L, 0.39
mmol) in THF (1 mL) was added NaN(TMS).sub.2 (0.39 mmol, 0.39 mL)
at ambient temperature. After 30 minutes, a solution of
6-(4-bromo-3-methyl-but-2-enyl)-5-methoxy-4-methyl-7-(2-trimethylsilanyl--
ethoxy)-3H-isobenzofuran-1-one (69 mg, 0.156 mmol) in THF (1 mL)
was added. The reaction mixture was stirred for 2 hours, when a
precipitate was observed. The reaction mixture was worked up by
addition of a saturated aqueous solution of ammonium chloride and
extraction of the product with EtOAc. The organic extract was dried
and the product was purified using silica gel chromatography with
0-100% EtOAc-Hexanes to provide 40 mg of the desired product as a
colorless oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.05 (s,
9H), 1.20-1.26 (m, 2H), 1.79 (s, 3H), 2.17 (s, 3H), 2.42-2.72 (m,
2H), 3.19 (ddd, 1H, J=4, 12, 23 Hz), 3.39 (d, 2H, J=7 Hz), 3.62 (s,
3H), 3.75 (s, 3H), 3.77-3.84 (m, 6H), 4.27-4.34 (m, 2H), 5.12 (s,
2H), 5.24 (t, 1H, J=7 Hz) ppm; .sup.31P (121.4 MHz, CDCl.sub.3)
.delta. 25.1 ppm; MS (m/z) 565.2 [M+Na].sup.+.
##STR00636##
6-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-4-m-
ethyl-2-phosphono-hex-4-enoic acid methyl ester
[1688] To a solution of
2-(dimethoxy-phosphoryl)-6-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilany-
l-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-hex-4-enoic acid
methyl ester (30 mg, 0.055 mmol) in acetonitrile (2 mL) was added
trimethylsilyl bromide (0.18 mL). After 10 minutes, 2,6-lutidine
(0.16 mL) was added to the reaction at ambient temperature. The
reaction was allowed to proceed for 16 hours before it was
concentrated to dryness. The residue was resuspended in a solution
of DMF: H.sub.2O (8:2, 1 mL) and purified by RP HPLC using a C18
column with a gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA
to provide 18 mg of the product as a white powder. .sup.1H NMR (300
MHz, CD.sub.3OD) .delta. 1.81 (s, 3H), 2.16 (s, 3H), 2.40-2.49 (m,
1H), 2.63 (dt, 1H, J=6, 17 Hz), 3.07 (ddd, 1H, J=4, 12, 23 Hz),
3.38 (3, 2H, J=7 Hz), 3.52 (s, 3H), 3.77 (s, 3H), 5.25 (s, 2H),
5.28 (t, 1H, J=7 Hz) ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta.
19.5 ppm; MS (m/z) 415.2 [M+H].sup.+, 437.2 [M+Na].sup.+.
Example 327
[1689] Representative compounds of the invention can be prepared as
illustrated below.
##STR00637##
2-(Bis-(2,2,2-trifluoroethoxy)phosphoryl)-6-[6-methoxy-7-methyl-3-oxo-4-(-
2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-hex-4--
enoic acid methyl ester
[1690] To a solution of
[bis-(2,2,2-trifluoro-ethoxy)-phosphoryl]-acetic acid methyl ester
(186 .mu.L, 0.88 mmol) in anhydrous THF (2 mL) was added a solution
of 1N NaN(TMS).sub.2 in THF (0.88 mL, 0.88 mmol). The solution was
stirred at room temperature for 30 minutes, whereupon a solution of
6-(4-bromo-3-methyl-but-2-enyl)-5-methoxy-4-methyl-7-(2-trimethylsilanyl--
ethoxy)-3H-isobenzofuran-1-one (98 mg, 0.22 mmol) in THF (1 mL) was
added. The reaction mixture was stirred overnight when a
precipitate was observed. The reaction mixture was worked up by
addition of a saturated aqueous solution of ammonium chloride and
extraction of the product with EtOAc. The organic extract was dried
and the product was purified by RP HPLC using a C18 column with a
gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA to provide 72
mg (48%) of the product as a colorless oil. .sup.1H NMR (300 MHz,
CDCl.sub.3) .delta. 0.05 (s, 9H), 1.22 (t, 3H, J=7 Hz), 1.81 (s,
3H), 2.18 (s, 3H), 2.5-2.7 (m, 2H), 3.3 (ddd, 1H, J=4, 12, 23 Hz),
3.40 (d, 2H, J=7 Hz), 3.65 (s, 3H), 3.76 (s, 3H), 4.29-5.13 (m,
6H), 5.13 (s, 2H), 5.28 (t, 1H, J=7 Hz) ppm; MS (m/z) 701.2
[M+Na].sup.+.
##STR00638##
2-(Bis-(2,2,2-trifluoroethoxy)phosphoryl)-6-[6-methoxy-7-methyl-3-oxo-4-(-
2-hydroxyoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-hex-4-enoic
acid methyl ester
[1691]
[2-(Bis-(2,2,2-trifluoroethoxy)phosphoryl)-6-[6-methoxy-7-methyl-3--
oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-isobenzofuran-5-yl]-4-methyl-
-hex-4-enoic acid methyl ester (70 mg) was dissolved in a solution
of 10% trifluoroacetic acid in dichloromethane (5 mL). After 10
minutes, the mixture was concentrated and the product was purified
by RP HPLC using a C18 column with a gradient of H.sub.2O, 0.1%
TFA-acetonitrile, 0.1% TFA to provide 45 mg (75%) of the product as
a colorless oil. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 1.81 (s,
3H), 2.16 (s, 3H), 2.5-2.7 (m, 2H), 3.3 (ddd, 1H), 3.38 (d, 2H, J=7
Hz), 3.65 (s, 3H), 3.77 (s, 3H), 4.33-4.43 (m, 4H), 5.21 (s, 2H),
5.33 (t, 1H, J=7 Hz) ppm; .sup.31P (121.4 MHz, CDCl.sub.3) .delta.
25.8 ppm; MS (m/z) 601.2 [M+Na].sup.+.
Example 328
[1692] Representative compounds of the invention can be prepared as
illustrated below.
##STR00639##
6-(4-Hydroxy-6-methoxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2-[-
hydroxy-(2,2,2-trifluoro-ethoxy)-phosphoryl]-4-methyl-hex-4-enoic
acid
[1693] To a solution of
[bis-(2,2,2-trifluoro-ethoxy)-phosphoryl]-acetic acid methyl ester
(186 .mu.L, 0.88 mmol) in anhydrous THF (0.5 mL) was added a
solution of 1N NaOH (aqueous; 0.06 mL) and N-methylpyrrolidinone
(0.2 mL). After 6.5 hours, another aliquot of 1N NaOH (0.06 mL) was
added and the mixture was stirred overnight. After concentration,
the residue was suspended in DMF (<1 mL), neutralized with a few
drops of TFA and purified by RP HPLC using a C18 column with a
gradient of H.sub.2O, 0.1% TFA-acetonitrile, 0.1% TFA to provide
5.6 mg (72%) of the product as a white powder after lyophilization.
.sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.83 (s, 3H), 2.16 (s,
3H), 2.43-2.51 (m, 1H), 2.59-2.70 (m, 1H), 3.13 (ddd, 1H), 3.40 (d,
2H), 3.76 (s, 3H), 4.36-4.47 (m, 2H), 5.25 (s, 2H), 5.34 (t, 1H,
J=7 Hz) ppm; MS (m/z) 505.2 [M+Na].sup.+.
##STR00640##
Example 329
[1694] Representative compounds of the invention can be prepared as
illustrated below.
[1695] Phosphorous acid
mono-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihyd-
ro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}ester
[1696] To a solution of
6-(4-hydroxy-3-methyl-but-2-enyl)-5-methoxy-4-methyl-7-(2-trimethylsilany-
l-ethoxy)-3H-isobenzofuran-1-one (75 mg, 0.20 mmol) and DIEA (49
.mu.L, 0.28 mmol) in dioxane (2 mL) was added
2-chloro-4H-1,3,2-benzodioxaphosphorin-4-one (56.7 mg, 0.28 mmol)
according the procedure of Shadid, B. et al., Tetrahedron, 1989,
45, 12, 3889. After 10 minutes, another portion of
2-chloro-4H-1,3,2-benzodioxaphosphorin-4-one (40 mg, 0.20 mmol) and
DIEA (35 .mu.L, 0.20 mmol) were added. The reaction was allowed to
proceed at room temperature for an additional hour, after which it
was quenched by the addition of H.sub.2O. The solution was stirred
for another 10 minutes and concentrated in vacuo to a small volume.
The product was triturated with diethyl ether and coevaporated from
acetonitrile (4.times.10 mL) to provide the product. .sup.1H NMR
(300 MHz, CDCl.sub.3) .delta. 0.03 (s, 9H), 1.08-1.30 (m, 2H), 1.84
(br s, 3H), 2.17 (s, 3H), 3.46 (br s, 2H), 3.76 (s, 3H), 4.21-4.39
(m, 4H), 5.12 (s, 2H), 5.43-5.60 (m, 1H), 7.83 (br s, 1H); .sup.31P
(121.4 MHz, CDCl.sub.3) .delta. 7.22; MS (m/z) 441 [M-H].sup.-.
##STR00641##
Example 330
[1697] Representative compounds of the invention can be prepared as
illustrated below.
Phosphoric acid
mono-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihyd-
ro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}ester
[1698] A solution of phosphorous acid
mono-{4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihyd-
ro-isobenzofuran-5-yl]-2-methyl-but-2-enyl}ester (27 mg, 0.06 mmol)
in dioxane (1 mL) was stirred with DIEA (21 .mu.L, 0.12 mmol) and
N,O-bis(trimethylsilyl)acetamide (29 .mu.L, 0.12 mmol) at room
temperature for 3 hours. To the reaction solution was added
2,2'-dipyridyldisulfide (16 mg, 0.072 mmol) and the mixture was
allowed to stir for an additional 2 hours at room temperature. The
reaction mixture was diluted by addition of H.sub.2O and the
solution was stirred for 2 more hours when it was concentrated. The
residue was dissolved in a solution of 10% TFA/CH.sub.2Cl.sub.2 and
stirred at room temperature for 9 hours. The reaction mixture was
dried under reduced pressure and the product was purified by
reverse-phase HPLC to provide the desired product as a white solid.
.sup.1H NMR (300 MHz, CD.sub.3OD) .delta. 1.87 (s, 3H), 2.16 (s,
3H), 3.47 (d, 2H, J=7 Hz), 3.79 (s, 3H), 4.28 (d, 2H, J=6 Hz), 5.26
(s, 2H), 5.50-5.61 (m, 1H); .sup.31P (121.4 MHz, CD.sub.3OD)
.delta. 0.50; MS (m/z) 357 [M-H].sup.-.
Example 331
[1699] Several compounds of the invention are presented below.
##STR00642##
Example 332
[1700] Additional representative compounds of the invention, and
intermediates thereof, can be prepared according to the methods
presented below.
##STR00643##
Synthesis of Phenacetaldehydes with Variants at R.sub.1,
R.sub.2
[1701] The parent compound (R.sub.1.dbd.OMe; R.sub.2=Me) is
accessible by semi-synthesis from mycophenolic acid as follows:
##STR00644##
[1702] To a solution of mycophenolic acid (500 g, 1.56 mol) in MeOH
(4 L) under nitrogen atmosphere was added sulfuric acid (10 mL)
dropwise, and the suspension was stirred at room temperature. After
2 hours, the reaction became homogeneous, and soon thereafter a
precipitate was formed. The reaction was allowed to stir at room
temperature for 10 hours, at which time TLC indicated complete
reaction. The reaction was cooled in an ice bath to 10.degree. C.
and then filtered using a Buchner funnel. The filter cake was
washed with ice cold methanol (750 mL) followed by hexanes (750 mL)
and then dried to give 497 g (95%) of the desired product as a
solid: .sup.1H NMR (300 MHz, CDCl.sub.3) 8, 1.81 (s, 3H), 2.18 (s,
3H), 2.15 (s, 3H), 2.37-2.50 (m, 4H), 3.38 (d, 2H, J=7 Hz), 3.62
(s, 3H), 3.77 (s, 3H), 5.13 (s, 2H), 5.22 (m, 1H), 7.17 (s,
1H).
##STR00645##
[1703] To a solution (3.99 g, 11.9 mmol), PPh.sub.3 (4.68 g, 17.9
mmol), and diisopropyl azodicarboxylate (3.46 mL, 17.9 mmol) in THF
(60 mL) at 0.degree. C. was added a solution of
2-trimethylsilylethanol (2.05 mL, 14.3 mmol) in THF (20 mL). The
resulting yellow solution was allowed to warm to room temperature
and stirred for 4 hours. The reaction was worked up by
concentrating the solution to dryness and addition of ether and
hexanes. Triphenylphosphine oxide was removed by filtration and the
filtrate was concentrated and purified by silica gel chromatography
to provide 4.8 g (100%) as a clear oil: .sup.1H NMR (300 MHz,
CDCl.sub.3) .delta. 0.03 (s, 9H), 1.18-1.30 (m, 2H), 1.81 (s, 3H),
2.18 (s, 3H), 2.25-2.33 (m, 2H), 2.37-2.45 (m, 2H), 3.42 (d, 2H,
J=7 Hz), 3.62 (s, 3H), 3.77 (s, 3H), 4.25-4.35 (m, 2H), 5.13 (s,
2H), 5.12-5.22 (m, 1H).
##STR00646##
[1704] A solution (9.6 g, 22 mmol) in MeOH (90 mL),
CH.sub.2Cl.sub.2 (90 mL) and pyridine (0.7 mL) was cooled to
-70.degree. C. using a dry ice/acetone bath. A stream of ozone was
bubbled through the reaction via a gas dispersion tube until the
reaction became blue in color (1.5 hours). The ozone line was
replaced with a stream of nitrogen and bubbling continued for
another 30 minutes, by which time the blue color had disappeared.
To this solution at -70.degree. C. was added thiourea (1.2 g, 15.4
mmol) in one portion, and the cooling bath was removed. The
reaction was allowed to warm to room temperature and stirred for 15
hours. The reaction was worked up by filtration to remove solid
thiourea S-dioxide, and then partitioned between CH.sub.2Cl.sub.2
and water. The organic layer was removed. The aqueous layer was
washed with CH.sub.2Cl.sub.2 and the organic extracts were
combined, washed with aqueous 1N HCl, saturated NaHCO.sub.3 and
brine, and dried in vacuo. The residue was purified by silica gel
chromatography to afford 7.3 g (99%) as a white solid: .sup.1H NMR
(300 MHz, CDCl.sub.3) .delta. -0.01 (s, 9H), 1.05-1.15 (m, 2H),
2.15 (s, 3H), 3.69 (s, 3H), 3.78 (d, 2H, J=1 Hz), 4.27-4.39 (m,
2H), 5.11 (s, 2H), 9.72 (d, 1H, J=1 Hz).
[1705] R.sub.1 Variants
##STR00647##
[1706] The starting material, synthesized according to J. Med.
Chem., 1996, 39, 4181-4196, is transformed to the desired aldehyde
using methods analogous to those described above.
##STR00648##
[1707] The starting material, synthesized according to J. Med.
Chem., 1996, 39, 4181-4196, is transformed to the desired aldehyde
using methods analogous to those described above.
##STR00649##
[1708] The starting material, synthesized according to J. Med.
Chem., 1996, 39, 4181-4196, is transformed to the desired aldehyde
using methods analogous to those described above.
##STR00650##
[1709] The aldehyde is dissolved in an organic solvent such as
methanol and sodium borohydride is added. At the end of the
reaction, aqueous HCl solution is added and the solvent is removed
in vacuo. Further purification is achieved by chromatography.
[1710] The resulting alcohol is dissolved in an organic solvent
such as dichloromethane (DCM). Pyridine and acetic anhydride are
added and stirring at room temperature is continued. At the end of
the reaction additional DCM is added and the solution is washed
with aqueous HCl solution, aqueous sodium bicarbonate solution, and
dried over sodium sulfate. Filtration and evaporation of the
solvent in vacuo gives the crude product. Further purification is
achieved by chromatography.
[1711] The acetate is dissolved in DCM and bromine is added,
according to a procedure from J. Med. Chem., 1996, 39, 4181-4196.
At the end of the reaction, additional DCM is added and the
solution is washed with aqueous sodium thiosulfate solution and
brine. The organic layer is dried over sodium sulfate. Filtration
and evaporation of solvents yields the crude material. Further
purification is achieved by chromatography.
[1712] The product of the previous step, lithium chloride,
triphenylarsine, tributylvinyltin, and
tris(dibenzylideneacetone)dipalladium(0)-chloroform adduct are
heated in an organic solvent such as N-methylpyrrolidinone at an
elevated temperature of approximately 55.degree. C., according to a
procedure from J. Med. Chem., 1996, 39, 4181-4196. At the end of
the reaction, the mixture is cooled to room temperature and poured
into a mixture of ice, potassium fluoride, water, and ethyl
acetate. Stirring is continued for one hour. The suspension is
filtered through Celite and extracted with ethyl acetate. The
combined organic extracts are dried over sodium sulfate. The
solvents are removed in vacuo and the crude material is further
purified by chromatography.
[1713] The product of the previous step is dissolved in an organic
solvent such as DCM or THF.
1,1,1-tris(acyloxy)-1,1-dihydro-1,2-benziodoxol-3-(1H)-one
(Dess-Martin reagent) is added and the solution is stirred at room
temperature, according to a procedure from J. Org. Chem., 1984, 48,
4155-4156. At the end of the reaction diethyl ether is added,
followed by aqueous sodium hydroxide solution. The layers are
separated and the organic layer is washed with aqueous sodium
hydroxide solution, water, and dried over sodium sulfate.
Filtration and evaporation of solvents yields the crude product.
Further purification is achieved by chromatography.
##STR00651##
[1714] The starting material is dissolved in an organic solvent
such as toluene. P(isobutylNCH.sub.2CH.sub.2).sub.3N, palladium(II)
acetate, sodium tert. butoxide, and benzylamine are added and the
mixture was heated at 80.degree. C., according to a procedure from
J. Org. Chem., 2003, 68, 452-459. At the end of the reaction, the
mixture is cooled to room temperature and the solvents are removed
in vacuo. The crude material is purified by chromatography. Any
residual acetate is removed by brief treatment with methanolic
sodium methoxide.
[1715] The benzyl-protected aniline is dissolved in an organic
solvent such as DMF. Palladium on carbon is added and the reaction
mixture is placed under an atmosphere of hydrogen. At the end of
the reaction, the mixture is filtered through Celite. The solvents
are removed in vacuo. Further purification is achieved by
chromatography.
[1716] The resulting primary aniline is dissolved in an organic
solvent such as THF, acetonitrile, or DMF and is treated with
formaldehyde and sodium triacetoxyborohydride as described in J.
Org. Chem, 1996, 61, 3849-3862. The reaction is quenched with
aqueous sodium bicarbonate and the product is extracted with an
organic solvent such as ethyl acetate. The crude material is
treated with di-t-butyl dicarbonate in an organic solvent such as
dimethylformamide and aqueous sodium hydroxide. The resulting
carbamate is purified by chromatography.
[1717] The primary alcohol product is dissolved in an organic
solvent such as DCM or THF.
1,1,1-tris(acyloxy)-1,1-dihydro-1,2-benziodoxol-3-(1H)-one
(Dess-Martin reagent) is added and the solution is stirred at room
temperature, according to a procedure from J. Org. Chem., 1984, 48,
4155-4156. At the end of the reaction diethyl ether is added,
followed by aqueous sodium hydroxide solution. The layers are
separated and the organic layer is washed with aqueous sodium
hydroxide solution, water, and dried over sodium sulfate.
Filtration and evaporation of solvents yields the crude product.
Further purification is achieved by chromatography.
##STR00652##
[1718] The starting material is dissolved in an organic solvent
such as DCM or THF and is treated with the mixed anhydride of
formic and pivalic acids, according to a procedure from Recl. Trav.
Chem. Pay-Bas, 1982, 101, 460. At the end of the reaction, the
solvent and all volatiles are removed in vacuo and the crude
product is further purified by chromatography.
[1719] The product is dissolved in an organic solvent such as DCM
or THF. 1,1,1-Tris(acyloxy)-1,1-dihydro-1,2-benziodoxol-3-(1H)-one
(Dess-Martin reagent) is added and the solution was stirred at room
temperature, according to a procedure from J. Org. Chem., 1984, 48,
4155-4156. At the end of the reaction diethyl ether is added,
followed by aqueous sodium hydroxide solution. The layers are
separated and the organic layer is washed with aqueous sodium
hydroxide solution, water, and dried over sodium sulfate.
Filtration and evaporation of solvents yields the crude product.
Further purification is achieved by chromatography.
[1720] R.sub.2 Variants
##STR00653##
[1721] The starting material is dissolved in an organic solvent
such as DMF and reacted with N-chlorosuccinimide, according to a
procedure from J. Med. Chem., 1996, 39, 4181-4196. After the
starting material is consumed the reaction mixture is poured into
water and the product is extracted with diethyl ether. The combined
organic layers are dried over sodium sulfate. Filtration and
evaporation of the solvent yields a crude reaction product.
[1722] The product of step one is dissolved in a mixture of organic
solvents such as methanol, DCM, and pyridine. The solution is
cooled to -78.degree. C. and ozone is bubbled into the solution
until a blue color persists. The excess ozone is removed with a
nitrogen stream. The reaction mixture is warmed to room temperature
and thiourea is added. Stirring at room temperature is continued.
The reaction mixture is filtered and partitioned between DCM and
water. The aqueous layer is extracted with DCM and the combined
organic layers are washed with HCl (1 N), saturated aqueous sodium
bicarbonate solution and brine. The solution is dried over sodium
sulfate. Filtration and evaporation of the solvents yields the
crude aldehyde. Further purification is achieved by
chromatography.
##STR00654##
[1723] The starting material is dissolved in a mixture of organic
solvents such as methanol, DCM, and pyridine. The solution is
cooled to -78.degree. C. and ozone is bubbled into the solution
until a blue color persists. The excess ozone is removed with a
nitrogen stream. The reaction mixture is warned to room temperature
and thiourea is added. Stirring at room temperature is continued.
The reaction mixture is filtered and partitioned between DCM and
water. The aqueous layer is extracted with DCM and the combined
organic layers are washed with HCl (1 N), saturated aqueous sodium
bicarbonate solution, and brine. The solution is dried over sodium
sulfate. Filtration and evaporation of the solvents yields the
crude aldehyde. Further purification is achieved by
chromatography.
[1724] The product of step one is dissolved in an organic solvent
such as benzene. Trifluoromethanesulfonyl chloride and
dichlorotris(triphenylphosphine)rhuthenium are added and the
solution is degassed. The reaction mixture is heated at 120.degree.
C., according to a procedure from J. Chem. Soc., Perkin Trans. 1,
1994, 1339-1346. At the end of the reaction the mixture is cooled
to room temperature and the solvent is removed in vacuo. Further
product purification is achieved by chromatography.
Synthesis of Olefins and Linkers to Phosphonates
##STR00655##
[1726] The phenacetaldehyde (5.3 g, 15.8 mmol) in toluene (50 mL)
was heated at 100.degree. C. with
2-(triphenyl-phosphanylidene)-propionaldehyde (6.8 g, 20.5 mmol)
overnight. After concentration, the residue was purified by silica
gel chromatography to provide 4.24 g (72%) of the unsaturated
aldehyde as a pale yellow solid. .sup.1H NMR (300 MHz, CDCl.sub.3)
.delta. 0.00 (s, 9H), 1.10-1.21 (m, 2H), 1.87 (s, 3H), 2.16 (s,
3H), 3.67-3.76 (m, 2H), 3.74 (s, 3H), 4.27-4.39 (m, 2H), 5.11 (s,
2H), 6.40-6.48 (m, 1H), 9.2 (s, 1H).
##STR00656##
[1727] The trimethylsilyethyl protected aldehyde is treated with
diethylphosphite in a solvent such as acetonitrile in the presence
of a base such as triethylamine to afford the hydroxy phosphonate,
according to a procedure such as that reported in Tetrahedron,
1995, 51, 2099. The hydroxy phosphonate is O-alkylated and then the
protecting group is removed by treatment with either
trifluoroacetic acid or tetrabutylammonium fluoride to generate the
desired methoxy phosphonate analog.
[1728] Alternatively, the aldehyde is mixed with diethyl
(2-aminoethyl)phosphonate and treated with a reducing agent such as
sodium triacetoxyborohydride to generate the amino phosphonate
analog.
##STR00657##
[1729] A solution of
4-[6-methoxy-7-methyl-3-oxo-4-(2-trimethylsilanyl-ethoxy)-1,3-dihydro-iso-
benzofuran-5-yl]-2-methyl-but-2-enal (103 mg, 0.27 mmol) in
methanol (5 mL) was cooled to 0.degree. C. A solution of CeCl.sub.3
(0.68 mL, MeOH: H.sub.2O, 9:1) was added, followed by LiBH.sub.4
(0.14 mL, 0.28 mmol of a 2M solution in THF). The ice bath was
removed and the reaction mixture was allowed to warm to room
temperature. The reaction mixture was stirred for an additional 40
minutes whereupon TLC indicated complete consumption of starting
aldehyde. The reaction was worked up by addition of aqueous 1N HCl
(0.5 mL) and the product was extracted with CH.sub.2Cl.sub.2. The
organic layer was washed with saturated aqueous sodium bicarbonate
solution and brine. The organic layer was concentrated under
reduced pressure and the residue was purified by silica gel
chromatography to provide 100 mg (97%) of the product as a clear
liquid. .sup.1H NMR (300 MHz, CDCl.sub.3) .delta. 0.00 (s, 9H),
1.20 (dd, 2H, J=7, 8 Hz), 1.81 (s, 3H), 2.13 (s, 3H), 3.38-3.50 (m,
2H), 3.74 (s, 3H), 3.95 (s, 2H), 4.27 (dd, 2H, J=7, 8 Hz), 5.08 (s,
2H), 5.17-5.44 (m, 1H).
##STR00658##
[1730] Polymer-supported triphenylphosphine is soaked in DCM for 1
hour. The allylic alcohol and carbon tetrabromide are sequentially
added. When the reaction is complete, the mixture is filtered and
the filtrate concentrated. The bromide is purified as necessary by
chromatography.
##STR00659##
[1731] The allylic bromide is treated in an inert organic solvent
such as dimethylformamide with an alkali metal salt of ethyl
diethoxyphosphorylacetate (prepared by reacting ethyl
diethoxyphosphorylacetate with sodium hexamethyldisilazide or
sodium hydride) to afford the ethoxycarbonyl phosphonate, according
to a procedure such as that described in WO 95/22538. The
carboxylic ester group is converted to both the carboxylic amide
and the hydroxymethyl groups according to the methods
conventionally utilized for amide formations and ester reductions.
For example, the carboxylic ester is saponified with aqueous
lithium hydroxide. The acid is activated with ethyl chloroformate
and reduced with sodium borohydride to generate, after removal of
the protecting group, the hydroxymethyl phosphonate analog. The
acid is also converted to its acyl chloride and then reacted with
ethylamine to afford the amide analog.
##STR00660##
[1732] The aryl acetaldehyde is coupled with
2-(diethoxyphosphoryl)-but-3-enoic acid ethyl ester to generate the
2-vinyl substituted ester, according to a procedure such as that
reported in Synthesis, 1999, 282. The 2-vinyl group is converted to
the 2-cyclopropyl group under cyclopropanation conditions such as
those described in Tetrahedron Lett. 1998, 39, 8621. The ester is
converted to the alcohol, which, optionally, can be further
subjected to reactions such as that described below to generate
various phosphonate-containing mycophenolic acid analogues.
##STR00661##
[1733] The allylic alcohol is treated with bromomethylphosphonic
acid diisopropyl ester in the presence of a base such as lithium
t-butoxide in a solvent such as dimethylformamide. The phenol
protecting group is then removed by treatment with trifluoroacetic
acid.
##STR00662##
[1734] The phenacetaldehyde can alternatively be converted to the
allyl phosphonium salt, according to a procedure such as that
reported in J. Org. Chem. 1987, 52, 849. The phosphonium salt is
then treated with the commercially available
3,3,3-trifluoro-2-oxo-propionic acid ethyl ester and a base such as
sodium hydride to generate the 2-trifluoromethyl substituted ester.
The ester is converted to the alcohol, which, optionally, can be
further subjected to reactions described earlier to generate
mycophenolic acid analogues with various side chains containing the
phosphonate group.
##STR00663##
Introduction of R.sub.4 Variants
##STR00664##
[1736] The enone (synthesis reviewed in Tetrahedron, 1985, 41,
4881-4889) and the diene (Chem. Pharm. Bull., 1989, 37, 2948-2951)
are dissolved in an organic solvent such as toluene, stirred at
room temperature for 24 hours and heated to reflux for additional 5
hours, according to a procedure from J. Med. Chem., 1996, 39,
4181-4196. The reaction mixture is cooled to room temperature and
the solvent removed in vacuo. The crude reaction product is further
purified by chromatography.
[1737] The product of step one is dissolved in an organic solvent
such as DCM and m-chloroperbenzoic acid is added, according to a
procedure from J. Med. Chem., 1996, 39, 4181-4196. At the end of
the reaction, the solution is poured into aqueous sodium hydrogen
sulfite solution. The organic layer is washed with saturated
aqueous sodium bicarbonate solution and is dried over sodium
sulfate. Filtration and evaporation of solvents yields the crude
product.
[1738] The crude product is dissolved in an organic solvent such as
toluene and treated with dichlorodicyanoquinone (DDQ), according to
a procedure from J. Med. Chem., 1996, 39, 4181-4196. At the end of
the reaction the solvent is removed in vacuo and the crude material
is further purified by chromatography.
[1739] The product is dissolved in an organic solvent such as DCM
and treated with boron trichloride at reflux temperature, according
to a modified procedure from J. Med. Chem., 1996, 39, 46-55. At the
end of the reaction the solution is washed with aqueous HCl
solution. The solution is dried over sodium sulfate. Removal of the
solvent yields the crude reaction product. Further purification is
achieved by chromatography.
[1740] The product of the previous step and triphenylphosphine are
dissolved in an organic solvent such as tetrahydrofuran (THF).
Diisopropylazodicarboxylate (DIAD) is added dropwise at 0.degree.
C. Stirring is continued. A solution of 2-trimethylsilyl ethanol in
THF is added and stirring is continued. At the end of the reaction,
the solvent is removed in vacuo. The crude reaction solid is
extracted with a mixture of organic solvents such as hexanes and
diethylether. The washings are combined and the solvents removed in
vacuo. The desired product is further purified and separated from
the undesired regioisomer by chromatography.
##STR00665##
[1741] The starting material is dissolved in an organic solvent
such as dimethylformamide (DMF) and reacted with
N-chlorosuccinimide, according to a procedure from J. Med. Chem.,
1996, 39, 4181-4196. After the starting material is consumed the
reaction mixture is poured into water and the product is extracted
with diethyl ether. The combined organic layers are dried over
sodium sulfate. Filtration and evaporation of the solvents yields
the crude product. Further purification is achieved by
chromatography.
##STR00666##
[1742] The starting material is dissolved in an organic solvent
such as benzene and reacted with dimethyl sulfoxide (DMSO),
dicyclohexylcarbodiimide (DCC), and orthophosphoric acid according
to a procedure from J. Am. Chem. Soc., 1966, 88, 5855-5866. At the
end of the reaction, the suspension is filtered and the organic
layer washed with aqueous sodium bicarbonate solution and dried
over sodium sulfate. Filtration and evaporation of solvents yields
the crude material. Further purification is achieved by
chromatography.
[1743] The product of step one is dissolved in an organic solvent
such as DCM or THF and treated with Raney nickel, according to
procedures reviewed in Chem. Rev., 1962, 62, 347-404. When all
starting material is consumed, the reaction is filtered and the
solvent removed in vacuo. Further purification is achieved by
chromatography.
##STR00667##
[1744] The starting material is dissolved in an organic solvent
such as DCM and bromine is added, according to a procedure from J.
Med. Chem., 1996, 39, 4181-4196. At the end of the reaction,
additional DCM is added and the solution washed with aqueous sodium
thiosulfate solution and brine. The organic layer is dried over
sodium sulfate. Filtration and evaporation of solvents yields the
crude material. Further purification is achieved by chromatography
on silica gel.
[1745] The starting material, lithium chloride, triphenylarsine,
tributylvinyltin, and
tris(dibenzylideneacetone)dipalladium(0)-chloroform adduct are
heated in an organic solvent such as N-methylpyrrolidinone at an
elevated temperature of approximately 55.degree. C., according to a
procedure from J. Med. Chem., 1996, 39, 4181-4196. At the end of
the reaction, the mixture is cooled to room temperature and poured
into a mixture of ice, potassium fluoride, water, and ethyl
acetate. Stirring is continued for 1 hour. The suspension is
filtered through Celite and extracted with ethyl acetate. The
combined organic extracts are dried over sodium sulfate. The
solvents are removed in vacuo and the crude material is further
purified by chromatography.
[1746] The product of step two is dissolved in a mixture of organic
solvents such as benzene and ethyl acetate.
Tris(triphenylphosphine)rhodium(I) chloride is added and the
reaction is placed under an atmosphere of hydrogen, according to a
procedure from J. Med. Chem., 1996, 39, 4181-4196. The solvents are
removed in vacuo and the crude reaction is filtered through silica
gel. Further purification is achieved by chromatography.
##STR00668##
[1747] The starting material is dissolved in an organic solvent
such as DMF. Potassium carbonate and allyl bromide are added and
stirring at room temperature is continued, according to a procedure
from J. Med. Chem., 1996, 39, 4181-4196. After all the starting
material is consumed, aqueous HCl solution and diethyl ether are
added and the organic layer is collected and the solvent is removed
in vacuo.
[1748] The crude material is dissolved in N,N diethylaniline and
the reaction mixture is heated at an elevated temperature of ca.
180.degree. C. At the end of the reaction, the mixture is cooled to
room temperature and poured into a mixture of aqueous HCl (2N) and
ethyl acetate. The organic layer is washed with aqueous HCl (2N)
and dried over sodium sulfate. Filtration and removal of the
solvents yields the crude product. Further purification is achieved
by chromatography.
[1749] The product of step 2 is dissolved in a mixture of organic
solvents such as methanol, DCM, and pyridine. The solution is
cooled to -78.degree. C. and ozone is bubbled into the solution
until a blue color persists. The excess ozone is removed with a
nitrogen stream. The reaction mixture is warmed to room temperature
and thiourea is added. Stirring at room temperature is continued.
The reaction mixture is filtered and partitioned between DCM and
water. The aqueous layer is extracted with DCM and the combined
organic layers are washed with HCl (1 N), saturated aqueous sodium
bicarbonate solution and brine. The solution is dried over sodium
sulfate. Filtration and evaporation of the solvents yields the
crude aldehyde. Further purification is achieved by
chromatography.
[1750] The aldehyde is dissolved in an organic solvent such as THF
and is reacted with triphenylphosphonium sec.propyl bromide and
potassium tert.butoxide, according to procedures reviewed in Chem.
Rev., 1989, 89, 863-927. At the end of the reaction, the solvent is
removed in vacuo and the crude material purified by
chromatography.
(A) Introduction of Linkers to Phosphonates
##STR00669##
[1752] The phenols shown herein may optionally be alkylated with
the reagent of choice. Optionally, the phosphonate moiety will be
part of such a reagent. Alternatively, it will be introduced in a
subsequent step by a variety of means, of which three are
illustrated above. For example, an alkyl halide may be heated with
triethylphosphite in a solvent such as toluene (or other Arbuzov
reaction conditions: see Engel, R., "Synthesis of Carbon-phosphorus
Bonds," CRC press, 1988). Alternatively, an epoxide may be reacted
with the anion of a dialkyl phosphinate. In a further example, the
phosphonate reagent may be the electrophile, e.g., an acetylide
anion may be condensed with phosphorus oxychloride and the
intermediate dichlorophosphonate quenched with ethanol to generate
the diethyl ester of the desired phosphonic acid.
Example 333
[1753] A specific compound of the invention can be prepared as
follows.
##STR00670##
[4-(6-Ethyl-4-hydroxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2-me-
thyl-but-2-enyloxymethyl]-phosphonic acid
[1754] This product was prepared using methods similar to those
described herein, e.g., in Examples 292 and 317. MS (negative
mode): 369.3 [M.sup.+-1].
Example 333A
[1755] A specific compound of the invention can be prepared as
follows.
##STR00671##
2-{[4-(6-Ethyl-4-hydroxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl)-2-
-methyl-but-2-enyloxymethyl]-phenoxy-phosphinoylamino}-propionic
acid ethyl ester
[1756] Using methods similar to those described herein, e.g., in
Example 302, the desired product was prepared, starting from
Example 333. MS (positive mode): 546.3 [M.sup.++1] & 568.3
[M.sup.++Na].
Example 334
[1757] A specific compound of the invention can be prepared as
follows:
##STR00672##
2-({2-[4-(6-Ethyl-4-hydroxy-7-methyl-3-oxo-1,3-dihydro-isobenzofuran-5-yl-
)-2-methyl-but-2-enylamino]-ethyl}-phenoxy-phosphinoylamino)-propionic
acid ethyl ester
[1758] This product was prepared using methods analogous to those
described herein, e.g., in Examples 309 and 333, using
2-[(2-amino-ethyl)-phenoxy-phosphinoylamino]-propionic acid ethyl
ester in the reductive amination step. MS (positive mode): 559.4
[M.sup.++1] & 581.3 [M.sup.++Na].
Example 335
[1759] A specific compound of the invention can be prepared as
follows:
##STR00673##
2-((1-Ethoxycarbonyl-ethylamino)-{2-[4-(6-ethyl-4-hydroxy-7-methyl-3-oxo--
1,3-dihydro-isobenzofuran-5-yl)-2-methyl-but-2-enylamino]-ethyl}-phosphino-
ylamino)-propionic acid ethyl ester
[1760] This product was prepared by methods analogous to those
described herein, e.g., in Example 334, using
2-[(2-aminoethyl)-(1-ethoxycarbonyl-ethylamino)-phosphinoylamino]-propion-
ic acid ethyl ester in the reductive amination step. MS (positive
mode): 582.4 [M.sup.++1] & 604.3 [M.sup.++Na].
Example 336
(2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-methy-
l)-phosphonic acid diethyl ester
##STR00674##
[1762] To a solution of
4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoic acid
hemihydrochloride dihydrate (67.0 mg, 177 .mu.mol) in DMF (3.0 mL)
was added diethyl cyanophosphonate (34.8 .mu.L, 230 .mu.mol) and
diisopropylethylamine (Hunig's Base, DIEA, 30.4 .mu.L, 177
.mu.mol). The solution was stirred at ambient temperature for 4
hours when diethyl(aminomethyl)-phosphonate (45.4 mg, 177 .mu.mol)
was added. The solution was stirred for 4 additional hours, when
complete consumption of the starting materials was observed. The
reaction was worked up by removal of the solvent in vacuo and
purifying the residue by silica gel chromatography using
MeOH--CH.sub.2Cl.sub.2 (10-30%). The product collected from this
chromatography step was sufficiently pure to be carried on to the
next reaction. A small amount of the product (20 mg) was repurified
by RP HPLC on C.sub.18 column using H.sub.2O/acetonitrile (2-95%)
to provide 12.9 mg (76%) of the pure product. .sup.1H NMR (300 MHz,
DMSO-d.sub.6) .delta. 1.19 (t, 6H, J=7.2 Hz), 3.21 (s, 3H), 3.70
(m, 2H), 4.00 (q, 4H, J=7.2 Hz), 4.81 (s, 2H), 6.81 (d, 2H, J=9
Hz), 7.71 (d, 2H, J=9 Hz), 8.40 (br s, 1H), 8.61 (s, 1H). .sup.31P
(121.4 MHz, DMSO-d.sub.6) .delta. 23.4. MS (m/z) 475.2 [M+H].sup.+,
597.2 [M+Na].sup.+.
Example 337
(2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-methy-
l)-phosphonic acid
##STR00675##
[1764] To a solution of crude
(2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-ethy-
l)-phosphonic acid diethyl ester post silica column chromatography
(60 mg, 126 .mu.mol) in dry DMF (0.90 mL) was added trimethylsilyl
bromide (bromotrimethylsilane, TMSBr, 130.6 .mu.L, 1,010 .mu.mol)
at ambient temperature. The solution was then heated at 70.degree.
C. for 4.0 hours, after which the reaction mixture was allowed to
cool to room temperature. The solvent volume was reduced to
.about.700 .mu.L in vacuo and diluted with H.sub.2O (100 .mu.L).
This solution was purified by RP HPLC on C.sub.18 column using
H.sub.2O/acetonitrile (2-95%) to provide 26.8 mg (51%) of the
desired compound as a yellow solid. .sup.1H NMR (300 MHz,
DMSO-d.sub.6) .delta. 3.18 (s, 3H), 3.50 (m, 2H), 4.77 (s, 2H),
6.79 (d, 2H, J=9 Hz), 7.79 (d, 2H, J=9 Hz), 8.07 (br s, 1H), 8.56
(s, 1H); MS (m/z) 419.2 [M+H].sup.+.
Example 338
(2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-ethyl-
)-phosphonic acid diethyl ester
##STR00676##
[1766] To a solution of
4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoic acid
hemihydrochloride dihydrate (61.2 mg, 161 .mu.mol) in DMF (2.8 mL)
were added diethyl cyanophosphonate (31.8 .mu.L, 210 .mu.mol) and
DIEA (27.8 .mu.L, 161 .mu.mol). The solution was stirred at ambient
temperature for 4 hours, when diethyl(aminoethyl)phosphonate (43.8
mg, 161 .mu.mol) was added. The solution was stirred for 3
additional hours, by which time complete consumption of the
starting materials was observed. The reaction was worked up by
removal of the solvent in vacuo and purifying the residue by silica
gel chromatography using MeOH--CH.sub.2Cl.sub.2 (10-30%). The
product collected from this chromatography step was sufficiently
pure to be carried on to the next reaction. A small amount of the
product (32 mg) was re-purified by RP HPLC on C.sub.18 column using
H.sub.2O/acetonitrile (2-95%) to provide 19 mg (70%) of the pure
product. .sup.1H NMR (300 MHz, DMSO-d.sub.6) .delta. 1.21 (t, 6H,
J=7 Hz), 1.95-2.05 (m, 2H), 3.20 (s, 3H), 3.13-3.22 (m, 2H), 3.98
(appt septet, 4H, J=7 Hz), 4.79 (s, 2H), 6.80 (d, 2H, J=9 Hz), 7.65
(d, 2H, J=9 Hz), 8.20 (br s, 1H), 8.60 (s, 1H). .sup.31P (121.4
MHz, DMSO-d.sub.6) .delta. 28.9. MS (m/z) 489.2 [M+H].sup.+, 511.2
[M+Na].sup.+.
Example 339
(2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-ethyl-
)-phosphonic acid
##STR00677##
[1768] To a solution of crude
(2-{4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-ethy-
l)-phosphonic acid diethyl ester post silica column chromatography
(61 mg, 125 .mu.mol) in dry DMF (1.00 mL) was added TMSBr (129.0
.mu.L, 999.2 .mu.mol) at ambient temperature. The solution was then
heated at 70.degree. C. for 5.5 hours, when LCMS analysis
demonstrated the reaction to be 90% complete. The reaction mixture
was allowed to cool to room temperature and stirred for an
additional 12 hours. The reaction was worked up by removal of the
solvent in vacuo and dissolving the residue in DMF/H.sub.2O (800
.mu.L, 1:1) and 1N aqueous NaOH (15 .mu.L). The product was
purified by RP HPLC on C.sub.18 column using H.sub.2O/acetonitrile
(2-95%) to provide 29 mg (53%) of the desired compound as a yellow
solid. .sup.1H NMR (300 MHz, DMSO-d.sub.6) .delta. 1.67-1.85 (m,
2H), 3.19 (s, 3H), 3.25-3.40 (m, 2H), 4.76 (s, 2H), 6.71 (br s,
2H), 5.80 (d, 2H, J=9 Hz), 7.64 (d, 2H, J=9 Hz), 7.73 (br s, 2H),
8.15 (br s, 1H), 8.56 (s, 1H). .sup.31P (121.4 MHz, DMSO-d.sub.6)
.delta. 23.0. MS (m/z) 431.3 [M-H].sup.-.
Example 340
(2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-propy-
l)-phosphonic acid diethyl ester
##STR00678##
[1770] To a solution of
4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoic acid
hemihydrochloride dihydrate (61.2 mg, 161 .mu.mol) in DMF (2.8 mL)
were added diethyl cyanophosphonate (31.8 .mu.L, 210 .mu.mol) and
DIEA (27.8 .mu.L, 161 .mu.mol). The solution was stirred at ambient
temperature for 3 hours, when diethyl(aminopropyl)phosphonate (34.9
mg, 122.6 .mu.mol) was added. The solution was stirred for 2
additional hours, whereupon complete consumption of the starting
materials was observed. The reaction was worked up by removal of
the solvent in vacuo and purifying the residue by silica gel
chromatography using MeOH--CH.sub.2Cl.sub.2 (10-30%). The product
(65.5 mg) collected from this chromatography step was sufficiently
pure to be carried on to the next reaction. A small amount (32.8
mg) was re-purified by RP HPLC on C.sub.18 column using
H.sub.2O/acetonitrile (2-95%) to provide 23.2 mg (75%) of the pure
product. .sup.1H NMR (300 MHz, DMSO-d.sub.6) .delta. 1.20 (t, 6H,
J=7.2 Hz), 1.64-1.75 (m, 4H), 3.22 (s, 3H), 3.41 (m, 2H), 3.98
(appt septet, 4H, J=7.2 Hz), 4.85 (s, 2H), 6.79 (d, 2H, J=9 Hz),
7.68 (d, 2H, J=9 Hz), 8.17 (br s, 1H), 8.70 (s, 1H); .sup.31P
(121.4 MHz, DMSO-d.sub.6) .delta. 31.9; MS (m/z) 503.2
[M+H].sup.+.
Example 341
(2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-propy-
l)-phosphonic acid
##STR00679##
[1772] To a solution of crude
(2-{4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-prop-
yl)-phosphonic acid diethyl ester post silica column chromatography
(32.2 mg, 66.2 .mu.mol) in dry DMF (0.50 mL) was added TMSBr (68.0
.mu.L, 529.6 .mu.mol) at ambient temperature. The solution was then
heated at 70.degree. C. for 1.0 hour, when LCMS analysis
demonstrated the reaction to be complete. The reaction mixture was
allowed to cool to room temperature, and water (60 .mu.L) and
methanol (60 .mu.L) were added. The crude reaction mixture was
purified by RP HPLC on C.sub.18 column using H.sub.2O/acetonitrile
(2-95%) to provide 11.2 mg (38%) of the desired compound as a
yellow solid. .sup.1H NMR (300 MHz, DMSO-d.sub.6) .delta. 1.50 (m,
2H), 1.61 (m, 2H), 3.22 (s, 3H), 3.25-3.40 (m, 2H), 4.84 (s, 2H),
6.80 (d, 2H, J=9 Hz), 7.69 (d, 2H, J=9 Hz), 8.20 (br s, 1H), 8.69
(s, 1H). .sup.31P (121.4 MHz, DMSO-d.sub.6) .delta. 26.3. MS (m/z)
447.3 [M-H].sup.-.
Example 342
2-[(2-{4-[(2,4-diaminopteridin-6-ylmethyl)methyl-amino]benzoylamino}-ethyl-
)phenoxyphosphinoyloxy]propionic acid ethyl ester [diastereomeric
mixture at phosphorus]
##STR00680##
[1774] To a solution of
4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoic acid
hemihydrochloride dihydrate (60.0 mg, 158.3 .mu.mol) in DMF (2.5
mL) were added diethyl cyanophosphonate (31.2 .mu.L, 205.7 .mu.mol)
and DIEA (81.8 .mu.L, 474.9 .mu.mol). The solution was stirred at
ambient temperature for 3.5 hours, when a solution of
(S)-2-[(2-aminoethyl)phenoxyphosphinoyloxy]-propionic acid ethyl
ester mono acetic acid salt (57.1 mg, 158.3 .mu.mol; mixture of
diastereomers at phosphorus) in DMF (200 .mu.L) was added. The
solution was stirred for 1.5 additional hours, whereupon complete
consumption of the starting materials was observed. The solvent was
removed in vacuo and the crude material was purified by silica gel
chromatography using MeOH--CH.sub.2Cl.sub.2 (10-30%). A small
amount of the product (24.8 mg) was repurified by RP HPLC on
C.sub.18 column using H.sub.2O/acetonitrile (2-95%) to provide 15.8
mg (65%) of the pure product. .sup.1H NMR (300 MHz, DMSO-d.sub.6)
.delta. 1.17-1.27 (m, 3H), 1.32 (d, 2H, J=7.5 Hz), 1.42 (d, 1H,
J=7.5 Hz) 2.27 (m, 2H), 3.19 (s, 3H), 3.53 (m, 2H), 4.08-4.14 (m,
2H), 4.77 (s, 2H), 4.98 (m, 1H), 6.72 (br s, 1H), 6.81 (d, 2H, J=9
Hz), 7.21 (m, 3H), 7.36 (m, 2H), 7.66 (d, 2H, J=9 Hz), 8.26 (br s,
1H), 8.56 (s, 1H); .sup.31P (121.4 MHz, DMSO-d.sub.6) .delta. 26.6,
27.4. MS (m/z) 609.2 [M+H].sup.+.
Example 343
2-[(2-{4-[(2,4-diaminopteridin-6-ylmethyl)methyl-amino]benzoylamino}-ethyl-
)phenoxyphosphinoyloxy]-propionic acid [diastereomeric mixture at
phosphorus]
##STR00681##
[1776] To a solution of
2-[(2-{4-[(2,4-diaminopteridin-6-ylmethyl)methyl-amino]benzoylamino}ethyl-
)phenoxy-phosphinoyloxy]propionic acid ethyl ester (mixture of
diastereomers at phosphorus; 40.0 mg, 65.7 .mu.mol) in DMF (0.4
mL), acetonitrile (0.2 mL) and water (0.2 mL) was added aqueous
sodium hydroxide (1 N, 131.4 .mu.L). The solution was stirred at
ambient temperature for 4 hours. The solvents were removed in vacuo
and the crude product was purified by RP HPLC on C.sub.18 column
using H.sub.2O/acetonitrile (2-95%) to provide 23.7 mg (71.3%) of
the pure product. .sup.1H NMR (300 MHz, DMSO-d.sub.6) .delta. 1.30
(d, 2H, J=6.9 Hz), 1.79 (m, 2H), 3.21 (s, 3H), 3.37 (m, 2H), 4.61
(m, 1H), 4.81 (s, 2H), 6.79 (d, 2H, J=8.7 Hz), 7.64 (d, 2H, J=9.7
Hz), 8.25 (br s, 1H), 8.63 (s, 1H); .sup.31P (121.4 MHz,
DMSO-d.sub.6) .delta. 25.1. MS (m/z) 505.2 [M+H].sup.+.
Example 343A
2-[(2-{4-[(2,4-diaminopteridin-6-ylmethyl)methylamino]-benzoy-lamino}ethyl-
)phenoxyphosphinoyloxy]propionic acid ethyl ester
[diastereomerically pure at phosphorus]
##STR00682##
[1778] To a solution of
4-[(2,4-diaminopteridin-6-ylmethyl)-methyl-amino]benzoic acid
hemihydrochloride dihydrate (101.9 mg, 268.9 .mu.mol) in DMF (3.3
mL) were added diethyl cyanophosphonate (53.0 .mu.L, 349.5 .mu.mol)
and DIEA (138.0 .mu.L, 806.7 .mu.mol). The solution was stirred at
ambient temperature for 2.5 hours, whereupon
(S)-2-[(2-aminoethyl)phenoxyphosphinoyloxy]-propionic acid ethyl
ester mono acetic acid salt (diastereomerically pure at phosphorus;
268.9 .mu.mol) in DMF (500 .mu.L) was added. The solution was
stirred for 30 additional minutes, whereupon complete consumption
of the starting materials was observed. The solvent was removed in
vacuo and the crude material was purified by silica gel
chromatography using MeOH--CH.sub.2Cl.sub.2 (10-30%). A small
amount of the product (40.0 mg) was repurified by RP HPLC on
C.sub.18 column using H.sub.2O/acetonitrile (2-95%) to provide 28.7
mg (75.1%) of the pure product. .sup.1H NMR (300 MHz, DMSO-d.sub.6)
.delta. 1.15 (t, 3H, J=7.2 Hz), 1.44 (d, 3H, J=6.9 Hz), 2.26 (m,
2H), 3.23 (s, 3H), 3.51 (m, 2H), 4.09 (q, 2H, J=7.2 Hz), 4.86 (s,
2H), 5.01 (m, 1H), 6.81 (d, 2H, J=9.3 Hz), 7.21 (m, 3H), 7.35 (m,
2H), 7.68 (d, 2H, J=9.3 Hz), 8.29 (br s, 1H), 8.71 (s, 1H);
.sup.31P (121.4 MHz, DMSO-d.sub.6) .delta. 26.6. MS (m/z) 609.2
[M+H].sup.+.
Example 344
2-[(2-{4-[(2,4-diaminopteridin-6-ylmethyl)methylamino]-benzoylamino}-ethyl-
)-phenoxyphosphinoylamino]propionic acid ethyl ester (mixture of
diastereomers at phosphorus)
##STR00683##
[1780] To a solution of
4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoic acid
hemihydrochloride dihydrate (39.6 mg, 104.0 .mu.mol) in DMF (1.2
mL) were added diethyl cyanophosphonate (20.6 .mu.L, 136.1 .mu.mol)
and DIEA (36.0 .mu.L, 209.4 .mu.mol). The solution was stirred at
ambient temperature for 3 hours, when
(S)-2-[(2-aminoethyl)phenoxyphosphinoylamino]propionic acid ethyl
ester mono acetic acid salt (mixture of diastereomers at
phosphorus; 104.0 .mu.mol) in DMF (200 .mu.L) was added. The
solution was stirred for 30 minutes when complete consumption of
the starting materials was observed. An aliquot (66%) of the
reaction was purified by silica gel chromatography using
MeOH--CH.sub.2Cl.sub.2 (10-30%), yielding 27.2 mg of crude product.
A small amount of the product (10 mg) was repurified by RP HPLC on
C.sub.18 column using H.sub.2O/acetonitrile (2-95%) to provide 4.2
mg (26%) of the pure product. .sup.1H NMR (300 MHz, DMSO-d.sub.6)
.delta. 1.11 (t, 3H, J=6.9 Hz), 1.18 (d, 3H, J=7.2 Hz), 2.06-2.17
(m, 2H), 3.20 (s, 3H), 3.51 (m, 2H), 3.88 (m, 1H), 4.02 (m, 2H),
4.79 (s, 2H), 5.61 (m, 1H), 6.80 (d, 2H, J=9 Hz), 6.98 (br s, 1H),
7.18 (m, 3H), 7.32 (m, 2H), 7.67 (d, 2H, J=9 Hz), 8.20 (br s, 1H),
8.59 (s, 1H) .sup.31P (121.4 MHz, DMSO-d.sub.6) .delta. 29.5, 30.1.
MS (m/z) 608.2 [M+H].sup.+.
Example 345
2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-6-(die-
thoxy-phosphoryl)-hexanoic acid
##STR00684##
[1782] To a solution of
4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoic acid
hemihydrochloride dihydrate (63.0 mg, 166.2 .mu.mol) in DMF (2.8
mL) were added diethyl cyano phosphonate (30.8 .mu.L, 199.4
.mu.mol) and DIEA (85.8 .mu.L, 498.6 .mu.mol). The solution was
stirred at ambient temperature for 3.5 hours when
(L)-2-amino-6-diethylphosphonatohexanoic acid (44.3 mg, 166.2
.mu.mol) was added. The solution was stirred for 48 additional
hours. The reaction was worked up by removal of the solvent in
vacuo and purifying the residue by silica gel chromatography using
MeOH--CH.sub.2Cl.sub.2 (10-30%). The product (87 mg) collected from
this chromatography step was sufficiently pure to be carried on to
the next reaction. An aliquot of the product (51.0 mg) was
repurified by RP HPLC on C.sub.18 column using
H.sub.2O/acetonitrile (2-95%) to provide 24.7 mg (44%) of the pure
product. .sup.1H NMR (300 MHz, DMSO-d.sub.6) .delta. 1.18 (t, 6H,
J=6.9 Hz), 1.42 (m, 4H), 1.65 (m, 4H), 3.20 (s, 3H), 3.92 (m, 4H),
4.29 (m, 1H), 4.78 (s, 2H), 6.72 (br s, 1H), 6.81 (d, 2H, J=9 Hz),
7.73 (d, 2H, J=9 Hz), 8.14 (d, 1H, J=7.8 Hz), 8.56 (s, 1H);
.sup.31P (121.4 MHz, DMSO-d.sub.6) .delta. 31.8; MS (m/z) 574.3
[M].sup.+.
Example 346
2-{4-[(2,4-Diaminopteridin-6-ylmethyl)methylamino]-benzoylamino}-6-(phosph-
oryl)hexanoic acid
##STR00685##
[1784] To a solution of crude
(2-{4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino})-2'
(L)-(6'-(phosphonic acid diethyl ester) hexanoic acid) post silica
column chromatography (20 mg, 34.6 .mu.mol) in dry DMF (0.60 mL)
was added TMSBr (18.0 .mu.L, 139.2 mmol) at ambient temperature.
The solution was then heated at 70.degree. C. for 18 hours, after
which the reaction mixture was allowed to cool to room temperature.
The solvent was removed in vacuo and dissolved in DMF (400 .mu.L)
and water (60 .mu.L). This solution was purified by RP HPLC on
C.sub.18 column using H.sub.2O/acetonitrile (2-95%) to provide 8.9
mg (49%) of the product as a yellow solid. .sup.1H NMR (300 MHz,
DMSO-d.sub.6) .delta. 1.45 (m, 6H), 1.75 (m, 2H), 3.20 (s, 3H),
4.25 (m, 1H), 4.77 (s, 2H), 6.62 (br s, 1H), 6.80 (d, 2H, J=8.7
Hz), 7.73 (d, 2H, J=8.7 Hz), 8.14 (br s, 1H), 8.55 (s, 1H); MS
(m/z) 519.2 [M+H].sup.+.
Example 347
2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-6'-(mo-
no phenyl-phosphonate)hexanoic acid
##STR00686##
[1786] The ethyl-TMS ester is hydrolyzed under suitable conditions
to provide the corresponding acid of the invention.
[1787] The intermediate
2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-6'-(m-
ono phenyl-phosphonate)-hexanoic acid TMS ethanol ester can be
prepared as follows.
a. (L)-2-Cbz-Amino-hexanoic acid 6-phosphonic acid
##STR00687##
[1789] To a suspension of
(L)-2-amino-6-(diethoxyphosphonyl)hexanoic acid (106 mg, 396.8
.mu.mol) in dry DMF (2.00 mL) was added TMSBr (307.0 .mu.L, 2,381.0
.mu.mol) at ambient temperature. The solution was then heated at
70.degree. C. for 2 hours, after which the reaction mixture was
allowed to cool to room temperature. The solvent was removed in
vacuo. The crude material was dissolved in water (0.25 mL) and NaOH
(1-N, 2.50 mL). Benzyl chloroformate (79.3 .mu.L, 555.5 .mu.mol)
was added and stirring at room temperature was continued. After 2
hours, the solution was washed with ether (2 mL) and the aqueous
layer was acidified with aqueous HCl to pH 1. The aqueous layer was
extracted with EtOAc (3.times.5 mL). The combined organic extracts
were dried over sodium sulfate. Filtration and evaporation of
solvents yielded a crude product, which was sufficiently pure for
further transformations. .sup.1H NMR (300 MHz, DMSO-d.sub.6)
.delta. 1.42-1.65 (m, 8H), 3.90 (m, 1H), 5.02 (s, 2H), 7.32 (s,
5H), 7.55 (m, 1H), 7.94 (s, 1H); .sup.31P (121.4 MHz, DMSO-d.sub.6)
.delta. 26.5; MS (m/z) 345.6 [M+H].sup.+.
b. (L)-2-Amino-hexanoic acid 2' TMS ethyl ester-6-phosphonic acid
mono phenyl ester
##STR00688##
[1791] To a solution of (L)-2-Cbz-amino-hexanoic acid-6-phosphonic
acid (137.3 mg, 397.9 .mu.mol) in 2-TMS ethanol (2.5 mL) was added
acetyl chloride (50 .mu.L). Stirring at room temperature was
continued. After 22 hours complete conversion was observed. The
solvents were removed in vacuo. The crude material was sufficiently
pure for the next step.
[1792] One half of the crude material (198.9 .mu.mol) was dissolved
in toluene (3.0 mL) at room temperature. Thionyl chloride (167.2
mg, 1,416.0 .mu.mol) was added and the reaction mixture was heated
at 70.degree. C. (oil bath). After 4 hours, the reaction was cooled
to room temperature and the solvent was removed in vacuo. The crude
material was re-dissolved in methylene chloride (2.0 mL) and a
solution of phenol (36.6 mg, 389.0 .mu.mol) and DIEA (67.0 .mu.L,
389.0 .mu.mol) in methylene chloride (1.0 mL) was added. Stirring
at room temperature was continued. After 4 hrs the solvents were
removed in vacuo.
[1793] The crude material was dissolved in tetrahydrofuran (THF)
(3.0 mL) and aqueous sodium hydroxide solution (1N, 0.885 mL) was
added. Stirring at room temperature was continued. After 14 hours
the solvent was removed in vacuo to provide the crude phosphonate
mono phenyl ester (63.8 mg). This material was dissolved in 2-TMS
ethanol (1.0 mL) and acetyl chloride (20 .mu.L) was added. Stirring
at room temperature was continued. After 22 hours complete
conversion to the carboxylate ester was observed. The solvents were
removed in vacuo. The material was sufficiently pure for the next
step.
[1794] One half of the crude material (75 .mu.mol) was dissolved in
ethanol (1.5 mL). Pd/C (5%, 20 mg) was added and the reaction was
placed under an atmosphere of hydrogen gas. After 1.5 hours Celite
was added and the crude reaction mixture was filtered through
Celite. The solvents were removed in vacuo and the crude material
was used in the next step without further purification.
c.
2-{4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-6'--
(mono phenyl-phosphonate)-hexanoic acid TMS ethanol ester
##STR00689##
[1796] To a solution of
4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoic acid
hemihydrochloride dihydrate (22.7 mg, 60.0 .mu.mol) in DMF (0.80
mL) were added diethyl cyano phosphonate (12.4 .mu.L, 78.0 .mu.mol)
and DIEA (31.0 .mu.L, 180.0 .mu.mol). The solution was stirred at
ambient temperature for one hour when
(L)-2-amino-6-monophenoxyphosphonatohexanoic acid 2' TMS ethyl
ester (70.5 .mu.mol), suspended in DMF (0.2 mL), was added. The
solution was stirred for 3.5 additional hours. The crude reaction
mixture was purified by RP HPLC on C.sub.18 column using
H.sub.2O/acetonitrile (5-95%) to provide 19.4 mg (46%) of
2-{4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-6'-(m-
ono phenyl-phosphonate)-hexanoic acid TMS ethanol ester. .sup.1H
NMR (300 MHz, DMSO-d.sub.6) .delta. 0.0 (s, 9H), 0.91 (t, 2H, J=8.1
Hz), 1.42-1.53 (m, 4H), 1.67-1.76 (m, 4H), 3.24 (s, 3H), 4.10 (t,
2H, J=8.1 Hz), 4.29 (m, 1H), 4.86 (s, 2H), 6.81 (d, 2H, J=9 Hz),
7.12 (m, 3H), 7.31 (m, 2H), 7.74 (d, 2H, J=9 Hz), 8.14 (d, 1H,
J=7.8 Hz), 8.71 (s, 1H); .sup.31P (121.4 MHz, DMSO-d.sub.6) .delta.
26.2; MS (m/z) 695.2 [M].sup.+.
Example 347A
4-[(2,4-Diamino-pteridin-6-ylmethyl)methylamino]-benzoylamino}-6'-(mono
phenyl mono (S) ethyl lactate-phosphonate)hexanoic acid
##STR00690##
[1798] The ethyl-TMS ester is hydrolyzed under suitable conditions
to provide the corresponding acid of the invention.
[1799] The intermediate
2-{4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-6'-(m-
ono phenyl mono (S) ethyl lactate-phosphonate)-hexanoic acid TMS
ethanol ester can be prepared as follows.
a.
2-{4-[(2,4-Diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-6'--
(mono phenyl mono (S) ethyl lactate-phosphonate)-hexanoic acid TMS
ethanol ester
##STR00691##
[1801] To a solution of
2-{4-[(2,4-diamino-pteridin-6-ylmethyl)-methyl-amino]-benzoylamino}-6'-(m-
ono phenyl-phosphonate)-hexanoic acid TMS ethanol ester (14.5 mg,
20.8 .mu.mol, Example 225) in DMF (0.70 mL) was added PYBOP (32.4
mg, 62.4 .mu.mol), DIEA (21.4 mg, 166.4 .mu.mol) and (S) ethyl
lactate (19.6 mg, 166.4 .mu.mol). The reaction mixture was stirred
at room temperature for one hour. The crude reaction mixture was
purified by RP HPLC on C.sub.18 column using H.sub.2O/acetonitrile
(5-95%) to provide 13.5 mg (81%) of the pure product as a mixture
of diastereomers at phosphorus (.about.4:1). .sup.1H NMR (300 MHz,
CDCl.sub.3) .delta. 0.0 (s, 9H), 1.02 (t, 2H, J=8.7 Hz), 1.23 (t,
3H, J=9.3 Hz), 1.35 (d, 2.4H, J=6.6 Hz), 1.42-1.53 (m, 4.6H),
1.67-1.86 (m, 4H), 3.14 (s, 3H), 4.03-4.27 (m, 4H), 4.71 (br s,
3H), 4.98 (m, 0.8H), 5.10 (m, 0.2H), 6.57 (d, 2H, J=7.5 Hz), 7.00
(m, 1H), 7.16 (m, 3H), 7.30 (m, 2H), 7.63 (d, 2H, J=7.5 Hz), 8.43
(s, 1H); .sup.31P (121.4 MHz, DMSO-d.sub.6) .delta. 30.5, 29.2; MS
(m/z) 795.2 [M].sup.+.
Example 348
[1802] By way of example and not limitation, embodiments of the
invention are named below in tabular format (Table 100). These
embodiments are of the general formula "MBF":
##STR00692##
Each embodiment of MBF is depicted as a substituted nucleus (Sc).
Sc is described in formula 1-151 herein, wherein A.sup.0 is the
point of covalent attachment of Sc to Lg, as well as in Tables 1.1
to 1.5 below. For those embodiments described in Table 100, Sc is a
nucleus designated by a number and each substituent is designated
in order by letter or number. Tables 1.1 to 1.5 are a schedule of
nuclei used in forming the embodiments of Table 100. Each nucleus
(Sc) is given a number designation from Tables 1.1 to 1.5, and this
designation appears first in each embodiment name. Similarly,
Tables 10.1 to 10.19 and 20.1 to 20.36 list the selected linking
groups (Lg) and prodrug (Pd.sup.1 and Pd.sup.2) substituents, again
by letter or number designation, respectively. Accordingly, a
compound of the formula MBF includes compounds having Sc groups
based on formula 1-151 herein as well as compounds according to
Table 100 below. In all cases, compounds of the formula MBF have
groups Lg, Pd.sup.1 and Pd.sup.2 setforth in the Tables below.
[1803] Accordingly, each named embodiment of Table 100 is depicted
by a number designating the nucleus from Table 1.1-1.5, followed by
a letter designating the linking group (Lg) from Table 10.1-10.19,
and two numbers designating the two prodrug groups (Pd.sup.1 and
Pd.sup.2) from Table 20.1-20.36. In graphical tabular form, each
embodiment of Table 100 appears as a name having the syntax:
Sc.Lg.Pd.sup.1.Pd.sup.2
[1804] Each Sc group is shown having a tilda (".about."). The tilda
is the point of covalent attachment of Sc to Lg. Q.sup.1 and
Q.sup.2 of the linking groups (Lg), it should be understood, do not
represent groups or atoms but are simply connectivity designations.
Q.sup.1 is the site of the covalent bond to the nucleus (Sc) and
Q.sup.2 is the site of the covalent bond to the phosphorous atom of
formula MBF. Each prodrug group (Pd.sup.1 and Pd.sup.2) are
covalently bonded to the phosphorous atom of MBF at the tilda
symbol (".about."). Some embodiments of Tables 10.1-10.19 and
20.1-20.36 may be designated as a combination of letters and
numbers (Table 10.1-10.19) or number and letter (Table 20.1-20.36).
For example there are Table 10 entries for BJ1 and BJ2. In any
event, entries of Table 10.1-10.19 always begin with a letter and
those of Table 20.1-20.36 always begin with a number. When a
nucleus (Sc) is shown enclosed within square brackets ("[ ]") and a
covalent bond extends outside the brackets, the point of covalent
attachment of Sc to Lg may be at any substitutable site on SC.
Selection of the point of attachment is described herein. By way of
example and not limitation, the point of attachment is selected
from those depicted in the schemes and examples.
TABLE-US-00004 TABLE 1.1 ##STR00693## ##STR00694## ##STR00695##
##STR00696##
TABLE-US-00005 TABLE 1.2 ##STR00697## ##STR00698##
TABLE-US-00006 TABLE 1.3 ##STR00699## ##STR00700## ##STR00701##
##STR00702##
TABLE-US-00007 TABLE 1.4 ##STR00703## ##STR00704##
TABLE-US-00008 TABLE 1.5 ##STR00705## ##STR00706##
TABLE-US-00009 TABLE 10.1 ##STR00707## Q.sup.1--Q.sup.2 B
##STR00708## ##STR00709## ##STR00710## ##STR00711## ##STR00712##
##STR00713## ##STR00714## ##STR00715## ##STR00716## ##STR00717##
##STR00718## ##STR00719## ##STR00720##
TABLE-US-00010 TABLE 10.2 ##STR00721## ##STR00722## ##STR00723##
##STR00724## ##STR00725## ##STR00726## ##STR00727## ##STR00728##
##STR00729## ##STR00730## ##STR00731## ##STR00732##
TABLE-US-00011 TABLE 10.3 ##STR00733## ##STR00734## ##STR00735##
##STR00736## ##STR00737## ##STR00738## ##STR00739## ##STR00740##
##STR00741## ##STR00742## ##STR00743## ##STR00744##
TABLE-US-00012 TABLE 10.4 ##STR00745## ##STR00746## ##STR00747##
##STR00748## ##STR00749## ##STR00750## ##STR00751## ##STR00752##
##STR00753## ##STR00754## ##STR00755## ##STR00756##
TABLE-US-00013 TABLE 10.5 ##STR00757## ##STR00758## ##STR00759##
##STR00760## ##STR00761## ##STR00762## ##STR00763## ##STR00764##
##STR00765## ##STR00766## ##STR00767## ##STR00768##
TABLE-US-00014 TABLE 10.6 ##STR00769## ##STR00770## ##STR00771##
##STR00772## ##STR00773## ##STR00774##
[1805] Table 10.7
TABLE-US-00015 TABLE 10.7 ##STR00775## BQ ##STR00776## BR
##STR00777## BS ##STR00778## BT ##STR00779## BU ##STR00780## BV
TABLE-US-00016 TABLE 10.8 ##STR00781## ##STR00782## ##STR00783##
##STR00784## ##STR00785## ##STR00786##
TABLE-US-00017 TABLE 10.9 ##STR00787## ##STR00788## ##STR00789##
##STR00790## ##STR00791## ##STR00792##
TABLE-US-00018 TABLE 10.10 ##STR00793## ##STR00794## ##STR00795##
##STR00796## ##STR00797## ##STR00798## ##STR00799## ##STR00800##
##STR00801## ##STR00802## ##STR00803## ##STR00804##
TABLE-US-00019 TABLE 10.11 ##STR00805## ##STR00806## ##STR00807##
##STR00808## ##STR00809## ##STR00810##
TABLE-US-00020 TABLE 10.12 ##STR00811## ##STR00812## ##STR00813##
##STR00814## ##STR00815## ##STR00816##
TABLE-US-00021 TABLE 10.13 ##STR00817## ##STR00818## ##STR00819##
##STR00820## ##STR00821## ##STR00822##
TABLE-US-00022 TABLE 10.14 ##STR00823## ##STR00824## ##STR00825##
##STR00826## ##STR00827## ##STR00828##
TABLE-US-00023 TABLE 10.15 ##STR00829## ##STR00830## ##STR00831##
##STR00832## ##STR00833## ##STR00834## ##STR00835## ##STR00836##
##STR00837## ##STR00838## ##STR00839## ##STR00840##
TABLE-US-00024 TABLE 10.16 ##STR00841## ##STR00842## ##STR00843##
##STR00844## ##STR00845## ##STR00846##
TABLE-US-00025 TABLE 10.17 ##STR00847## ##STR00848## ##STR00849##
##STR00850## ##STR00851## ##STR00852##
TABLE-US-00026 TABLE 10.18 ##STR00853## ##STR00854## ##STR00855##
##STR00856## ##STR00857## ##STR00858##
TABLE-US-00027 TABLE 10.19 ##STR00859## ##STR00860## ##STR00861##
##STR00862## ##STR00863## ##STR00864##
TABLE-US-00028 TABLE 20.1 ##STR00865## ##STR00866## ##STR00867##
##STR00868## ##STR00869## ##STR00870## ##STR00871##
##STR00872##
TABLE-US-00029 TABLE 20.2 ##STR00873## ##STR00874##
##STR00875##
TABLE-US-00030 TABLE 20.3 ##STR00876## ##STR00877## ##STR00878##
##STR00879## ##STR00880## ##STR00881## ##STR00882##
##STR00883##
TABLE-US-00031 TABLE 20.4 ##STR00884## ##STR00885##
##STR00886##
TABLE-US-00032 TABLE 20.5 ##STR00887## ##STR00888## ##STR00889##
##STR00890## ##STR00891## ##STR00892## ##STR00893##
##STR00894##
TABLE-US-00033 TABLE 20.6 ##STR00895## ##STR00896##
##STR00897##
TABLE-US-00034 TABLE 20.7 ##STR00898## ##STR00899## ##STR00900##
##STR00901## ##STR00902## ##STR00903## ##STR00904##
##STR00905##
TABLE-US-00035 TABLE 20.8 ##STR00906## ##STR00907## ##STR00908##
##STR00909## ##STR00910## ##STR00911## ##STR00912##
##STR00913##
TABLE-US-00036 TABLE 20.9 ##STR00914## ##STR00915## ##STR00916##
##STR00917## ##STR00918## ##STR00919## ##STR00920##
##STR00921##
TABLE-US-00037 TABLE 20.10 ##STR00922## ##STR00923##
##STR00924##
TABLE-US-00038 TABLE 20.11 ##STR00925## ##STR00926## ##STR00927##
##STR00928## ##STR00929## ##STR00930## ##STR00931##
##STR00932##
TABLE-US-00039 TABLE 20.12 ##STR00933## ##STR00934##
##STR00935##
TABLE-US-00040 TABLE 20.13 ##STR00936## ##STR00937## ##STR00938##
##STR00939## ##STR00940## ##STR00941## ##STR00942##
##STR00943##
TABLE-US-00041 TABLE 20.14 ##STR00944## ##STR00945##
##STR00946##
TABLE-US-00042 TABLE 20.15 ##STR00947## ##STR00948## ##STR00949##
##STR00950## ##STR00951## ##STR00952## ##STR00953##
##STR00954##
TABLE-US-00043 TABLE 20.16 ##STR00955## ##STR00956## ##STR00957##
##STR00958## ##STR00959## ##STR00960## ##STR00961##
##STR00962##
TABLE-US-00044 TABLE 20.17 ##STR00963## ##STR00964## ##STR00965##
##STR00966## ##STR00967## ##STR00968## ##STR00969##
##STR00970##
TABLE-US-00045 TABLE 20.18 ##STR00971## ##STR00972##
##STR00973##
TABLE-US-00046 TABLE 20.19 ##STR00974## ##STR00975## ##STR00976##
##STR00977## ##STR00978## ##STR00979## ##STR00980##
##STR00981##
TABLE-US-00047 TABLE 20.20 ##STR00982## ##STR00983##
##STR00984##
TABLE-US-00048 TABLE 20.21 ##STR00985## ##STR00986## ##STR00987##
##STR00988## ##STR00989## ##STR00990## ##STR00991##
##STR00992##
TABLE-US-00049 TABLE 20.22 ##STR00993## ##STR00994##
##STR00995##
TABLE-US-00050 TABLE 20.23 ##STR00996## 132 ##STR00997## 133
##STR00998## 134 ##STR00999## 135 ##STR01000## 136 ##STR01001## 137
##STR01002## 138 ##STR01003## 139
TABLE-US-00051 TABLE 20.24 ##STR01004## 140 ##STR01005## 141
##STR01006## 142 ##STR01007## 143 ##STR01008## 144 ##STR01009## 145
##STR01010## 146 ##STR01011## 147
TABLE-US-00052 TABLE 20.25 ##STR01012## 148 ##STR01013## 149
##STR01014## 150 ##STR01015## 151 ##STR01016## 152 ##STR01017## 153
##STR01018## 154 ##STR01019## 155 ##STR01020## 156 ##STR01021## 157
##STR01022## 158 ##STR01023## 159
TABLE-US-00053 TABLE 20.26 ##STR01024## 160 ##STR01025## 161
##STR01026## 162 ##STR01027## 163 ##STR01028## 164 ##STR01029## 165
##STR01030## 166 ##STR01031## 167 ##STR01032## 168 ##STR01033## 169
##STR01034## 170 ##STR01035## 171
TABLE-US-00054 TABLE 20.27 ##STR01036## 172 ##STR01037## 173
##STR01038## 174 ##STR01039## 175 ##STR01040## 176 ##STR01041## 177
##STR01042## 178 ##STR01043## 179
TABLE-US-00055 TABLE 20.28 ##STR01044## 180 ##STR01045## 181
##STR01046## 182 ##STR01047## 183 ##STR01048## 184 ##STR01049##
185
TABLE-US-00056 TABLE 20.29 ##STR01050## 186 ##STR01051## 187
##STR01052## 188 ##STR01053## 189 ##STR01054## 190 ##STR01055## 191
##STR01056## 192 ##STR01057## 193
TABLE-US-00057 TABLE 20.30 ##STR01058## 194 ##STR01059## 195
##STR01060## 196 ##STR01061## 197 ##STR01062## 198 ##STR01063##
199
TABLE-US-00058 TABLE 20.31 ##STR01064## 200 ##STR01065## 201
##STR01066## 202 ##STR01067## 203 ##STR01068## 204 ##STR01069## 205
##STR01070## 206 ##STR01071## 207
TABLE-US-00059 TABLE 20.32 ##STR01072## 208 ##STR01073## 209
##STR01074## 210 ##STR01075## 211 ##STR01076## 212 ##STR01077##
213
TABLE-US-00060 TABLE 20.33 ##STR01078## 214 ##STR01079## 215
##STR01080## 216 ##STR01081## 217 ##STR01082## 218 ##STR01083## 219
##STR01084## 220 ##STR01085## 221
TABLE-US-00061 TABLE 20.34 ##STR01086## 222 ##STR01087## 223
##STR01088## 224 ##STR01089## 225 ##STR01090## 226 ##STR01091##
227
TABLE-US-00062 TABLE 20.35 ##STR01092## 228 ##STR01093## 229
##STR01094## 230 ##STR01095## 231 ##STR01096## 232 ##STR01097## 233
##STR01098## 234 ##STR01099## 235
TABLE-US-00063 TABLE 20.36 ##STR01100## 236 ##STR01101## 237
##STR01102## 238 ##STR01103## 239 ##STR01104## 240 ##STR01105## 241
##STR01106## 242 ##STR01107## 243
TABLE-US-00064 TABLE 20.37 ##STR01108## 244 ##STR01109## 245
##STR01110## 246 ##STR01111## 247
TABLE-US-00065 TABLE 100 Prodrugs of 1.B 1.B.228.228; 1.B.228.229;
1.B.228.230; 1.B.228.231; 1.B.228.236; 1.B.228.237; 1.B.228.238;
1.B.228.239; 1.B.228.154; 1.B.228.157; 1.B.228.166; 1.B.228.169;
1.B.228.172; 1.B.228.175; 1.B.228.240; 1.B.228.244; 1.B.229.228;
1.B.229.229; 1.B.229.230; 1.B.229.231; 1.B.229.236; 1.B.229.237;
1.B.229.238; 1.B.229.239; 1.B.229.154; 1.B.229.157; 1.B.229.166;
1.B.229.169; 1.B.229.172; 1.B.229.175; 1.B.229.240; 1.B.229.244;
1.B.230.228; 1.B.230.229; 1.B.230.230; 1.B.230.231; 1.B.230.236;
1.B.230.237; 1.B.230.238; 1.B.230.239; 1.B.230.154; 1.B.230.157;
1.B.230.166; 1.B.230.169; 1.B.230.172; 1.B.230.175; 1.B.230.240;
1.B.230.244; 1.B.231.228; 1.B.231.229; 1.B.231.230; 1.B.231.231;
1.B.231.236; 1.B.231.237; 1.B.231.238; 1.B.231.239; 1.B.231.154;
1.B.231.157; 1.B.231.166; 1.B.231.169; 1.B.231.172; 1.B.231.175;
1.B.231.240; 1.B.231.244; 1.B.236.228; 1.B.236.229; 1.B.236.230;
1.B.236.231; 1.B.236.236; 1.B.236.237; 1.B.236.238; 1.B.236.239;
1.B.236.154; 1.B.236.157; 1.B.236.166; 1.B.236.169; 1.B.236.172;
1.B.236.175; 1.B.236.240; 1.B.236.244; 1.B.237.228; 1.B.237.229;
1.B.237.230; 1.B.237.231; 1.B.237.236; 1.B.237.237; 1.B.237.238;
1.B.237.239; 1.B.237.154; 1.B.237.157; 1.B.237.166; 1.B.237.169;
1.B.237.172; 1.B.237.175; 1.B.237.240; 1.B.237.244; 1.B.238.228;
1.B.238.229; 1.B.238.230; 1.B.238.231; 1.B.238.236; 1.B.238.237;
1.B.238.238; 1.B.238.239; 1.B.238.154; 1.B.238.157; 1.B.238.166;
1.B.238.169; 1.B.238.172; 1.B.238.175; 1.B.238.240; 1.B.238.244;
1.B.239.228; 1.B.239.229; 1.B.239.230; 1.B.239.231; 1.B.239.236;
1.B.239.237; 1.B.239.238; 1.B.239.239; 1.B.239.154; 1.B.239.157;
1.B.239.166; 1.B.239.169; 1.B.239.172; 1.B.239.175; 1.B.239.240;
1.B.239.244; 1.B.154.228; 1.B.154.229; 1.B.154.230; 1.B.154.231;
1.B.154.236; 1.B.154.237; 1.B.154.238; 1.B.154.239; 1.B.154.154;
1.B.154.157; 1.B.154.166; 1.B.154.169; 1.B.154.172; 1.B.154.175;
1.B.154.240; 1.B.154.244; 1.B.157.228; 1.B.157.229; 1.B.157.230;
1.B.157.231; 1.B.157.236; 1.B.157.237; 1.B.157.238; 1.B.157.239;
1.B.157.154; 1.B.157.157; 1.B.157.166; 1.B.157.169; 1.B.157.172;
1.B.157.175; 1.B.157.240; 1.B.157.244; 1.B.166.228; 1.B.166.229;
1.B.166.230; 1.B.166.231; 1.B.166.236; 1.B.166.237; 1.B.166.238;
1.B.166.239; 1.B.166.154; 1.B.166.157; 1.B.166.166; 1.B.166.169;
1.B.166.172; 1.B.166.175; 1.B.166.240; 1.B.166.244; 1.B.169.228;
1.B.169.229; 1.B.169.230; 1.B.169.231; 1.B.169.236; 1.B.169.237;
1.B.169.238; 1.B.169.239; 1.B.169.154; 1.B.169.157; 1.B.169.166;
1.B.169.169; 1.B.169.172; 1.B.169.175; 1.B.169.240; 1.B.169.244;
1.B.172.228; 1.B.172.229; 1.B.172.230; 1.B.172.231; 1.B.172.236;
1.B.172.237; 1.B.172.238; 1.B.172.239; 1.B.172.154; 1.B.172.157;
1.B.172.166; 1.B.172.169; 1.B.172.172; 1.B.172.175; 1.B.172.240;
1.B.172.244; 1.B.175.228; 1.B.175.229; 1.B.175.230; 1.B.175.231;
1.B.175.236; 1.B.175.237; 1.B.175.238; 1.B.175.239; 1.B.175.154;
1.B.175.157; 1.B.175.166; 1.B.175.169; 1.B.175.172; 1.B.175.175;
1.B.175.240; 1.B.175.244; 1.B.240.228; 1.B.240.229; 1.B.240.230;
1.B.240.231; 1.B.240.236; 1.B.240.237; 1.B.240.238; 1.B.240.239;
1.B.240.154; 1.B.240.157; 1.B.240.166; 1.B.240.169; 1.B.240.172;
1.B.240.175; 1.B.240.240; 1.B.240.244; 1.B.244.228; 1.B.244.229;
1.B.244.230; 1.B.244.231; 1.B.244.236; 1.B.244.237; 1.B.244.238;
1.B.244.239; 1.B.244.154; 1.B.244.157; 1.B.244.166; 1.B.244.169;
1.B.244.172; 1.B.244.175; 1.B.244.240; 1.B.244.244; Prodrugs of 1.D
1.D.228.228; 1.D.228.229; 1.D.228.230; 1.D.228.231; 1.D.228.236;
1.D.228.237; 1.D.228.238; 1.D.228.239; 1.D.228.154; 1.D.228.157;
1.D.228.166; 1.D.228.169; 1.D.228.172; 1.D.228.175; 1.D.228.240;
1.D.228.244; 1.D.229.228; 1.D.229.229; 1.D.229.230; 1.D.229.231;
1.D.229.236; 1.D.229.237; 1.D.229.238; 1.D.229.239; 1.D.229.154;
1.D.229.157; 1.D.229.166; 1.D.229.169; 1.D.229.172; 1.D.229.175;
1.D.229.240; 1.D.229.244; 1.D.230.228; 1.D.230.229; 1.D.230.230;
1.D.230.231; 1.D.230.236; 1.D.230.237; 1.D.230.238; 1.D.230.239;
1.D.230.154; 1.D.230.157; 1.D.230.166; 1.D.230.169; 1.D.230.172;
1.D.230.175; 1.D.230.240; 1.D.230.244; 1.D.231.228; 1.D.231.229;
1.D.231.230; 1.D.231.231; 1.D.231.236; 1.D.231.237; 1.D.231.238;
1.D.231.239; 1.D.231.154; 1.D.231.157; 1.D.231.166; 1.D.231.169;
1.D.231.172; 1.D.231.175; 1.D.231.240; 1.D.231.244; 1.D.236.228;
1.D.236.229; 1.D.236.230; 1.D.236.231; 1.D.236.236; 1.D.236.237;
1.D.236.238; 1.D.236.239; 1.D.236.154; 1.D.236.157; 1.D.236.166;
1.D.236.169; 1.D.236.172; 1.D.236.175; 1.D.236.240; 1.D.236.244;
1.D.237.228; 1.D.237.229; 1.D.237.230; 1.D.237.231; 1.D.237.236;
1.D.237.237; 1.D.237.238; 1.D.237.239; 1.D.237.154; 1.D.237.157;
1.D.237.166; 1.D.237.169; 1.D.237.172; 1.D.237.175; 1.D.237.240;
1.D.237.244; 1.D.238.228; 1.D.238.229; 1.D.238.230; 1.D.238.231;
1.D.238.236; 1.D.238.237; 1.D.238.238; 1.D.238.239; 1.D.238.154;
1.D.238.157; 1.D.238.166; 1.D.238.169; 1.D.238.172; 1.D.238.175;
1.D.238.240; 1.D.238.244; 1.D.239.228; 1.D.239.229; 1.D.239.230;
1.D.239.231; 1.D.239.236; 1.D.239.237; 1.D.239.238; 1.D.239.239;
1.D.239.154; 1.D.239.157; 1.D.239.166; 1.D.239.169; 1.D.239.172;
1.D.239.175; 1.D.239.240; 1.D.239.244; 1.D.154.228; 1.D.154.229;
1.D.154.230; 1.D.154.231; 1.D.154.236; 1.D.154.237; 1.D.154.238;
1.D.154.239; 1.D.154.154; 1.D.154.157; 1.D.154.166; 1.D.154.169;
1.D.154.172; 1.D.154.175; 1.D.154.240; 1.D.154.244; 1.D.157.228;
1.D.157.229; 1.D.157.230; 1.D.157.231; 1.D.157.236; 1.D.157.237;
1.D.157.238; 1.D.157.239; 1.D.157.154; 1.D.157.157; 1.D.157.166;
1.D.157.169; 1.D.157.172; 1.D.157.175; 1.D.157.240; 1.D.157.244;
1.D.166.228; 1.D.166.229; 1.D.166.230; 1.D.166.231; 1.D.166.236;
1.D.166.237; 1.D.166.238; 1.D.166.239; 1.D.166.154; 1.D.166.157;
1.D.166.166; 1.D.166.169; 1.D.166.172; 1.D.166.175; 1.D.166.240;
1.D.166.244; 1.D.169.228; 1.D.169.229; 1.D.169.230; 1.D.169.231;
1.D.169.236; 1.D.169.237; 1.D.169.238; 1.D.169.239; 1.D.169.154;
1.D.169.157; 1.D.169.166; 1.D.169.169; 1.D.169.172; 1.D.169.175;
1.D.169.240; 1.D.169.244; 1.D.172.228; 1.D.172.229; 1.D.172.230;
1.D.172.231; 1.D.172.236; 1.D.172.237; 1.D.172.238; 1.D.172.239;
1.D.172.154; 1.D.172.157; 1.D.172.166; 1.D.172.169; 1.D.172.172;
1.D.172.175; 1.D.172.240; 1.D.172.244; 1.D.175.228; 1.D.175.229;
1.D.175.230; 1.D.175.231; 1.D.175.236; 1.D.175.237; 1.D.175.238;
1.D.175.239; 1.D.175.154; 1.D.175.157; 1.D.175.166; 1.D.175.169;
1.D.175.172; 1.D.175.175; 1.D.175.240; 1.D.175.244; 1.D.240.228;
1.D.240.229; 1.D.240.230; 1.D.240.231; 1.D.240.236; 1.D.240.237;
1.D.240.238; 1.D.240.239; 1.D.240.154; 1.D.240.157; 1.D.240.166;
1.D.240.169; 1.D.240.172; 1.D.240.175; 1.D.240.240; 1.D.240.244;
1.D.244.228; 1.D.244.229; 1.D.244.230; 1.D.244.231; 1.D.244.236;
1.D.244.237; 1.D.244.238; 1.D.244.239; 1.D.244.154; 1.D.244.157;
1.D.244.166; 1.D.244.169; 1.D.244.172; 1.D.244.175; 1.D.244.240;
1.D.244.244; Prodrugs of 1.E 1.E.228.228; 1.E.228.229; 1.E.228.230;
1.E.228.231; 1.E.228.236; 1.E.228.237; 1.E.228.238; 1.E.228.239;
1.E.228.154; 1.E.228.157; 1.E.228.166; 1.E.228.169; 1.E.228.172;
1.E.228.175; 1.E.228.240; 1.E.228.244; 1.E.229.228; 1.E.229.229;
1.E.229.230; 1.E.229.231; 1.E.229.236; 1.E.229.237; 1.E.229.238;
1.E.229.239; 1.E.229.154; 1.E.229.157; 1.E.229.166; 1.E.229.169;
1.E.229.172; 1.E.229.175; 1.E.229.240; 1.E.229.244; 1.E.230.228;
1.E.230.229; 1.E.230.230; 1.E.230.231; 1.E.230.236; 1.E.230.237;
1.E.230.238; 1.E.230.239; 1.E.230.154; 1.E.230.157; 1.E.230.166;
1.E.230.169; 1.E.230.172; 1.E.230.175; 1.E.230.240; 1.E.230.244;
1.E.231.228; 1.E.231.229; 1.E.231.230; 1.E.231.231; 1.E.231.236;
1.E.231.237; 1.E.231.238; 1.E.231.239; 1.E.231.154; 1.E.231.157;
1.E.231.166; 1.E.231.169; 1.E.231.172; 1.E.231.175; 1.E.231.240;
1.E.231.244; 1.E.236.228; 1.E.236.229; 1.E.236.230; 1.E.236.231;
1.E.236.236; 1.E.236.237; 1.E.236.238; 1.E.236.239; 1.E.236.154;
1.E.236.157; 1.E.236.166; 1.E.236.169; 1.E.236.172; 1.E.236.175;
1.E.236.240; 1.E.236.244; 1.E.237.228; 1.E.237.229; 1.E.237.230;
1.E.237.231; 1.E.237.236; 1.E.237.237; 1.E.237.238; 1.E.237.239;
1.E.237.154; 1.E.237.157; 1.E.237.166; 1.E.237.169; 1.E.237.172;
1.E.237.175; 1.E.237.240; 1.E.237.244; 1.E.238.228; 1.E.238.229;
1.E.238.230; 1.E.238.231; 1.E.238.236; 1.E.238.237; 1.E.238.238;
1.E.238.239; 1.E.238.154; 1.E.238.157; 1.E.238.166; 1.E.238.169;
1.E.238.172; 1.E.238.175; 1.E.238.240; 1.E.238.244; 1.E.239.228;
1.E.239.229; 1.E.239.230; 1.E.239.231; 1.E.239.236; 1.E.239.237;
1.E.239.238; 1.E.239.239; 1.E.239.154; 1.E.239.157; 1.E.239.166;
1.E.239.169; 1.E.239.172; 1.E.239.175; 1.E.239.240; 1.E.239.244;
1.E.154.228; 1.E.154.229; 1.E.154.230; 1.E.154.231; 1.E.154.236;
1.E.154.237; 1.E.154.238; 1.E.154.239; 1.E.154.154; 1.E.154.157;
1.E.154.166; 1.E.154.169; 1.E.154.172; 1.E.154.175; 1.E.154.240;
1.E.154.244; 1.E.157.228; 1.E.157.229; 1.E.157.230; 1.E.157.231;
1.E.157.236; 1.E.157.237; 1.E.157.238; 1.E.157.239; 1.E.157.154;
1.E.157.157; 1.E.157.166; 1.E.157.169; 1.E.157.172; 1.E.157.175;
1.E.157.240; 1.E.157.244; 1.E.166.228; 1.E.166.229; 1.E.166.230;
1.E.166.231; 1.E.166.236; 1.E.166.237; 1.E.166.238; 1.E.166.239;
1.E.166.154; 1.E.166.157; 1.E.166.166; 1.E.166.169; 1.E.166.172;
1.E.166.175; 1.E.166.240; 1.E.166.244; 1.E.169.228; 1.E.169.229;
1.E.169.230; 1.E.169.231; 1.E.169.236; 1.E.169.237; 1.E.169.238;
1.E.169.239; 1.E.169.154; 1.E.169.157; 1.E.169.166; 1.E.169.169;
1.E.169.172; 1.E.169.175; 1.E.169.240; 1.E.169.244; 1.E.172.228;
1.E.172.229; 1.E.172.230; 1.E.172.231; 1.E.172.236; 1.E.172.237;
1.E.172.238; 1.E.172.239; 1.E.172.154; 1.E.172.157; 1.E.172.166;
1.E.172.169; 1.E.172.172; 1.E.172.175; 1.E.172.240; 1.E.172.244;
1.E.175.228; 1.E.175.229; 1.E.175.230; 1.E.175.231; 1.E.175.236;
1.E.175.237; 1.E.175.238; 1.E.175.239; 1.E.175.154; 1.E.175.157;
1.E.175.166; 1.E.175.169; 1.E.175.172; 1.E.175.175; 1.E.175.240;
1.E.175.244; 1.E.240.228; 1.E.240.229; 1.E.240.230; 1.E.240.231;
1.E.240.236; 1.E.240.237; 1.E.240.238; 1.E.240.239; 1.E.240.154;
1.E.240.157; 1.E.240.166; 1.E.240.169; 1.E.240.172; 1.E.240.175;
1.E.240.240; 1.E.240.244; 1.E.244.228; 1.E.244.229; 1.E.244.230;
1.E.244.231; 1.E.244.236; 1.E.244.237; 1.E.244.238; 1.E.244.239;
1.E.244.154; 1.E.244.157; 1.E.244.166; 1.E.244.169; 1.E.244.172;
1.E.244.175; 1.E.244.240; 1.E.244.244; Prodrugs of 1.G 1.G.228.228;
1.G.228.229; 1.G.228.230; 1.G.228.231; 1.G.228.236; 1.G.228.237;
1.G.228.238; 1.G.228.239; 1.G.228.154; 1.G.228.157; 1.G.228.166;
1.G.228.169; 1.G.228.172; 1.G.228.175; 1.G.228.240; 1.G.228.244;
1.G.229.228; 1.G.229.229; 1.G.229.230; 1.G.229.231; 1.G.229.236;
1.G.229.237; 1.G.229.238; 1.G.229.239; 1.G.229.154; 1.G.229.157;
1.G.229.166; 1.G.229.169; 1.G.229.172; 1.G.229.175; 1.G.229.240;
1.G.229.244; 1.G.230.228; 1.G.230.229; 1.G.230.230; 1.G.230.231;
1.G.230.236; 1.G.230.237; 1.G.230.238; 1.G.230.239; 1.G.230.154;
1.G.230.157; 1.G.230.166; 1.G.230.169; 1.G.230.172; 1.G.230.175;
1.G.230.240; 1.G.230.244; 1.G.231.228; 1.G.231.229; 1.G.231.230;
1.G.231.231; 1.G.231.236; 1.G.231.237; 1.G.231.238; 1.G.231.239;
1.G.231.154; 1.G.231.157; 1.G.231.166; 1.G.231.169; 1.G.231.172;
1.G.231.175; 1.G.231.240; 1.G.231.244; 1.G.236.228; 1.G.236.229;
1.G.236.230; 1.G.236.231; 1.G.236.236; 1.G.236.237; 1.G.236.238;
1.G.236.239; 1.G.236.154; 1.G.236.157; 1.G.236.166; 1.G.236.169;
1.G.236.172; 1.G.236.175; 1.G.236.240; 1.G.236.244; 1.G.237.228;
1.G.237.229; 1.G.237.230; 1.G.237.231; 1.G.237.236; 1.G.237.237;
1.G.237.238; 1.G.237.239; 1.G.237.154; 1.G.237.157; 1.G.237.166;
1.G.237.169; 1.G.237.172; 1.G.237.175; 1.G.237.240; 1.G.237.244;
1.G.238.228; 1.G.238.229; 1.G.238.230; 1.G.238.231; 1.G.238.236;
1.G.238.237; 1.G.238.238; 1.G.238.239; 1.G.238.154; 1.G.238.157;
1.G.238.166; 1.G.238.169; 1.G.238.172; 1.G.238.175; 1.G.238.240;
1.G.238.244; 1.G.239.228; 1.G.239.229; 1.G.239.230; 1.G.239.231;
1.G.239.236; 1.G.239.237; 1.G.239.238; 1.G.239.239; 1.G.239.154;
1.G.239.157; 1.G.239.166; 1.G.239.169; 1.G.239.172; 1.G.239.175;
1.G.239.240; 1.G.239.244; 1.G.154.228; 1.G.154.229; 1.G.154.230;
1.G.154.231; 1.G.154.236; 1.G.154.237; 1.G.154.238; 1.G.154.239;
1.G.154.154; 1.G.154.157; 1.G.154.166; 1.G.154.169; 1.G.154.172;
1.G.154.175; 1.G.154.240; 1.G.154.244; 1.G.157.228; 1.G.157.229;
1.G.157.230; 1.G.157.231; 1.G.157.236; 1.G.157.237; 1.G.157.238;
1.G.157.239; 1.G.157.154; 1.G.157.157; 1.G.157.166; 1.G.157.169;
1.G.157.172; 1.G.157.175; 1.G.157.240; 1.G.157.244; 1.G.166.228;
1.G.166.229; 1.G.166.230; 1.G.166.231; 1.G.166.236; 1.G.166.237;
1.G.166.238; 1.G.166.239; 1.G.166.154; 1.G.166.157; 1.G.166.166;
1.G.166.169; 1.G.166.172; 1.G.166.175; 1.G.166.240; 1.G.166.244;
1.G.169.228; 1.G.169.229; 1.G.169.230; 1.G.169.231; 1.G.169.236;
1.G.169.237; 1.G.169.238; 1.G.169.239; 1.G.169.154; 1.G.169.157;
1.G.169.166; 1.G.169.169; 1.G.169.172; 1.G.169.175; 1.G.169.240;
1.G.169.244; 1.G.172.228; 1.G.172.229; 1.G.172.230; 1.G.172.231;
1.G.172.236; 1.G.172.237; 1.G.172.238; 1.G.172.239; 1.G.172.154;
1.G.172.157; 1.G.172.166; 1.G.172.169; 1.G.172.172; 1.G.172.175;
1.G.172.240; 1.G.172.244; 1.G.175.228; 1.G.175.229; 1.G.175.230;
1.G.175.231; 1.G.175.236; 1.G.175.237; 1.G.175.238; 1.G.175.239;
1.G.175.154; 1.G.175.157; 1.G.175.166; 1.G.175.169; 1.G.175.172;
1.G.175.175; 1.G.175.240; 1.G.175.244; 1.G.240.228; 1.G.240.229;
1.G.240.230; 1.G.240.231; 1.G.240.236; 1.G.240.237; 1.G.240.238;
1.G.240.239; 1.G.240.154; 1.G.240.157; 1.G.240.166; 1.G.240.169;
1.G.240.172; 1.G.240.175; 1.G.240.240; 1.G.240.244; 1.G.244.228;
1.G.244.229; 1.G.244.230; 1.G.244.231; 1.G.244.236; 1.G.244.237;
1.G.244.238; 1.G.244.239; 1.G.244.154; 1.G.244.157; 1.G.244.166;
1.G.244.169; 1.G.244.172; 1.G.244.175; 1.G.244.240; 1.G.244.244;
Prodrugs of 1.I 1.I.228.228; 1.I.228.229; 1.I.228.230; 1.I.228.231;
1.I.228.236; 1.I.228.237; 1.I.228.238; 1.I.228.239; 1.I.228.154;
1.I.228.157; 1.I.228.166; 1.I.228.169; 1.I.228.172; 1.I.228.175;
1.I.228.240; 1.I.228.244; 1.I.229.228; 1.I.229.229; 1.I.229.230;
1.I.229.231; 1.I.229.236; 1.I.229.237; 1.I.229.238; 1.I.229.239;
1.I.229.154; 1.I.229.157; 1.I.229.166; 1.I.229.169; 1.I.229.172;
1.I.229.175; 1.I.229.240; 1.I.229.244; 1.I.230.228; 1.I.230.229;
1.I.230.230; 1.I.230.231; 1.I.230.236; 1.I.230.237; 1.I.230.238;
1.I.230.239; 1.I.230.154; 1.I.230.157; 1.I.230.166; 1.I.230.169;
1.I.230.172; 1.I.230.175; 1.I.230.240; 1.I.230.244; 1.I.231.228;
1.I.231.229; 1.I.231.230; 1.I.231.231; 1.I.231.236; 1.I.231.237;
1.I.231.238; 1.I.231.239; 1.I.231.154; 1.I.231.157; 1.I.231.166;
1.I.231.169; 1.I.231.172; 1.I.231.175; 1.I.231.240; 1.I.231.244;
1.I.236.228; 1.I.236.229; 1.I.236.230; 1.I.236.231; 1.I.236.236;
1.I.236.237; 1.I.236.238; 1.I.236.239; 1.I.236.154; 1.I.236.157;
1.I.236.166; 1.I.236.169; 1.I.236.172; 1.I.236.175; 1.I.236.240;
1.I.236.244; 1.I.237.228; 1.I.237.229; 1.I.237.230; 1.I.237.231;
1.I.237.236; 1.I.237.237; 1.I.237.238; 1.I.237.239; 1.I.237.154;
1.I.237.157; 1.I.237.166; 1.I.237.169; 1.I.237.172; 1.I.237.175;
1.I.237.240; 1.I.237.244; 1.I.238.228; 1.I.238.229; 1.I.238.230;
1.I.238.231; 1.I.238.236; 1.I.238.237; 1.I.238.238; 1.I.238.239;
1.I.238.154; 1.I.238.157; 1.I.238.166; 1.I.238.169; 1.I.238.172;
1.I.238.175; 1.I.238.240; 1.I.238.244; 1.I.239.228; 1.I.239.229;
1.I.239.230; 1.I.239.231; 1.I.239.236; 1.I.239.237; 1.I.239.238;
1.I.239.239; 1.I.239.154; 1.I.239.157; 1.I.239.166; 1.I.239.169;
1.I.239.172; 1.I.239.175; 1.I.239.240; 1.I.239.244; 1.I.154.228;
1.I.154.229; 1.I.154.230; 1.I.154.231; 1.I.154.236; 1.I.154.237;
1.I.154.238; 1.I.154.239; 1.I.154.154; 1.I.154.157; 1.I.154.166;
1.I.154.169; 1.I.154.172; 1.I.154.175; 1.I.154.240; 1.I.154.244;
1.I.157.228; 1.I.157.229; 1.I.157.230; 1.I.157.231; 1.I.157.236;
1.I.157.237; 1.I.157.238; 1.I.157.239; 1.I.157.154; 1.I.157.157;
1.I.157.166; 1.I.157.169; 1.I.157.172; 1.I.157.175; 1.I.157.240;
1.I.157.244; 1.I.166.228; 1.I.166.229; 1.I.166.230; 1.I.166.231;
1.I.166.236; 1.I.166.237; 1.I.166.238; 1.I.166.239; 1.I.166.154;
1.I.166.157; 1.I.166.166; 1.I.166.169; 1.I.166.172; 1.I.166.175;
1.I.166.240;
1.I.166.244; 1.I.169.228; 1.I.169.229; 1.I.169.230; 1.I.169.231;
1.I.169.236; 1.I.169.237; 1.I.169.238; 1.I.169.239; 1.I.169.154;
1.I.169.157; 1.I.169.166; 1.I.169.169; 1.I.169.172; 1.I.169.175;
1.I.169.240; 1.I.169.244; 1.I.172.228; 1.I.172.229; 1.I.172.230;
1.I.172.231; 1.I.172.236; 1.I.172.237; 1.I.172.238; 1.I.172.239;
1.I.172.154; 1.I.172.157; 1.I.172.166; 1.I.172.169; 1.I.172.172;
1.I.172.175; 1.I.172.240; 1.I.172.244; 1.I.175.228; 1.I.175.229;
1.I.175.230; 1.I.175.231; 1.I.175.236; 1.I.175.237; 1.I.175.238;
1.I.175.239; 1.I.175.154; 1.I.175.157; 1.I.175.166; 1.I.175.169;
1.I.175.172; 1.I.175.175; 1.I.175.240; 1.I.175.244; 1.I.240.228;
1.I.240.229; 1.I.240.230; 1.I.240.231; 1.I.240.236; 1.I.240.237;
1.I.240.238; 1.I.240.239; 1.I.240.154; 1.I.240.157; 1.I.240.166;
1.I.240.169; 1.I.240.172; 1.I.240.175; 1.I.240.240; 1.I.240.244;
1.I.244.228; 1.I.244.229; 1.I.244.230; 1.I.244.231; 1.I.244.236;
1.I.244.237; 1.I.244.238; 1.I.244.239; 1.I.244.154; 1.I.244.157;
1.I.244.166; 1.I.244.169; 1.I.244.172; 1.I.244.175; 1.I.244.240;
1.I.244.244; Prodrugs of 1.J 1.J.228.228; 1.J.228.229; 1.J.228.230;
1.J.228.231; 1.J.228.236; 1.J.228.237; 1.J.228.238; 1.J.228.239;
1.J.228.154; 1.J.228.157; 1.J.228.166; 1.J.228.169; 1.J.228.172;
1.J.228.175; 1.J.228.240; 1.J.228.244; 1.J.229.228; 1.J.229.229;
1.J.229.230; 1.J.229.231; 1.J.229.236; 1.J.229.237; 1.J.229.238;
1.J.229.239; 1.J.229.154; 1.J.229.157; 1.J.229.166; 1.J.229.169;
1.J.229.172; 1.J.229.175; 1.J.229.240; 1.J.229.244; 1.J.230.228;
1.J.230.229; 1.J.230.230; 1.J.230.231; 1.J.230.236; 1.J.230.237;
1.J.230.238; 1.J.230.239; 1.J.230.154; 1.J.230.157; 1.J.230.166;
1.J.230.169; 1.J.230.172; 1.J.230.175; 1.J.230.240; 1.J.230.244;
1.J.231.228; 1.J.231.229; 1.J.231.230; 1.J.231.231; 1.J.231.236;
1.J.231.237; 1.J.231.238; 1.J.231.239; 1.J.231.154; 1.J.231.157;
1.J.231.166; 1.J.231.169; 1.J.231.172; 1.J.231.175; 1.J.231.240;
1.J.231.244; 1.J.236.228; 1.J.236.229; 1.J.236.230; 1.J.236.231;
1.J.236.236; 1.J.236.237; 1.J.236.238; 1.J.236.239; 1.J.236.154;
1.J.236.157; 1.J.236.166; 1.J.236.169; 1.J.236.172; 1.J.236.175;
1.J.236.240; 1.J.236.244; 1.J.237.228; 1.J.237.229; 1.J.237.230;
1.J.237.231; 1.J.237.236; 1.J.237.237; 1.J.237.238; 1.J.237.239;
1.J.237.154; 1.J.237.157; 1.J.237.166; 1.J.237.169; 1.J.237.172;
1.J.237.175; 1.J.237.240; 1.J.237.244; 1.J.238.228; 1.J.238.229;
1.J.238.230; 1.J.238.231; 1.J.238.236; 1.J.238.237; 1.J.238.238;
1.J.238.239; 1.J.238.154; 1.J.238.157; 1.J.238.166; 1.J.238.169;
1.J.238.172; 1.J.238.175; 1.J.238.240; 1.J.238.244; 1.J.239.228;
1.J.239.229; 1.J.239.230; 1.J.239.231; 1.J.239.236; 1.J.239.237;
1.J.239.238; 1.J.239.239; 1.J.239.154; 1.J.239.157; 1.J.239.166;
1.J.239.169; 1.J.239.172; 1.J.239.175; 1.J.239.240; 1.J.239.244;
1.J.154.228; 1.J.154.229; 1.J.154.230; 1.J.154.231; 1.J.154.236;
1.J.154.237; 1.J.154.238; 1.J.154.239; 1.J.154.154; 1.J.154.157;
1.J.154.166; 1.J.154.169; 1.J.154.172; 1.J.154.175; 1.J.154.240;
1.J.154.244; 1.J.157.228; 1.J.157.229; 1.J.157.230; 1.J.157.231;
1.J.157.236; 1.J.157.237; 1.J.157.238; 1.J.157.239; 1.J.157.154;
1.J.157.157; 1.J.157.166; 1.J.157.169; 1.J.157.172; 1.J.157.175;
1.J.157.240; 1.J.157.244; 1.J.166.228; 1.J.166.229; 1.J.166.230;
1.J.166.231; 1.J.166.236; 1.J.166.237; 1.J.166.238; 1.J.166.239;
1.J.166.154; 1.J.166.157; 1.J.166.166; 1.J.166.169; 1.J.166.172;
1.J.166.175; 1.J.166.240; 1.J.166.244; 1.J.169.228; 1.J.169.229;
1.J.169.230; 1.J.169.231; 1.J.169.236; 1.J.169.237; 1.J.169.238;
1.J.169.239; 1.J.169.154; 1.J.169.157; 1.J.169.166; 1.J.169.169;
1.J.169.172; 1.J.169.175; 1.J.169.240; 1.J.169.244; 1.J.172.228;
1.J.172.229; 1.J.172.230; 1.J.172.231; 1.J.172.236; 1.J.172.237;
1.J.172.238; 1.J.172.239; 1.J.172.154; 1.J.172.157; 1.J.172.166;
1.J.172.169; 1.J.172.172; 1.J.172.175; 1.J.172.240; 1.J.172.244;
1.J.175.228; 1.J.175.229; 1.J.175.230; 1.J.175.231; 1.J.175.236;
1.J.175.237; 1.J.175.238; 1.J.175.239; 1.J.175.154; 1.J.175.157;
1.J.175.166; 1.J.175.169; 1.J.175.172; 1.J.175.175; 1.J.175.240;
1.J.175.244; 1.J.240.228; 1.J.240.229; 1.J.240.230; 1.J.240.231;
1.J.240.236; 1.J.240.237; 1.J.240.238; 1.J.240.239; 1.J.240.154;
1.J.240.157; 1.J.240.166; 1.J.240.169; 1.J.240.172; 1.J.240.175;
1.J.240.240; 1.J.240.244; 1.J.244.228; 1.J.244.229; 1.J.244.230;
1.J.244.231; 1.J.244.236; 1.J.244.237; 1.J.244.238; 1.J.244.239;
1.J.244.154; 1.J.244.157; 1.J.244.166; 1.J.244.169; 1.J.244.172;
1.J.244.175; 1.J.244.240; 1.J.244.244; Prodrugs of 1.L 1.L.228.228;
1.L.228.229; 1.L.228.230; 1.L.228.231; 1.L.228.236; 1.L.228.237;
1.L.228.238; 1.L.228.239; 1.L.228.154; 1.L.228.157; 1.L.228.166;
1.L.228.169; 1.L.228.172; 1.L.228.175; 1.L.228.240; 1.L.228.244;
1.L.229.228; 1.L.229.229; 1.L.229.230; 1.L.229.231; 1.L.229.236;
1.L.229.237; 1.L.229.238; 1.L.229.239; 1.L.229.154; 1.L.229.157;
1.L.229.166; 1.L.229.169; 1.L.229.172; 1.L.229.175; 1.L.229.240;
1.L.229.244; 1.L.230.228; 1.L.230.229; 1.L.230.230; 1.L.230.231;
1.L.230.236; 1.L.230.237; 1.L.230.238; 1.L.230.239; 1.L.230.154;
1.L.230.157; 1.L.230.166; 1.L.230.169; 1.L.230.172; 1.L.230.175;
1.L.230.240; 1.L.230.244; 1.L.231.228; 1.L.231.229; 1.L.231.230;
1.L.231.231; 1.L.231.236; 1.L.231.237; 1.L.231.238; 1.L.231.239;
1.L.231.154; 1.L.231.157; 1.L.231.166; 1.L.231.169; 1.L.231.172;
1.L.231.175; 1.L.231.240; 1.L.231.244; 1.L.236.228; 1.L.236.229;
1.L.236.230; 1.L.236.231; 1.L.236.236; 1.L.236.237; 1.L.236.238;
1.L.236.239; 1.L.236.154; 1.L.236.157; 1.L.236.166; 1.L.236.169;
1.L.236.172; 1.L.236.175; 1.L.236.240; 1.L.236.244; 1.L.237.228;
1.L.237.229; 1.L.237.230; 1.L.237.231; 1.L.237.236; 1.L.237.237;
1.L.237.238; 1.L.237.239; 1.L.237.154; 1.L.237.157; 1.L.237.166;
1.L.237.169; 1.L.237.172; 1.L.237.175; 1.L.237.240; 1.L.237.244;
1.L.238.228; 1.L.238.229; 1.L.238.230; 1.L.238.231; 1.L.238.236;
1.L.238.237; 1.L.238.238; 1.L.238.239; 1.L.238.154; 1.L.238.157;
1.L.238.166; 1.L.238.169; 1.L.238.172; 1.L.238.175; 1.L.238.240;
1.L.238.244; 1.L.239.228; 1.L.239.229; 1.L.239.230; 1.L.239.231;
1.L.239.236; 1.L.239.237; 1.L.239.238; 1.L.239.239; 1.L.239.154;
1.L.239.157; 1.L.239.166; 1.L.239.169; 1.L.239.172; 1.L.239.175;
1.L.239.240; 1.L.239.244; 1.L.154.228; 1.L.154.229; 1.L.154.230;
1.L.154.231; 1.L.154.236; 1.L.154.237; 1.L.154.238; 1.L.154.239;
1.L.154.154; 1.L.154.157; 1.L.154.166; 1.L.154.169; 1.L.154.172;
1.L.154.175; 1.L.154.240; 1.L.154.244; 1.L.157.228; 1.L.157.229;
1.L.157.230; 1.L.157.231; 1.L.157.236; 1.L.157.237; 1.L.157.238;
1.L.157.239; 1.L.157.154; 1.L.157.157; 1.L.157.166; 1.L.157.169;
1.L.157.172; 1.L.157.175; 1.L.157.240; 1.L.157.244; 1.L.166.228;
1.L.166.229; 1.L.166.230; 1.L.166.231; 1.L.166.236; 1.L.166.237;
1.L.166.238; 1.L.166.239; 1.L.166.154; 1.L.166.157; 1.L.166.166;
1.L.166.169; 1.L.166.172; 1.L.166.175; 1.L.166.240; 1.L.166.244;
1.L.169.228; 1.L.169.229; 1.L.169.230; 1.L.169.231; 1.L.169.236;
1.L.169.237; 1.L.169.238; 1.L.169.239; 1.L.169.154; 1.L.169.157;
1.L.169.166; 1.L.169.169; 1.L.169.172; 1.L.169.175; 1.L.169.240;
1.L.169.244; 1.L.172.228; 1.L.172.229; 1.L.172.230; 1.L.172.231;
1.L.172.236; 1.L.172.237; 1.L.172.238; 1.L.172.239; 1.L.172.154;
1.L.172.157; 1.L.172.166; 1.L.172.169; 1.L.172.172; 1.L.172.175;
1.L.172.240; 1.L.172.244; 1.L.175.228; 1.L.175.229; 1.L.175.230;
1.L.175.231; 1.L.175.236; 1.L.175.237; 1.L.175.238; 1.L.175.239;
1.L.175.154; 1.L.175.157; 1.L.175.166; 1.L.175.169; 1.L.175.172;
1.L.175.175; 1.L.175.240; 1.L.175.244; 1.L.240.228; 1.L.240.229;
1.L.240.230; 1.L.240.231; 1.L.240.236; 1.L.240.237; 1.L.240.238;
1.L.240.239; 1.L.240.154; 1.L.240.157; 1.L.240.166; 1.L.240.169;
1.L.240.172; 1.L.240.175; 1.L.240.240; 1.L.240.244; 1.L.244.228;
1.L.244.229; 1.L.244.230; 1.L.244.231; 1.L.244.236; 1.L.244.237;
1.L.244.238; 1.L.244.239; 1.L.244.154; 1.L.244.157; 1.L.244.166;
1.L.244.169; 1.L.244.172; 1.L.244.175; 1.L.244.240; 1.L.244.244;
Prodrugs of 1.O 1.O.228.228; 1.O.228.229; 1.O.228.230; 1.O.228.231;
1.O.228.236; 1.O.228.237; 1.O.228.238; 1.O.228.239; 1.O.228.154;
1.O.228.157; 1.O.228.166; 1.O.228.169; 1.O.228.172; 1.O.228.175;
1.O.228.240; 1.O.228.244; 1.O.229.228; 1.O.229.229; 1.O.229.230;
1.O.229.231; 1.O.229.236; 1.O.229.237; 1.O.229.238; 1.O.229.239;
1.O.229.154; 1.O.229.157; 1.O.229.166; 1.O.229.169; 1.O.229.172;
1.O.229.175; 1.O.229.240; 1.O.229.244; 1.O.230.228; 1.O.230.229;
1.O.230.230; 1.O.230.231; 1.O.230.236; 1.O.230.237; 1.O.230.238;
1.O.230.239; 1.O.230.154; 1.O.230.157; 1.O.230.166; 1.O.230.169;
1.O.230.172; 1.O.230.175; 1.O.230.240; 1.O.230.244; 1.O.231.228;
1.O.231.229; 1.O.231.230; 1.O.231.231; 1.O.231.236; 1.O.231.237;
1.O.231.238; 1.O.231.239; 1.O.231.154; 1.O.231.157; 1.O.231.166;
1.O.231.169; 1.O.231.172; 1.O.231.175; 1.O.231.240; 1.O.231.244;
1.O.236.228; 1.O.236.229; 1.O.236.230; 1.O.236.231; 1.O.236.236;
1.O.236.237; 1.O.236.238; 1.O.236.239; 1.O.236.154; 1.O.236.157;
1.O.236.166; 1.O.236.169; 1.O.236.172; 1.O.236.175; 1.O.236.240;
1.O.236.244; 1.O.237.228; 1.O.237.229; 1.O.237.230; 1.O.237.231;
1.O.237.236; 1.O.237.237; 1.O.237.238; 1.O.237.239; 1.O.237.154;
1.O.237.157; 1.O.237.166; 1.O.237.169; 1.O.237.172; 1.O.237.175;
1.O.237.240; 1.O.237.244; 1.O.238.228; 1.O.238.229; 1.O.238.230;
1.O.238.231; 1.O.238.236; 1.O.238.237; 1.O.238.238; 1.O.238.239;
1.O.238.154; 1.O.238.157; 1.O.238.166; 1.O.238.169; 1.O.238.172;
1.O.238.175; 1.O.238.240; 1.O.238.244; 1.O.239.228; 1.O.239.229;
1.O.239.230; 1.O.239.231; 1.O.239.236; 1.O.239.237; 1.O.239.238;
1.O.239.239; 1.O.239.154; 1.O.239.157; 1.O.239.166; 1.O.239.169;
1.O.239.172; 1.O.239.175; 1.O.239.240; 1.O.239.244; 1.O.154.228;
1.O.154.229; 1.O.154.230; 1.O.154.231; 1.O.154.236; 1.O.154.237;
1.O.154.238; 1.O.154.239; 1.O.154.154; 1.O.154.157; 1.O.154.166;
1.O.154.169; 1.O.154.172; 1.O.154.175; 1.O.154.240; 1.O.154.244;
1.O.157.228; 1.O.157.229; 1.O.157.230; 1.O.157.231; 1.O.157.236;
1.O.157.237; 1.O.157.238; 1.O.157.239; 1.O.157.154; 1.O.157.157;
1.O.157.166; 1.O.157.169; 1.O.157.172; 1.O.157.175; 1.O.157.240;
1.O.157.244; 1.O.166.228; 1.O.166.229; 1.O.166.230; 1.O.166.231;
1.O.166.236; 1.O.166.237; 1.O.166.238; 1.O.166.239; 1.O.166.154;
1.O.166.157; 1.O.166.166; 1.O.166.169; 1.O.166.172; 1.O.166.175;
1.O.166.240; 1.O.166.244; 1.O.169.228; 1.O.169.229; 1.O.169.230;
1.O.169.231; 1.O.169.236; 1.O.169.237; 1.O.169.238; 1.O.169.239;
1.O.169.154; 1.O.169.157; 1.O.169.166; 1.O.169.169; 1.O.169.172;
1.O.169.175; 1.O.169.240; 1.O.169.244; 1.O.172.228; 1.O.172.229;
1.O.172.230; 1.O.172.231; 1.O.172.236; 1.O.172.237; 1.O.172.238;
1.O.172.239; 1.O.172.154; 1.O.172.157; 1.O.172.166; 1.O.172.169;
1.O.172.172; 1.O.172.175; 1.O.172.240; 1.O.172.244; 1.O.175.228;
1.O.175.229; 1.O.175.230; 1.O.175.231; 1.O.175.236; 1.O.175.237;
1.O.175.238; 1.O.175.239; 1.O.175.154; 1.O.175.157; 1.O.175.166;
1.O.175.169; 1.O.175.172; 1.O.175.175; 1.O.175.240; 1.O.175.244;
1.O.240.228; 1.O.240.229; 1.O.240.230; 1.O.240.231; 1.O.240.236;
1.O.240.237; 1.O.240.238; 1.O.240.239; 1.O.240.154; 1.O.240.157;
1.O.240.166; 1.O.240.169; 1.O.240.172; 1.O.240.175; 1.O.240.240;
1.O.240.244; 1.O.244.228; 1.O.244.229; 1.O.244.230; 1.O.244.231;
1.O.244.236; 1.O.244.237; 1.O.244.238; 1.O.244.239; 1.O.244.154;
1.O.244.157; 1.O.244.166; 1.O.244.169; 1.O.244.172; 1.O.244.175;
1.O.244.240; 1.O.244.244; Prodrugs of 1.P 1.P.228.228; 1.P.228.229;
1.P.228.230; 1.P.228.231; 1.P.228.236; 1.P.228.237; 1.P.228.238;
1.P.228.239; 1.P.228.154; 1.P.228.157; 1.P.228.166; 1.P.228.169;
1.P.228.172; 1.P.228.175; 1.P.228.240; 1.P.228.244; 1.P.229.228;
1.P.229.229; 1.P.229.230; 1.P.229.231; 1.P.229.236; 1.P.229.237;
1.P.229.238; 1.P.229.239; 1.P.229.154; 1.P.229.157; 1.P.229.166;
1.P.229.169; 1.P.229.172; 1.P.229.175; 1.P.229.240; 1.P.229.244;
1.P.230.228; 1.P.230.229; 1.P.230.230; 1.P.230.231; 1.P.230.236;
1.P.230.237; 1.P.230.238; 1.P.230.239; 1.P.230.154; 1.P.230.157;
1.P.230.166; 1.P.230.169; 1.P.230.172; 1.P.230.175; 1.P.230.240;
1.P.230.244; 1.P.231.228; 1.P.231.229; 1.P.231.230; 1.P.231.231;
1.P.231.236; 1.P.231.237; 1.P.231.238; 1.P.231.239; 1.P.231.154;
1.P.231.157; 1.P.231.166; 1.P.231.169; 1.P.231.172; 1.P.231.175;
1.P.231.240; 1.P.231.244; 1.P.236.228; 1.P.236.229; 1.P.236.230;
1.P.236.231; 1.P.236.236; 1.P.236.237; 1.P.236.238; 1.P.236.239;
1.P.236.154; 1.P.236.157; 1.P.236.166; 1.P.236.169; 1.P.236.172;
1.P.236.175; 1.P.236.240; 1.P.236.244; 1.P.237.228; 1.P.237.229;
1.P.237.230; 1.P.237.231; 1.P.237.236; 1.P.237.237; 1.P.237.238;
1.P.237.239; 1.P.237.154; 1.P.237.157; 1.P.237.166; 1.P.237.169;
1.P.237.172; 1.P.237.175; 1.P.237.240; 1.P.237.244; 1.P.238.228;
1.P.238.229; 1.P.238.230; 1.P.238.231; 1.P.238.236; 1.P.238.237;
1.P.238.238; 1.P.238.239; 1.P.238.154; 1.P.238.157; 1.P.238.166;
1.P.238.169; 1.P.238.172; 1.P.238.175; 1.P.238.240; 1.P.238.244;
1.P.239.228; 1.P.239.229; 1.P.239.230; 1.P.239.231; 1.P.239.236;
1.P.239.237; 1.P.239.238; 1.P.239.239; 1.P.239.154; 1.P.239.157;
1.P.239.166; 1.P.239.169; 1.P.239.172; 1.P.239.175; 1.P.239.240;
1.P.239.244; 1.P.154.228; 1.P.154.229; 1.P.154.230; 1.P.154.231;
1.P.154.236; 1.P.154.237; 1.P.154.238; 1.P.154.239; 1.P.154.154;
1.P.154.157; 1.P.154.166; 1.P.154.169; 1.P.154.172; 1.P.154.175;
1.P.154.240; 1.P.154.244; 1.P.157.228; 1.P.157.229; 1.P.157.230;
1.P.157.231; 1.P.157.236; 1.P.157.237; 1.P.157.238; 1.P.157.239;
1.P.157.154; 1.P.157.157; 1.P.157.166; 1.P.157.169; 1.P.157.172;
1.P.157.175; 1.P.157.240; 1.P.157.244; 1.P.166.228; 1.P.166.229;
1.P.166.230; 1.P.166.231; 1.P.166.236; 1.P.166.237; 1.P.166.238;
1.P.166.239; 1.P.166.154; 1.P.166.157; 1.P.166.166; 1.P.166.169;
1.P.166.172; 1.P.166.175; 1.P.166.240; 1.P.166.244; 1.P.169.228;
1.P.169.229; 1.P.169.230; 1.P.169.231; 1.P.169.236; 1.P.169.237;
1.P.169.238; 1.P.169.239; 1.P.169.154; 1.P.169.157; 1.P.169.166;
1.P.169.169; 1.P.169.172; 1.P.169.175; 1.P.169.240; 1.P.169.244;
1.P.172.228; 1.P.172.229; 1.P.172.230; 1.P.172.231; 1.P.172.236;
1.P.172.237; 1.P.172.238; 1.P.172.239; 1.P.172.154; 1.P.172.157;
1.P.172.166; 1.P.172.169; 1.P.172.172; 1.P.172.175; 1.P.172.240;
1.P.172.244; 1.P.175.228; 1.P.175.229; 1.P.175.230; 1.P.175.231;
1.P.175.236; 1.P.175.237; 1.P.175.238; 1.P.175.239; 1.P.175.154;
1.P.175.157; 1.P.175.166; 1.P.175.169; 1.P.175.172; 1.P.175.175;
1.P.175.240; 1.P.175.244; 1.P.240.228; 1.P.240.229; 1.P.240.230;
1.P.240.231; 1.P.240.236; 1.P.240.237; 1.P.240.238; 1.P.240.239;
1.P.240.154; 1.P.240.157; 1.P.240.166; 1.P.240.169; 1.P.240.172;
1.P.240.175; 1.P.240.240; 1.P.240.244; 1.P.244.228; 1.P.244.229;
1.P.244.230; 1.P.244.231; 1.P.244.236; 1.P.244.237; 1.P.244.238;
1.P.244.239; 1.P.244.154; 1.P.244.157; 1.P.244.166; 1.P.244.169;
1.P.244.172; 1.P.244.175; 1.P.244.240; 1.P.244.244; Prodrugs of 1.U
1.U.228.228; 1.U.228.229; 1.U.228.230; 1.U.228.231; 1.U.228.236;
1.U.228.237; 1.U.228.238; 1.U.228.239; 1.U.228.154; 1.U.228.157;
1.U.228.166; 1.U.228.169; 1.U.228.172; 1.U.228.175; 1.U.228.240;
1.U.228.244; 1.U.229.228; 1.U.229.229; 1.U.229.230; 1.U.229.231;
1.U.229.236; 1.U.229.237; 1.U.229.238; 1.U.229.239; 1.U.229.154;
1.U.229.157; 1.U.229.166; 1.U.229.169; 1.U.229.172; 1.U.229.175;
1.U.229.240; 1.U.229.244; 1.U.230.228; 1.U.230.229; 1.U.230.230;
1.U.230.231; 1.U.230.236; 1.U.230.237; 1.U.230.238; 1.U.230.239;
1.U.230.154; 1.U.230.157; 1.U.230.166; 1.U.230.169; 1.U.230.172;
1.U.230.175; 1.U.230.240; 1.U.230.244; 1.U.231.228; 1.U.231.229;
1.U.231.230; 1.U.231.231; 1.U.231.236; 1.U.231.237; 1.U.231.238;
1.U.231.239; 1.U.231.154; 1.U.231.157; 1.U.231.166; 1.U.231.169;
1.U.231.172; 1.U.231.175; 1.U.231.240; 1.U.231.244; 1.U.236.228;
1.U.236.229; 1.U.236.230; 1.U.236.231; 1.U.236.236; 1.U.236.237;
1.U.236.238; 1.U.236.239; 1.U.236.154; 1.U.236.157; 1.U.236.166;
1.U.236.169; 1.U.236.172; 1.U.236.175; 1.U.236.240; 1.U.236.244;
1.U.237.228; 1.U.237.229; 1.U.237.230; 1.U.237.231; 1.U.237.236;
1.U.237.237; 1.U.237.238; 1.U.237.239; 1.U.237.154; 1.U.237.157;
1.U.237.166; 1.U.237.169; 1.U.237.172; 1.U.237.175; 1.U.237.240;
1.U.237.244; 1.U.238.228; 1.U.238.229; 1.U.238.230; 1.U.238.231;
1.U.238.236; 1.U.238.237; 1.U.238.238; 1.U.238.239;
1.U.238.154;
1.U.238.157; 1.U.238.166; 1.U.238.169; 1.U.238.172; 1.U.238.175;
1.U.238.240; 1.U.238.244; 1.U.239.228; 1.U.239.229; 1.U.239.230;
1.U.239.231; 1.U.239.236; 1.U.239.237; 1.U.239.238; 1.U.239.239;
1.U.239.154; 1.U.239.157; 1.U.239.166; 1.U.239.169; 1.U.239.172;
1.U.239.175; 1.U.239.240; 1.U.239.244; 1.U.154.228; 1.U.154.229;
1.U.154.230; 1.U.154.231; 1.U.154.236; 1.U.154.237; 1.U.154.238;
1.U.154.239; 1.U.154.154; 1.U.154.157; 1.U.154.166; 1.U.154.169;
1.U.154.172; 1.U.154.175; 1.U.154.240; 1.U.154.244; 1.U.157.228;
1.U.157.229; 1.U.157.230; 1.U.157.231; 1.U.157.236; 1.U.157.237;
1.U.157.238; 1.U.157.239; 1.U.157.154; 1.U.157.157; 1.U.157.166;
1.U.157.169; 1.U.157.172; 1.U.157.175; 1.U.157.240; 1.U.157.244;
1.U.166.228; 1.U.166.229; 1.U.166.230; 1.U.166.231; 1.U.166.236;
1.U.166.237; 1.U.166.238; 1.U.166.239; 1.U.166.154; 1.U.166.157;
1.U.166.166; 1.U.166.169; 1.U.166.172; 1.U.166.175; 1.U.166.240;
1.U.166.244; 1.U.169.228; 1.U.169.229; 1.U.169.230; 1.U.169.231;
1.U.169.236; 1.U.169.237; 1.U.169.238; 1.U.169.239; 1.U.169.154;
1.U.169.157; 1.U.169.166; 1.U.169.169; 1.U.169.172; 1.U.169.175;
1.U.169.240; 1.U.169.244; 1.U.172.228; 1.U.172.229; 1.U.172.230;
1.U.172.231; 1.U.172.236; 1.U.172.237; 1.U.172.238; 1.U.172.239;
1.U.172.154; 1.U.172.157; 1.U.172.166; 1.U.172.169; 1.U.172.172;
1.U.172.175; 1.U.172.240; 1.U.172.244; 1.U.175.228; 1.U.175.229;
1.U.175.230; 1.U.175.231; 1.U.175.236; 1.U.175.237; 1.U.175.238;
1.U.175.239; 1.U.175.154; 1.U.175.157; 1.U.175.166; 1.U.175.169;
1.U.175.172; 1.U.175.175; 1.U.175.240; 1.U.175.244; 1.U.240.228;
1.U.240.229; 1.U.240.230; 1.U.240.231; 1.U.240.236; 1.U.240.237;
1.U.240.238; 1.U.240.239; 1.U.240.154; 1.U.240.157; 1.U.240.166;
1.U.240.169; 1.U.240.172; 1.U.240.175; 1.U.240.240; 1.U.240.244;
1.U.244.228; 1.U.244.229; 1.U.244.230; 1.U.244.231; 1.U.244.236;
1.U.244.237; 1.U.244.238; 1.U.244.239; 1.U.244.154; 1.U.244.157;
1.U.244.166; 1.U.244.169; 1.U.244.172; 1.U.244.175; 1.U.244.240;
1.U.244.244; Prodrugs of 1.W 1.W.228.228; 1.W.228.229; 1.W.228.230;
1.W.228.231; 1.W.228.236; 1.W.228.237; 1.W.228.238; 1.W.228.239;
1.W.228.154; 1.W.228.157; 1.W.228.166; 1.W.228.169; 1.W.228.172;
1.W.228.175; 1.W.228.240; 1.W.228.244; 1.W.229.228; 1.W.229.229;
1.W.229.230; 1.W.229.231; 1.W.229.236; 1.W.229.237; 1.W.229.238;
1.W.229.239; 1.W.229.154; 1.W.229.157; 1.W.229.166; 1.W.229.169;
1.W.229.172; 1.W.229.175; 1.W.229.240; 1.W.229.244; 1.W.230.228;
1.W.230.229; 1.W.230.230; 1.W.230.231; 1.W.230.236; 1.W.230.237;
1.W.230.238; 1.W.230.239; 1.W.230.154; 1.W.230.157; 1.W.230.166;
1.W.230.169; 1.W.230.172; 1.W.230.175; 1.W.230.240; 1.W.230.244;
1.W.231.228; 1.W.231.229; 1.W.231.230; 1.W.231.231; 1.W.231.236;
1.W.231.237; 1.W.231.238; 1.W.231.239; 1.W.231.154; 1.W.231.157;
1.W.231.166; 1.W.231.169; 1.W.231.172; 1.W.231.175; 1.W.231.240;
1.W.231.244; 1.W.236.228; 1.W.236.229; 1.W.236.230; 1.W.236.231;
1.W.236.236; 1.W.236.237; 1.W.236.238; 1.W.236.239; 1.W.236.154;
1.W.236.157; 1.W.236.166; 1.W.236.169; 1.W.236.172; 1.W.236.175;
1.W.236.240; 1.W.236.244; 1.W.237.228; 1.W.237.229; 1.W.237.230;
1.W.237.231; 1.W.237.236; 1.W.237.237; 1.W.237.238; 1.W.237.239;
1.W.237.154; 1.W.237.157; 1.W.237.166; 1.W.237.169; 1.W.237.172;
1.W.237.175; 1.W.237.240; 1.W.237.244; 1.W.238.228; 1.W.238.229;
1.W.238.230; 1.W.238.231; 1.W.238.236; 1.W.238.237; 1.W.238.238;
1.W.238.239; 1.W.238.154; 1.W.238.157; 1.W.238.166; 1.W.238.169;
1.W.238.172; 1.W.238.175; 1.W.238.240; 1.W.238.244; 1.W.239.228;
1.W.239.229; 1.W.239.230; 1.W.239.231; 1.W.239.236; 1.W.239.237;
1.W.239.238; 1.W.239.239; 1.W.239.154; 1.W.239.157; 1.W.239.166;
1.W.239.169; 1.W.239.172; 1.W.239.175; 1.W.239.240; 1.W.239.244;
1.W.154.228; 1.W.154.229; 1.W.154.230; 1.W.154.231; 1.W.154.236;
1.W.154.237; 1.W.154.238; 1.W.154.239; 1.W.154.154; 1.W.154.157;
1.W.154.166; 1.W.154.169; 1.W.154.172; 1.W.154.175; 1.W.154.240;
1.W.154.244; 1.W.157.228; 1.W.157.229; 1.W.157.230; 1.W.157.231;
1.W.157.236; 1.W.157.237; 1.W.157.238; 1.W.157.239; 1.W.157.154;
1.W.157.157; 1.W.157.166; 1.W.157.169; 1.W.157.172; 1.W.157.175;
1.W.157.240; 1.W.157.244; 1.W.166.228; 1.W.166.229; 1.W.166.230;
1.W.166.231; 1.W.166.236; 1.W.166.237; 1.W.166.238; 1.W.166.239;
1.W.166.154; 1.W.166.157; 1.W.166.166; 1.W.166.169; 1.W.166.172;
1.W.166.175; 1.W.166.240; 1.W.166.244; 1.W.169.228; 1.W.169.229;
1.W.169.230; 1.W.169.231; 1.W.169.236; 1.W.169.237; 1.W.169.238;
1.W.169.239; 1.W.169.154; 1.W.169.157; 1.W.169.166; 1.W.169.169;
1.W.169.172; 1.W.169.175; 1.W.169.240; 1.W.169.244; 1.W.172.228;
1.W.172.229; 1.W.172.230; 1.W.172.231; 1.W.172.236; 1.W.172.237;
1.W.172.238; 1.W.172.239; 1.W.172.154; 1.W.172.157; 1.W.172.166;
1.W.172.169; 1.W.172.172; 1.W.172.175; 1.W.172.240; 1.W.172.244;
1.W.175.228; 1.W.175.229; 1.W.175.230; 1.W.175.231; 1.W.175.236;
1.W.175.237; 1.W.175.238; 1.W.175.239; 1.W.175.154; 1.W.175.157;
1.W.175.166; 1.W.175.169; 1.W.175.172; 1.W.175.175; 1.W.175.240;
1.W.175.244; 1.W.240.228; 1.W.240.229; 1.W.240.230; 1.W.240.231;
1.W.240.236; 1.W.240.237; 1.W.240.238; 1.W.240.239; 1.W.240.154;
1.W.240.157; 1.W.240.166; 1.W.240.169; 1.W.240.172; 1.W.240.175;
1.W.240.240; 1.W.240.244; 1.W.244.228; 1.W.244.229; 1.W.244.230;
1.W.244.231; 1.W.244.236; 1.W.244.237; 1.W.244.238; 1.W.244.239;
1.W.244.154; 1.W.244.157; 1.W.244.166; 1.W.244.169; 1.W.244.172;
1.W.244.175; 1.W.244.240; 1.W.244.244; Prodrugs of 1.Y 1.Y.228.228;
1.Y.228.229; 1.Y.228.230; 1.Y.228.231; 1.Y.228.236; 1.Y.228.237;
1.Y.228.238; 1.Y.228.239; 1.Y.228.154; 1.Y.228.157; 1.Y.228.166;
1.Y.228.169; 1.Y.228.172; 1.Y.228.175; 1.Y.228.240; 1.Y.228.244;
1.Y.229.228; 1.Y.229.229; 1.Y.229.230; 1.Y.229.231; 1.Y.229.236;
1.Y.229.237; 1.Y.229.238; 1.Y.229.239; 1.Y.229.154; 1.Y.229.157;
1.Y.229.166; 1.Y.229.169; 1.Y.229.172; 1.Y.229.175; 1.Y.229.240;
1.Y.229.244; 1.Y.230.228; 1.Y.230.229; 1.Y.230.230; 1.Y.230.231;
1.Y.230.236; 1.Y.230.237; 1.Y.230.238; 1.Y.230.239; 1.Y.230.154;
1.Y.230.157; 1.Y.230.166; 1.Y.230.169; 1.Y.230.172; 1.Y.230.175;
1.Y.230.240; 1.Y.230.244; 1.Y.231.228; 1.Y.231.229; 1.Y.231.230;
1.Y.231.231; 1.Y.231.236; 1.Y.231.237; 1.Y.231.238; 1.Y.231.239;
1.Y.231.154; 1.Y.231.157; 1.Y.231.166; 1.Y.231.169; 1.Y.231.172;
1.Y.231.175; 1.Y.231.240; 1.Y.231.244; 1.Y.236.228; 1.Y.236.229;
1.Y.236.230; 1.Y.236.231; 1.Y.236.236; 1.Y.236.237; 1.Y.236.238;
1.Y.236.239; 1.Y.236.154; 1.Y.236.157; 1.Y.236.166; 1.Y.236.169;
1.Y.236.172; 1.Y.236.175; 1.Y.236.240; 1.Y.236.244; 1.Y.237.228;
1.Y.237.229; 1.Y.237.230; 1.Y.237.231; 1.Y.237.236; 1.Y.237.237;
1.Y.237.238; 1.Y.237.239; 1.Y.237.154; 1.Y.237.157; 1.Y.237.166;
1.Y.237.169; 1.Y.237.172; 1.Y.237.175; 1.Y.237.240; 1.Y.237.244;
1.Y.238.228; 1.Y.238.229; 1.Y.238.230; 1.Y.238.231; 1.Y.238.236;
1.Y.238.237; 1.Y.238.238; 1.Y.238.239; 1.Y.238.154; 1.Y.238.157;
1.Y.238.166; 1.Y.238.169; 1.Y.238.172; 1.Y.238.175; 1.Y.238.240;
1.Y.238.244; 1.Y.239.228; 1.Y.239.229; 1.Y.239.230; 1.Y.239.231;
1.Y.239.236; 1.Y.239.237; 1.Y.239.238; 1.Y.239.239; 1.Y.239.154;
1.Y.239.157; 1.Y.239.166; 1.Y.239.169; 1.Y.239.172; 1.Y.239.175;
1.Y.239.240; 1.Y.239.244; 1.Y.154.228; 1.Y.154.229; 1.Y.154.230;
1.Y.154.231; 1.Y.154.236; 1.Y.154.237; 1.Y.154.238; 1.Y.154.239;
1.Y.154.154; 1.Y.154.157; 1.Y.154.166; 1.Y.154.169; 1.Y.154.172;
1.Y.154.175; 1.Y.154.240; 1.Y.154.244; 1.Y.157.228; 1.Y.157.229;
1.Y.157.230; 1.Y.157.231; 1.Y.157.236; 1.Y.157.237; 1.Y.157.238;
1.Y.157.239; 1.Y.157.154; 1.Y.157.157; 1.Y.157.166; 1.Y.157.169;
1.Y.157.172; 1.Y.157.175; 1.Y.157.240; 1.Y.157.244; 1.Y.166.228;
1.Y.166.229; 1.Y.166.230; 1.Y.166.231; 1.Y.166.236; 1.Y.166.237;
1.Y.166.238; 1.Y.166.239; 1.Y.166.154; 1.Y.166.157; 1.Y.166.166;
1.Y.166.169; 1.Y.166.172; 1.Y.166.175; 1.Y.166.240; 1.Y.166.244;
1.Y.169.228; 1.Y.169.229; 1.Y.169.230; 1.Y.169.231; 1.Y.169.236;
1.Y.169.237; 1.Y.169.238; 1.Y.169.239; 1.Y.169.154; 1.Y.169.157;
1.Y.169.166; 1.Y.169.169; 1.Y.169.172; 1.Y.169.175; 1.Y.169.240;
1.Y.169.244; 1.Y.172.228; 1.Y.172.229; 1.Y.172.230; 1.Y.172.231;
1.Y.172.236; 1.Y.172.237; 1.Y.172.238; 1.Y.172.239; 1.Y.172.154;
1.Y.172.157; 1.Y.172.166; 1.Y.172.169; 1.Y.172.172; 1.Y.172.175;
1.Y.172.240; 1.Y.172.244; 1.Y.175.228; 1.Y.175.229; 1.Y.175.230;
1.Y.175.231; 1.Y.175.236; 1.Y.175.237; 1.Y.175.238; 1.Y.175.239;
1.Y.175.154; 1.Y.175.157; 1.Y.175.166; 1.Y.175.169; 1.Y.175.172;
1.Y.175.175; 1.Y.175.240; 1.Y.175.244; 1.Y.240.228; 1.Y.240.229;
1.Y.240.230; 1.Y.240.231; 1.Y.240.236; 1.Y.240.237; 1.Y.240.238;
1.Y.240.239; 1.Y.240.154; 1.Y.240.157; 1.Y.240.166; 1.Y.240.169;
1.Y.240.172; 1.Y.240.175; 1.Y.240.240; 1.Y.240.244; 1.Y.244.228;
1.Y.244.229; 1.Y.244.230; 1.Y.244.231; 1.Y.244.236; 1.Y.244.237;
1.Y.244.238; 1.Y.244.239; 1.Y.244.154; 1.Y.244.157; 1.Y.244.166;
1.Y.244.169; 1.Y.244.172; 1.Y.244.175; 1.Y.244.240; 1.Y.244.244;
Prodrugs of 2.B 2.B.228.228; 2.B.228.229; 2.B.228.230; 2.B.228.231;
2.B.228.236; 2.B.228.237; 2.B.228.238; 2.B.228.239; 2.B.228.154;
2.B.228.157; 2.B.228.166; 2.B.228.169; 2.B.228.172; 2.B.228.175;
2.B.228.240; 2.B.228.244; 2.B.229.228; 2.B.229.229; 2.B.229.230;
2.B.229.231; 2.B.229.236; 2.B.229.237; 2.B.229.238; 2.B.229.239;
2.B.229.154; 2.B.229.157; 2.B.229.166; 2.B.229.169; 2.B.229.172;
2.B.229.175; 2.B.229.240; 2.B.229.244; 2.B.230.228; 2.B.230.229;
2.B.230.230; 2.B.230.231; 2.B.230.236; 2.B.230.237; 2.B.230.238;
2.B.230.239; 2.B.230.154; 2.B.230.157; 2.B.230.166; 2.B.230.169;
2.B.230.172; 2.B.230.175; 2.B.230.240; 2.B.230.244; 2.B.231.228;
2.B.231.229; 2.B.231.230; 2.B.231.231; 2.B.231.236; 2.B.231.237;
2.B.231.238; 2.B.231.239; 2.B.231.154; 2.B.231.157; 2.B.231.166;
2.B.231.169; 2.B.231.172; 2.B.231.175; 2.B.231.240; 2.B.231.244;
2.B.236.228; 2.B.236.229; 2.B.236.230; 2.B.236.231; 2.B.236.236;
2.B.236.237; 2.B.236.238; 2.B.236.239; 2.B.236.154; 2.B.236.157;
2.B.236.166; 2.B.236.169; 2.B.236.172; 2.B.236.175; 2.B.236.240;
2.B.236.244; 2.B.237.228; 2.B.237.229; 2.B.237.230; 2.B.237.231;
2.B.237.236; 2.B.237.237; 2.B.237.238; 2.B.237.239; 2.B.237.154;
2.B.237.157; 2.B.237.166; 2.B.237.169; 2.B.237.172; 2.B.237.175;
2.B.237.240; 2.B.237.244; 2.B.238.228; 2.B.238.229; 2.B.238.230;
2.B.238.231; 2.B.238.236; 2.B.238.237; 2.B.238.238; 2.B.238.239;
2.B.238.154; 2.B.238.157; 2.B.238.166; 2.B.238.169; 2.B.238.172;
2.B.238.175; 2.B.238.240; 2.B.238.244; 2.B.239.228; 2.B.239.229;
2.B.239.230; 2.B.239.231; 2.B.239.236; 2.B.239.237; 2.B.239.238;
2.B.239.239; 2.B.239.154; 2.B.239.157; 2.B.239.166; 2.B.239.169;
2.B.239.172; 2.B.239.175; 2.B.239.240; 2.B.239.244; 2.B.154.228;
2.B.154.229; 2.B.154.230; 2.B.154.231; 2.B.154.236; 2.B.154.237;
2.B.154.238; 2.B.154.239; 2.B.154.154; 2.B.154.157; 2.B.154.166;
2.B.154.169; 2.B.154.172; 2.B.154.175; 2.B.154.240; 2.B.154.244;
2.B.157.228; 2.B.157.229; 2.B.157.230; 2.B.157.231; 2.B.157.236;
2.B.157.237; 2.B.157.238; 2.B.157.239; 2.B.157.154; 2.B.157.157;
2.B.157.166; 2.B.157.169; 2.B.157.172; 2.B.157.175; 2.B.157.240;
2.B.157.244; 2.B.166.228; 2.B.166.229; 2.B.166.230; 2.B.166.231;
2.B.166.236; 2.B.166.237; 2.B.166.238; 2.B.166.239; 2.B.166.154;
2.B.166.157; 2.B.166.166; 2.B.166.169; 2.B.166.172; 2.B.166.175;
2.B.166.240; 2.B.166.244; 2.B.169.228; 2.B.169.229; 2.B.169.230;
2.B.169.231; 2.B.169.236; 2.B.169.237; 2.B.169.238; 2.B.169.239;
2.B.169.154; 2.B.169.157; 2.B.169.166; 2.B.169.169; 2.B.169.172;
2.B.169.175; 2.B.169.240; 2.B.169.244; 2.B.172.228; 2.B.172.229;
2.B.172.230; 2.B.172.231; 2.B.172.236; 2.B.172.237; 2.B.172.238;
2.B.172.239; 2.B.172.154; 2.B.172.157; 2.B.172.166; 2.B.172.169;
2.B.172.172; 2.B.172.175; 2.B.172.240; 2.B.172.244; 2.B.175.228;
2.B.175.229; 2.B.175.230; 2.B.175.231; 2.B.175.236; 2.B.175.237;
2.B.175.238; 2.B.175.239; 2.B.175.154; 2.B.175.157; 2.B.175.166;
2.B.175.169; 2.B.175.172; 2.B.175.175; 2.B.175.240; 2.B.175.244;
2.B.240.228; 2.B.240.229; 2.B.240.230; 2.B.240.231; 2.B.240.236;
2.B.240.237; 2.B.240.238; 2.B.240.239; 2.B.240.154; 2.B.240.157;
2.B.240.166; 2.B.240.169; 2.B.240.172; 2.B.240.175; 2.B.240.240;
2.B.240.244; 2.B.244.228; 2.B.244.229; 2.B.244.230; 2.B.244.231;
2.B.244.236; 2.B.244.237; 2.B.244.238; 2.B.244.239; 2.B.244.154;
2.B.244.157; 2.B.244.166; 2.B.244.169; 2.B.244.172; 2.B.244.175;
2.B.244.240; 2.B.244.244; Prodrugs of 2.D 2.D.228.228; 2.D.228.229;
2.D.228.230; 2.D.228.231; 2.D.228.236; 2.D.228.237; 2.D.228.238;
2.D.228.239; 2.D.228.154; 2.D.228.157; 2.D.228.166; 2.D.228.169;
2.D.228.172; 2.D.228.175; 2.D.228.240; 2.D.228.244; 2.D.229.228;
2.D.229.229; 2.D.229.230; 2.D.229.231; 2.D.229.236; 2.D.229.237;
2.D.229.238; 2.D.229.239; 2.D.229.154; 2.D.229.157; 2.D.229.166;
2.D.229.169; 2.D.229.172; 2.D.229.175; 2.D.229.240; 2.D.229.244;
2.D.230.228; 2.D.230.229; 2.D.230.230; 2.D.230.231; 2.D.230.236;
2.D.230.237; 2.D.230.238; 2.D.230.239; 2.D.230.154; 2.D.230.157;
2.D.230.166; 2.D.230.169; 2.D.230.172; 2.D.230.175; 2.D.230.240;
2.D.230.244; 2.D.231.228; 2.D.231.229; 2.D.231.230; 2.D.231.231;
2.D.231.236; 2.D.231.237; 2.D.231.238; 2.D.231.239; 2.D.231.154;
2.D.231.157; 2.D.231.166; 2.D.231.169; 2.D.231.172; 2.D.231.175;
2.D.231.240; 2.D.231.244; 2.D.236.228; 2.D.236.229; 2.D.236.230;
2.D.236.231; 2.D.236.236; 2.D.236.237; 2.D.236.238; 2.D.236.239;
2.D.236.154; 2.D.236.157; 2.D.236.166; 2.D.236.169; 2.D.236.172;
2.D.236.175; 2.D.236.240; 2.D.236.244; 2.D.237.228; 2.D.237.229;
2.D.237.230; 2.D.237.231; 2.D.237.236; 2.D.237.237; 2.D.237.238;
2.D.237.239; 2.D.237.154; 2.D.237.157; 2.D.237.166; 2.D.237.169;
2.D.237.172; 2.D.237.175; 2.D.237.240; 2.D.237.244; 2.D.238.228;
2.D.238.229; 2.D.238.230; 2.D.238.231; 2.D.238.236; 2.D.238.237;
2.D.238.238; 2.D.238.239; 2.D.238.154; 2.D.238.157; 2.D.238.166;
2.D.238.169; 2.D.238.172; 2.D.238.175; 2.D.238.240; 2.D.238.244;
2.D.239.228; 2.D.239.229; 2.D.239.230; 2.D.239.231; 2.D.239.236;
2.D.239.237; 2.D.239.238; 2.D.239.239; 2.D.239.154; 2.D.239.157;
2.D.239.166; 2.D.239.169; 2.D.239.172; 2.D.239.175; 2.D.239.240;
2.D.239.244; 2.D.154.228; 2.D.154.229; 2.D.154.230; 2.D.154.231;
2.D.154.236; 2.D.154.237; 2.D.154.238; 2.D.154.239; 2.D.154.154;
2.D.154.157; 2.D.154.166; 2.D.154.169; 2.D.154.172; 2.D.154.175;
2.D.154.240; 2.D.154.244; 2.D.157.228; 2.D.157.229; 2.D.157.230;
2.D.157.231; 2.D.157.236; 2.D.157.237; 2.D.157.238; 2.D.157.239;
2.D.157.154; 2.D.157.157; 2.D.157.166; 2.D.157.169; 2.D.157.172;
2.D.157.175; 2.D.157.240; 2.D.157.244; 2.D.166.228; 2.D.166.229;
2.D.166.230; 2.D.166.231; 2.D.166.236; 2.D.166.237; 2.D.166.238;
2.D.166.239; 2.D.166.154; 2.D.166.157; 2.D.166.166; 2.D.166.169;
2.D.166.172; 2.D.166.175; 2.D.166.240; 2.D.166.244; 2.D.169.228;
2.D.169.229; 2.D.169.230; 2.D.169.231; 2.D.169.236; 2.D.169.237;
2.D.169.238; 2.D.169.239; 2.D.169.154; 2.D.169.157; 2.D.169.166;
2.D.169.169; 2.D.169.172; 2.D.169.175; 2.D.169.240; 2.D.169.244;
2.D.172.228; 2.D.172.229; 2.D.172.230; 2.D.172.231; 2.D.172.236;
2.D.172.237; 2.D.172.238; 2.D.172.239; 2.D.172.154; 2.D.172.157;
2.D.172.166; 2.D.172.169; 2.D.172.172; 2.D.172.175; 2.D.172.240;
2.D.172.244; 2.D.175.228; 2.D.175.229; 2.D.175.230; 2.D.175.231;
2.D.175.236; 2.D.175.237; 2.D.175.238; 2.D.175.239; 2.D.175.154;
2.D.175.157; 2.D.175.166; 2.D.175.169; 2.D.175.172; 2.D.175.175;
2.D.175.240; 2.D.175.244; 2.D.240.228; 2.D.240.229; 2.D.240.230;
2.D.240.231; 2.D.240.236; 2.D.240.237; 2.D.240.238; 2.D.240.239;
2.D.240.154; 2.D.240.157; 2.D.240.166; 2.D.240.169; 2.D.240.172;
2.D.240.175; 2.D.240.240; 2.D.240.244; 2.D.244.228; 2.D.244.229;
2.D.244.230; 2.D.244.231; 2.D.244.236; 2.D.244.237; 2.D.244.238;
2.D.244.239; 2.D.244.154; 2.D.244.157; 2.D.244.166; 2.D.244.169;
2.D.244.172; 2.D.244.175; 2.D.244.240; 2.D.244.244; Prodrugs of 2.E
2.E.228.228; 2.E.228.229; 2.E.228.230; 2.E.228.231; 2.E.228.236;
2.E.228.237; 2.E.228.238; 2.E.228.239; 2.E.228.154; 2.E.228.157;
2.E.228.166; 2.E.228.169; 2.E.228.172; 2.E.228.175; 2.E.228.240;
2.E.228.244; 2.E.229.228; 2.E.229.229; 2.E.229.230; 2.E.229.231;
2.E.229.236; 2.E.229.237; 2.E.229.238; 2.E.229.239; 2.E.229.154;
2.E.229.157; 2.E.229.166; 2.E.229.169; 2.E.229.172; 2.E.229.175;
2.E.229.240; 2.E.229.244; 2.E.230.228; 2.E.230.229;
2.E.230.230;
2.E.230.231; 2.E.230.236; 2.E.230.237; 2.E.230.238; 2.E.230.239;
2.E.230.154; 2.E.230.157; 2.E.230.166; 2.E.230.169; 2.E.230.172;
2.E.230.175; 2.E.230.240; 2.E.230.244; 2.E.231.228; 2.E.231.229;
2.E.231.230; 2.E.231.231; 2.E.231.236; 2.E.231.237; 2.E.231.238;
2.E.231.239; 2.E.231.154; 2.E.231.157; 2.E.231.166; 2.E.231.169;
2.E.231.172; 2.E.231.175; 2.E.231.240; 2.E.231.244; 2.E.236.228;
2.E.236.229; 2.E.236.230; 2.E.236.231; 2.E.236.236; 2.E.236.237;
2.E.236.238; 2.E.236.239; 2.E.236.154; 2.E.236.157; 2.E.236.166;
2.E.236.169; 2.E.236.172; 2.E.236.175; 2.E.236.240; 2.E.236.244;
2.E.237.228; 2.E.237.229; 2.E.237.230; 2.E.237.231; 2.E.237.236;
2.E.237.237; 2.E.237.238; 2.E.237.239; 2.E.237.154; 2.E.237.157;
2.E.237.166; 2.E.237.169; 2.E.237.172; 2.E.237.175; 2.E.237.240;
2.E.237.244; 2.E.238.228; 2.E.238.229; 2.E.238.230; 2.E.238.231;
2.E.238.236; 2.E.238.237; 2.E.238.238; 2.E.238.239; 2.E.238.154;
2.E.238.157; 2.E.238.166; 2.E.238.169; 2.E.238.172; 2.E.238.175;
2.E.238.240; 2.E.238.244; 2.E.239.228; 2.E.239.229; 2.E.239.230;
2.E.239.231; 2.E.239.236; 2.E.239.237; 2.E.239.238; 2.E.239.239;
2.E.239.154; 2.E.239.157; 2.E.239.166; 2.E.239.169; 2.E.239.172;
2.E.239.175; 2.E.239.240; 2.E.239.244; 2.E.154.228; 2.E.154.229;
2.E.154.230; 2.E.154.231; 2.E.154.236; 2.E.154.237; 2.E.154.238;
2.E.154.239; 2.E.154.154; 2.E.154.157; 2.E.154.166; 2.E.154.169;
2.E.154.172; 2.E.154.175; 2.E.154.240; 2.E.154.244; 2.E.157.228;
2.E.157.229; 2.E.157.230; 2.E.157.231; 2.E.157.236; 2.E.157.237;
2.E.157.238; 2.E.157.239; 2.E.157.154; 2.E.157.157; 2.E.157.166;
2.E.157.169; 2.E.157.172; 2.E.157.175; 2.E.157.240; 2.E.157.244;
2.E.166.228; 2.E.166.229; 2.E.166.230; 2.E.166.231; 2.E.166.236;
2.E.166.237; 2.E.166.238; 2.E.166.239; 2.E.166.154; 2.E.166.157;
2.E.166.166; 2.E.166.169; 2.E.166.172; 2.E.166.175; 2.E.166.240;
2.E.166.244; 2.E.169.228; 2.E.169.229; 2.E.169.230; 2.E.169.231;
2.E.169.236; 2.E.169.237; 2.E.169.238; 2.E.169.239; 2.E.169.154;
2.E.169.157; 2.E.169.166; 2.E.169.169; 2.E.169.172; 2.E.169.175;
2.E.169.240; 2.E.169.244; 2.E.172.228; 2.E.172.229; 2.E.172.230;
2.E.172.231; 2.E.172.236; 2.E.172.237; 2.E.172.238; 2.E.172.239;
2.E.172.154; 2.E.172.157; 2.E.172.166; 2.E.172.169; 2.E.172.172;
2.E.172.175; 2.E.172.240; 2.E.172.244; 2.E.175.228; 2.E.175.229;
2.E.175.230; 2.E.175.231; 2.E.175.236; 2.E.175.237; 2.E.175.238;
2.E.175.239; 2.E.175.154; 2.E.175.157; 2.E.175.166; 2.E.175.169;
2.E.175.172; 2.E.175.175; 2.E.175.240; 2.E.175.244; 2.E.240.228;
2.E.240.229; 2.E.240.230; 2.E.240.231; 2.E.240.236; 2.E.240.237;
2.E.240.238; 2.E.240.239; 2.E.240.154; 2.E.240.157; 2.E.240.166;
2.E.240.169; 2.E.240.172; 2.E.240.175; 2.E.240.240; 2.E.240.244;
2.E.244.228; 2.E.244.229; 2.E.244.230; 2.E.244.231; 2.E.244.236;
2.E.244.237; 2.E.244.238; 2.E.244.239; 2.E.244.154; 2.E.244.157;
2.E.244.166; 2.E.244.169; 2.E.244.172; 2.E.244.175; 2.E.244.240;
2.E.244.244; Prodrugs of 2.G 2.G.228.228; 2.G.228.229; 2.G.228.230;
2.G.228.231; 2.G.228.236; 2.G.228.237; 2.G.228.238; 2.G.228.239;
2.G.228.154; 2.G.228.157; 2.G.228.166; 2.G.228.169; 2.G.228.172;
2.G.228.175; 2.G.228.240; 2.G.228.244; 2.G.229.228; 2.G.229.229;
2.G.229.230; 2.G.229.231; 2.G.229.236; 2.G.229.237; 2.G.229.238;
2.G.229.239; 2.G.229.154; 2.G.229.157; 2.G.229.166; 2.G.229.169;
2.G.229.172; 2.G.229.175; 2.G.229.240; 2.G.229.244; 2.G.230.228;
2.G.230.229; 2.G.230.230; 2.G.230.231; 2.G.230.236; 2.G.230.237;
2.G.230.238; 2.G.230.239; 2.G.230.154; 2.G.230.157; 2.G.230.166;
2.G.230.169; 2.G.230.172; 2.G.230.175; 2.G.230.240; 2.G.230.244;
2.G.231.228; 2.G.231.229; 2.G.231.230; 2.G.231.231; 2.G.231.236;
2.G.231.237; 2.G.231.238; 2.G.231.239; 2.G.231.154; 2.G.231.157;
2.G.231.166; 2.G.231.169; 2.G.231.172; 2.G.231.175; 2.G.231.240;
2.G.231.244; 2.G.236.228; 2.G.236.229; 2.G.236.230; 2.G.236.231;
2.G.236.236; 2.G.236.237; 2.G.236.238; 2.G.236.239; 2.G.236.154;
2.G.236.157; 2.G.236.166; 2.G.236.169; 2.G.236.172; 2.G.236.175;
2.G.236.240; 2.G.236.244; 2.G.237.228; 2.G.237.229; 2.G.237.230;
2.G.237.231; 2.G.237.236; 2.G.237.237; 2.G.237.238; 2.G.237.239;
2.G.237.154; 2.G.237.157; 2.G.237.166; 2.G.237.169; 2.G.237.172;
2.G.237.175; 2.G.237.240; 2.G.237.244; 2.G.238.228; 2.G.238.229;
2.G.238.230; 2.G.238.231; 2.G.238.236; 2.G.238.237; 2.G.238.238;
2.G.238.239; 2.G.238.154; 2.G.238.157; 2.G.238.166; 2.G.238.169;
2.G.238.172; 2.G.238.175; 2.G.238.240; 2.G.238.244; 2.G.239.228;
2.G.239.229; 2.G.239.230; 2.G.239.231; 2.G.239.236; 2.G.239.237;
2.G.239.238; 2.G.239.239; 2.G.239.154; 2.G.239.157; 2.G.239.166;
2.G.239.169; 2.G.239.172; 2.G.239.175; 2.G.239.240; 2.G.239.244;
2.G.154.228; 2.G.154.229; 2.G.154.230; 2.G.154.231; 2.G.154.236;
2.G.154.237; 2.G.154.238; 2.G.154.239; 2.G.154.154; 2.G.154.157;
2.G.154.166; 2.G.154.169; 2.G.154.172; 2.G.154.175; 2.G.154.240;
2.G.154.244; 2.G.157.228; 2.G.157.229; 2.G.157.230; 2.G.157.231;
2.G.157.236; 2.G.157.237; 2.G.157.238; 2.G.157.239; 2.G.157.154;
2.G.157.157; 2.G.157.166; 2.G.157.169; 2.G.157.172; 2.G.157.175;
2.G.157.240; 2.G.157.244; 2.G.166.228; 2.G.166.229; 2.G.166.230;
2.G.166.231; 2.G.166.236; 2.G.166.237; 2.G.166.238; 2.G.166.239;
2.G.166.154; 2.G.166.157; 2.G.166.166; 2.G.166.169; 2.G.166.172;
2.G.166.175; 2.G.166.240; 2.G.166.244; 2.G.169.228; 2.G.169.229;
2.G.169.230; 2.G.169.231; 2.G.169.236; 2.G.169.237; 2.G.169.238;
2.G.169.239; 2.G.169.154; 2.G.169.157; 2.G.169.166; 2.G.169.169;
2.G.169.172; 2.G.169.175; 2.G.169.240; 2.G.169.244; 2.G.172.228;
2.G.172.229; 2.G.172.230; 2.G.172.231; 2.G.172.236; 2.G.172.237;
2.G.172.238; 2.G.172.239; 2.G.172.154; 2.G.172.157; 2.G.172.166;
2.G.172.169; 2.G.172.172; 2.G.172.175; 2.G.172.240; 2.G.172.244;
2.G.175.228; 2.G.175.229; 2.G.175.230; 2.G.175.231; 2.G.175.236;
2.G.175.237; 2.G.175.238; 2.G.175.239; 2.G.175.154; 2.G.175.157;
2.G.175.166; 2.G.175.169; 2.G.175.172; 2.G.175.175; 2.G.175.240;
2.G.175.244; 2.G.240.228; 2.G.240.229; 2.G.240.230; 2.G.240.231;
2.G.240.236; 2.G.240.237; 2.G.240.238; 2.G.240.239; 2.G.240.154;
2.G.240.157; 2.G.240.166; 2.G.240.169; 2.G.240.172; 2.G.240.175;
2.G.240.240; 2.G.240.244; 2.G.244.228; 2.G.244.229; 2.G.244.230;
2.G.244.231; 2.G.244.236; 2.G.244.237; 2.G.244.238; 2.G.244.239;
2.G.244.154; 2.G.244.157; 2.G.244.166; 2.G.244.169; 2.G.244.172;
2.G.244.175; 2.G.244.240; 2.G.244.244; Prodrugs of 2.I 2.I.228.228;
2.I.228.229; 2.I.228.230; 2.I.228.231; 2.I.228.236; 2.I.228.237;
2.I.228.238; 2.I.228.239; 2.I.228.154; 2.I.228.157; 2.I.228.166;
2.I.228.169; 2.I.228.172; 2.I.228.175; 2.I.228.240; 2.I.228.244;
2.I.229.228; 2.I.229.229; 2.I.229.230; 2.I.229.231; 2.I.229.236;
2.I.229.237; 2.I.229.238; 2.I.229.239; 2.I.229.154; 2.I.229.157;
2.I.229.166; 2.I.229.169; 2.I.229.172; 2.I.229.175; 2.I.229.240;
2.I.229.244; 2.I.230.228; 2.I.230.229; 2.I.230.230; 2.I.230.231;
2.I.230.236; 2.I.230.237; 2.I.230.238; 2.I.230.239; 2.I.230.154;
2.I.230.157; 2.I.230.166; 2.I.230.169; 2.I.230.172; 2.I.230.175;
2.I.230.240; 2.I.230.244; 2.I.231.228; 2.I.231.229; 2.I.231.230;
2.I.231.231; 2.I.231.236; 2.I.231.237; 2.I.231.238; 2.I.231.239;
2.I.231.154; 2.I.231.157; 2.I.231.166; 2.I.231.169; 2.I.231.172;
2.I.231.175; 2.I.231.240; 2.I.231.244; 2.I.236.228; 2.I.236.229;
2.I.236.230; 2.I.236.231; 2.I.236.236; 2.I.236.237; 2.I.236.238;
2.I.236.239; 2.I.236.154; 2.I.236.157; 2.I.236.166; 2.I.236.169;
2.I.236.172; 2.I.236.175; 2.I.236.240; 2.I.236.244; 2.I.237.228;
2.I.237.229; 2.I.237.230; 2.I.237.231; 2.I.237.236; 2.I.237.237;
2.I.237.238; 2.I.237.239; 2.I.237.154; 2.I.237.157; 2.I.237.166;
2.I.237.169; 2.I.237.172; 2.I.237.175; 2.I.237.240; 2.I.237.244;
2.I.238.228; 2.I.238.229; 2.I.238.230; 2.I.238.231; 2.I.238.236;
2.I.238.237; 2.I.238.238; 2.I.238.239; 2.I.238.154; 2.I.238.157;
2.I.238.166; 2.I.238.169; 2.I.238.172; 2.I.238.175; 2.I.238.240;
2.I.238.244; 2.I.239.228; 2.I.239.229; 2.I.239.230; 2.I.239.231;
2.I.239.236; 2.I.239.237; 2.I.239.238; 2.I.239.239; 2.I.239.154;
2.I.239.157; 2.I.239.166; 2.I.239.169; 2.I.239.172; 2.I.239.175;
2.I.239.240; 2.I.239.244; 2.I.154.228; 2.I.154.229; 2.I.154.230;
2.I.154.231; 2.I.154.236; 2.I.154.237; 2.I.154.238; 2.I.154.239;
2.I.154.154; 2.I.154.157; 2.I.154.166; 2.I.154.169; 2.I.154.172;
2.I.154.175; 2.I.154.240; 2.I.154.244; 2.I.157.228; 2.I.157.229;
2.I.157.230; 2.I.157.231; 2.I.157.236; 2.I.157.237; 2.I.157.238;
2.I.157.239; 2.I.157.154; 2.I.157.157; 2.I.157.166; 2.I.157.169;
2.I.157.172; 2.I.157.175; 2.I.157.240; 2.I.157.244; 2.I.166.228;
2.I.166.229; 2.I.166.230; 2.I.166.231; 2.I.166.236; 2.I.166.237;
2.I.166.238; 2.I.166.239; 2.I.166.154; 2.I.166.157; 2.I.166.166;
2.I.166.169; 2.I.166.172; 2.I.166.175; 2.I.166.240; 2.I.166.244;
2.I.169.228; 2.I.169.229; 2.I.169.230; 2.I.169.231; 2.I.169.236;
2.I.169.237; 2.I.169.238; 2.I.169.239; 2.I.169.154; 2.I.169.157;
2.I.169.166; 2.I.169.169; 2.I.169.172; 2.I.169.175; 2.I.169.240;
2.I.169.244; 2.I.172.228; 2.I.172.229; 2.I.172.230; 2.I.172.231;
2.I.172.236; 2.I.172.237; 2.I.172.238; 2.I.172.239; 2.I.172.154;
2.I.172.157; 2.I.172.166; 2.I.172.169; 2.I.172.172; 2.I.172.175;
2.I.172.240; 2.I.172.244; 2.I.175.228; 2.I.175.229; 2.I.175.230;
2.I.175.231; 2.I.175.236; 2.I.175.237; 2.I.175.238; 2.I.175.239;
2.I.175.154; 2.I.175.157; 2.I.175.166; 2.I.175.169; 2.I.175.172;
2.I.175.175; 2.I.175.240; 2.I.175.244; 2.I.240.228; 2.I.240.229;
2.I.240.230; 2.I.240.231; 2.I.240.236; 2.I.240.237; 2.I.240.238;
2.I.240.239; 2.I.240.154; 2.I.240.157; 2.I.240.166; 2.I.240.169;
2.I.240.172; 2.I.240.175; 2.I.240.240; 2.I.240.244; 2.I.244.228;
2.I.244.229; 2.I.244.230; 2.I.244.231; 2.I.244.236; 2.I.244.237;
2.I.244.238; 2.I.244.239; 2.I.244.154; 2.I.244.157; 2.I.244.166;
2.I.244.169; 2.I.244.172; 2.I.244.175; 2.I.244.240; 2.I.244.244;
Prodrugs of 2.J 2.J.228.228; 2.J.228.229; 2.J.228.230; 2.J.228.231;
2.J.228.236; 2.J.228.237; 2.J.228.238; 2.J.228.239; 2.J.228.154;
2.J.228.157; 2.J.228.166; 2.J.228.169; 2.J.228.172; 2.J.228.175;
2.J.228.240; 2.J.228.244; 2.J.229.228; 2.J.229.229; 2.J.229.230;
2.J.229.231; 2.J.229.236; 2.J.229.237; 2.J.229.238; 2.J.229.239;
2.J.229.154; 2.J.229.157; 2.J.229.166; 2.J.229.169; 2.J.229.172;
2.J.229.175; 2.J.229.240; 2.J.229.244; 2.J.230.228; 2.J.230.229;
2.J.230.230; 2.J.230.231; 2.J.230.236; 2.J.230.237; 2.J.230.238;
2.J.230.239; 2.J.230.154; 2.J.230.157; 2.J.230.166; 2.J.230.169;
2.J.230.172; 2.J.230.175; 2.J.230.240; 2.J.230.244; 2.J.231.228;
2.J.231.229; 2.J.231.230; 2.J.231.231; 2.J.231.236; 2.J.231.237;
2.J.231.238; 2.J.231.239; 2.J.231.154; 2.J.231.157; 2.J.231.166;
2.J.231.169; 2.J.231.172; 2.J.231.175; 2.J.231.240; 2.J.231.244;
2.J.236.228; 2.J.236.229; 2.J.236.230; 2.J.236.231; 2.J.236.236;
2.J.236.237; 2.J.236.238; 2.J.236.239; 2.J.236.154; 2.J.236.157;
2.J.236.166; 2.J.236.169; 2.J.236.172; 2.J.236.175; 2.J.236.240;
2.J.236.244; 2.J.237.228; 2.J.237.229; 2.J.237.230; 2.J.237.231;
2.J.237.236; 2.J.237.237; 2.J.237.238; 2.J.237.239; 2.J.237.154;
2.J.237.157; 2.J.237.166; 2.J.237.169; 2.J.237.172; 2.J.237.175;
2.J.237.240; 2.J.237.244; 2.J.238.228; 2.J.238.229; 2.J.238.230;
2.J.238.231; 2.J.238.236; 2.J.238.237; 2.J.238.238; 2.J.238.239;
2.J.238.154; 2.J.238.157; 2.J.238.166; 2.J.238.169; 2.J.238.172;
2.J.238.175; 2.J.238.240; 2.J.238.244; 2.J.239.228; 2.J.239.229;
2.J.239.230; 2.J.239.231; 2.J.239.236; 2.J.239.237; 2.J.239.238;
2.J.239.239; 2.J.239.154; 2.J.239.157; 2.J.239.166; 2.J.239.169;
2.J.239.172; 2.J.239.175; 2.J.239.240; 2.J.239.244; 2.J.154.228;
2.J.154.229; 2.J.154.230; 2.J.154.231; 2.J.154.236; 2.J.154.237;
2.J.154.238; 2.J.154.239; 2.J.154.154; 2.J.154.157; 2.J.154.166;
2.J.154.169; 2.J.154.172; 2.J.154.175; 2.J.154.240; 2.J.154.244;
2.J.157.228; 2.J.157.229; 2.J.157.230; 2.J.157.231; 2.J.157.236;
2.J.157.237; 2.J.157.238; 2.J.157.239; 2.J.157.154; 2.J.157.157;
2.J.157.166; 2.J.157.169; 2.J.157.172; 2.J.157.175; 2.J.157.240;
2.J.157.244; 2.J.166.228; 2.J.166.229; 2.J.166.230; 2.J.166.231;
2.J.166.236; 2.J.166.237; 2.J.166.238; 2.J.166.239; 2.J.166.154;
2.J.166.157; 2.J.166.166; 2.J.166.169; 2.J.166.172; 2.J.166.175;
2.J.166.240; 2.J.166.244; 2.J.169.228; 2.J.169.229; 2.J.169.230;
2.J.169.231; 2.J.169.236; 2.J.169.237; 2.J.169.238; 2.J.169.239;
2.J.169.154; 2.J.169.157; 2.J.169.166; 2.J.169.169; 2.J.169.172;
2.J.169.175; 2.J.169.240; 2.J.169.244; 2.J.172.228; 2.J.172.229;
2.J.172.230; 2.J.172.231; 2.J.172.236; 2.J.172.237; 2.J.172.238;
2.J.172.239; 2.J.172.154; 2.J.172.157; 2.J.172.166; 2.J.172.169;
2.J.172.172; 2.J.172.175; 2.J.172.240; 2.J.172.244; 2.J.175.228;
2.J.175.229; 2.J.175.230; 2.J.175.231; 2.J.175.236; 2.J.175.237;
2.J.175.238; 2.J.175.239; 2.J.175.154; 2.J.175.157; 2.J.175.166;
2.J.175.169; 2.J.175.172; 2.J.175.175; 2.J.175.240; 2.J.175.244;
2.J.240.228; 2.J.240.229; 2.J.240.230; 2.J.240.231; 2.J.240.236;
2.J.240.237; 2.J.240.238; 2.J.240.239; 2.J.240.154; 2.J.240.157;
2.J.240.166; 2.J.240.169; 2.J.240.172; 2.J.240.175; 2.J.240.240;
2.J.240.244; 2.J.244.228; 2.J.244.229; 2.J.244.230; 2.J.244.231;
2.J.244.236; 2.J.244.237; 2.J.244.238; 2.J.244.239; 2.J.244.154;
2.J.244.157; 2.J.244.166; 2.J.244.169; 2.J.244.172; 2.J.244.175;
2.J.244.240; 2.J.244.244; Prodrugs of 2.L 2.L.228.228; 2.L.228.229;
2.L.228.230; 2.L.228.231; 2.L.228.236; 2.L.228.237; 2.L.228.238;
2.L.228.239; 2.L.228.154; 2.L.228.157; 2.L.228.166; 2.L.228.169;
2.L.228.172; 2.L.228.175; 2.L.228.240; 2.L.228.244; 2.L.229.228;
2.L.229.229; 2.L.229.230; 2.L.229.231; 2.L.229.236; 2.L.229.237;
2.L.229.238; 2.L.229.239; 2.L.229.154; 2.L.229.157; 2.L.229.166;
2.L.229.169; 2.L.229.172; 2.L.229.175; 2.L.229.240; 2.L.229.244;
2.L.230.228; 2.L.230.229; 2.L.230.230; 2.L.230.231; 2.L.230.236;
2.L.230.237; 2.L.230.238; 2.L.230.239; 2.L.230.154; 2.L.230.157;
2.L.230.166; 2.L.230.169; 2.L.230.172; 2.L.230.175; 2.L.230.240;
2.L.230.244; 2.L.231.228; 2.L.231.229; 2.L.231.230; 2.L.231.231;
2.L.231.236; 2.L.231.237; 2.L.231.238; 2.L.231.239; 2.L.231.154;
2.L.231.157; 2.L.231.166; 2.L.231.169; 2.L.231.172; 2.L.231.175;
2.L.231.240; 2.L.231.244; 2.L.236.228; 2.L.236.229; 2.L.236.230;
2.L.236.231; 2.L.236.236; 2.L.236.237; 2.L.236.238; 2.L.236.239;
2.L.236.154; 2.L.236.157; 2.L.236.166; 2.L.236.169; 2.L.236.172;
2.L.236.175; 2.L.236.240; 2.L.236.244; 2.L.237.228; 2.L.237.229;
2.L.237.230; 2.L.237.231; 2.L.237.236; 2.L.237.237; 2.L.237.238;
2.L.237.239; 2.L.237.154; 2.L.237.157; 2.L.237.166; 2.L.237.169;
2.L.237.172; 2.L.237.175; 2.L.237.240; 2.L.237.244; 2.L.238.228;
2.L.238.229; 2.L.238.230; 2.L.238.231; 2.L.238.236; 2.L.238.237;
2.L.238.238; 2.L.238.239; 2.L.238.154; 2.L.238.157; 2.L.238.166;
2.L.238.169; 2.L.238.172; 2.L.238.175; 2.L.238.240; 2.L.238.244;
2.L.239.228; 2.L.239.229; 2.L.239.230; 2.L.239.231; 2.L.239.236;
2.L.239.237; 2.L.239.238; 2.L.239.239; 2.L.239.154; 2.L.239.157;
2.L.239.166; 2.L.239.169; 2.L.239.172; 2.L.239.175; 2.L.239.240;
2.L.239.244; 2.L.154.228; 2.L.154.229; 2.L.154.230; 2.L.154.231;
2.L.154.236; 2.L.154.237; 2.L.154.238; 2.L.154.239; 2.L.154.154;
2.L.154.157; 2.L.154.166; 2.L.154.169; 2.L.154.172; 2.L.154.175;
2.L.154.240; 2.L.154.244; 2.L.157.228; 2.L.157.229; 2.L.157.230;
2.L.157.231; 2.L.157.236; 2.L.157.237; 2.L.157.238; 2.L.157.239;
2.L.157.154; 2.L.157.157; 2.L.157.166; 2.L.157.169; 2.L.157.172;
2.L.157.175; 2.L.157.240; 2.L.157.244; 2.L.166.228; 2.L.166.229;
2.L.166.230; 2.L.166.231; 2.L.166.236; 2.L.166.237; 2.L.166.238;
2.L.166.239; 2.L.166.154; 2.L.166.157; 2.L.166.166; 2.L.166.169;
2.L.166.172; 2.L.166.175; 2.L.166.240; 2.L.166.244; 2.L.169.228;
2.L.169.229; 2.L.169.230; 2.L.169.231; 2.L.169.236; 2.L.169.237;
2.L.169.238; 2.L.169.239; 2.L.169.154; 2.L.169.157; 2.L.169.166;
2.L.169.169; 2.L.169.172; 2.L.169.175; 2.L.169.240; 2.L.169.244;
2.L.172.228; 2.L.172.229; 2.L.172.230; 2.L.172.231; 2.L.172.236;
2.L.172.237; 2.L.172.238; 2.L.172.239; 2.L.172.154; 2.L.172.157;
2.L.172.166; 2.L.172.169; 2.L.172.172; 2.L.172.175; 2.L.172.240;
2.L.172.244; 2.L.175.228; 2.L.175.229; 2.L.175.230; 2.L.175.231;
2.L.175.236; 2.L.175.237; 2.L.175.238; 2.L.175.239; 2.L.175.154;
2.L.175.157; 2.L.175.166; 2.L.175.169; 2.L.175.172; 2.L.175.175;
2.L.175.240; 2.L.175.244; 2.L.240.228; 2.L.240.229; 2.L.240.230;
2.L.240.231; 2.L.240.236; 2.L.240.237;
2.L.240.238; 2.L.240.239; 2.L.240.154; 2.L.240.157; 2.L.240.166;
2.L.240.169; 2.L.240.172; 2.L.240.175; 2.L.240.240; 2.L.240.244;
2.L.244.228; 2.L.244.229; 2.L.244.230; 2.L.244.231; 2.L.244.236;
2.L.244.237; 2.L.244.238; 2.L.244.239; 2.L.244.154; 2.L.244.157;
2.L.244.166; 2.L.244.169; 2.L.244.172; 2.L.244.175; 2.L.244.240;
2.L.244.244; Prodrugs of 2.O 2.O.228.228; 2.O.228.229; 2.O.228.230;
2.O.228.231; 2.O.228.236; 2.O.228.237; 2.O.228.238; 2.O.228.239;
2.O.228.154; 2.O.228.157; 2.O.228.166; 2.O.228.169; 2.O.228.172;
2.O.228.175; 2.O.228.240; 2.O.228.244; 2.O.229.228; 2.O.229.229;
2.O.229.230; 2.O.229.231; 2.O.229.236; 2.O.229.237; 2.O.229.238;
2.O.229.239; 2.O.229.154; 2.O.229.157; 2.O.229.166; 2.O.229.169;
2.O.229.172; 2.O.229.175; 2.O.229.240; 2.O.229.244; 2.O.230.228;
2.O.230.229; 2.O.230.230; 2.O.230.231; 2.O.230.236; 2.O.230.237;
2.O.230.238; 2.O.230.239; 2.O.230.154; 2.O.230.157; 2.O.230.166;
2.O.230.169; 2.O.230.172; 2.O.230.175; 2.O.230.240; 2.O.230.244;
2.O.231.228; 2.O.231.229; 2.O.231.230; 2.O.231.231; 2.O.231.236;
2.O.231.237; 2.O.231.238; 2.O.231.239; 2.O.231.154; 2.O.231.157;
2.O.231.166; 2.O.231.169; 2.O.231.172; 2.O.231.175; 2.O.231.240;
2.O.231.244; 2.O.236.228; 2.O.236.229; 2.O.236.230; 2.O.236.231;
2.O.236.236; 2.O.236.237; 2.O.236.238; 2.O.236.239; 2.O.236.154;
2.O.236.157; 2.O.236.166; 2.O.236.169; 2.O.236.172; 2.O.236.175;
2.O.236.240; 2.O.236.244; 2.O.237.228; 2.O.237.229; 2.O.237.230;
2.O.237.231; 2.O.237.236; 2.O.237.237; 2.O.237.238; 2.O.237.239;
2.O.237.154; 2.O.237.157; 2.O.237.166; 2.O.237.169; 2.O.237.172;
2.O.237.175; 2.O.237.240; 2.O.237.244; 2.O.238.228; 2.O.238.229;
2.O.238.230; 2.O.238.231; 2.O.238.236; 2.O.238.237; 2.O.238.238;
2.O.238.239; 2.O.238.154; 2.O.238.157; 2.O.238.166; 2.O.238.169;
2.O.238.172; 2.O.238.175; 2.O.238.240; 2.O.238.244; 2.O.239.228;
2.O.239.229; 2.O.239.230; 2.O.239.231; 2.O.239.236; 2.O.239.237;
2.O.239.238; 2.O.239.239; 2.O.239.154; 2.O.239.157; 2.O.239.166;
2.O.239.169; 2.O.239.172; 2.O.239.175; 2.O.239.240; 2.O.239.244;
2.O.154.228; 2.O.154.229; 2.O.154.230; 2.O.154.231; 2.O.154.236;
2.O.154.237; 2.O.154.238; 2.O.154.239; 2.O.154.154; 2.O.154.157;
2.O.154.166; 2.O.154.169; 2.O.154.172; 2.O.154.175; 2.O.154.240;
2.O.154.244; 2.O.157.228; 2.O.157.229; 2.O.157.230; 2.O.157.231;
2.O.157.236; 2.O.157.237; 2.O.157.238; 2.O.157.239; 2.O.157.154;
2.O.157.157; 2.O.157.166; 2.O.157.169; 2.O.157.172; 2.O.157.175;
2.O.157.240; 2.O.157.244; 2.O.166.228; 2.O.166.229; 2.O.166.230;
2.O.166.231; 2.O.166.236; 2.O.166.237; 2.O.166.238; 2.O.166.239;
2.O.166.154; 2.O.166.157; 2.O.166.166; 2.O.166.169; 2.O.166.172;
2.O.166.175; 2.O.166.240; 2.O.166.244; 2.O.169.228; 2.O.169.229;
2.O.169.230; 2.O.169.231; 2.O.169.236; 2.O.169.237; 2.O.169.238;
2.O.169.239; 2.O.169.154; 2.O.169.157; 2.O.169.166; 2.O.169.169;
2.O.169.172; 2.O.169.175; 2.O.169.240; 2.O.169.244; 2.O.172.228;
2.O.172.229; 2.O.172.230; 2.O.172.231; 2.O.172.236; 2.O.172.237;
2.O.172.238; 2.O.172.239; 2.O.172.154; 2.O.172.157; 2.O.172.166;
2.O.172.169; 2.O.172.172; 2.O.172.175; 2.O.172.240; 2.O.172.244;
2.O.175.228; 2.O.175.229; 2.O.175.230; 2.O.175.231; 2.O.175.236;
2.O.175.237; 2.O.175.238; 2.O.175.239; 2.O.175.154; 2.O.175.157;
2.O.175.166; 2.O.175.169; 2.O.175.172; 2.O.175.175; 2.O.175.240;
2.O.175.244; 2.O.240.228; 2.O.240.229; 2.O.240.230; 2.O.240.231;
2.O.240.236; 2.O.240.237; 2.O.240.238; 2.O.240.239; 2.O.240.154;
2.O.240.157; 2.O.240.166; 2.O.240.169; 2.O.240.172; 2.O.240.175;
2.O.240.240; 2.O.240.244; 2.O.244.228; 2.O.244.229; 2.O.244.230;
2.O.244.231; 2.O.244.236; 2.O.244.237; 2.O.244.238; 2.O.244.239;
2.O.244.154; 2.O.244.157; 2.O.244.166; 2.O.244.169; 2.O.244.172;
2.O.244.175; 2.O.244.240; 2.O.244.244; Prodrugs of 2.P 2.P.228.228;
2.P.228.229; 2.P.228.230; 2.P.228.231; 2.P.228.236; 2.P.228.237;
2.P.228.238; 2.P.228.239; 2.P.228.154; 2.P.228.157; 2.P.228.166;
2.P.228.169; 2.P.228.172; 2.P.228.175; 2.P.228.240; 2.P.228.244;
2.P.229.228; 2.P.229.229; 2.P.229.230; 2.P.229.231; 2.P.229.236;
2.P.229.237; 2.P.229.238; 2.P.229.239; 2.P.229.154; 2.P.229.157;
2.P.229.166; 2.P.229.169; 2.P.229.172; 2.P.229.175; 2.P.229.240;
2.P.229.244; 2.P.230.228; 2.P.230.229; 2.P.230.230; 2.P.230.231;
2.P.230.236; 2.P.230.237; 2.P.230.238; 2.P.230.239; 2.P.230.154;
2.P.230.157; 2.P.230.166; 2.P.230.169; 2.P.230.172; 2.P.230.175;
2.P.230.240; 2.P.230.244; 2.P.231.228; 2.P.231.229; 2.P.231.230;
2.P.231.231; 2.P.231.236; 2.P.231.237; 2.P.231.238; 2.P.231.239;
2.P.231.154; 2.P.231.157; 2.P.231.166; 2.P.231.169; 2.P.231.172;
2.P.231.175; 2.P.231.240; 2.P.231.244; 2.P.236.228; 2.P.236.229;
2.P.236.230; 2.P.236.231; 2.P.236.236; 2.P.236.237; 2.P.236.238;
2.P.236.239; 2.P.236.154; 2.P.236.157; 2.P.236.166; 2.P.236.169;
2.P.236.172; 2.P.236.175; 2.P.236.240; 2.P.236.244; 2.P.237.228;
2.P.237.229; 2.P.237.230; 2.P.237.231; 2.P.237.236; 2.P.237.237;
2.P.237.238; 2.P.237.239; 2.P.237.154; 2.P.237.157; 2.P.237.166;
2.P.237.169; 2.P.237.172; 2.P.237.175; 2.P.237.240; 2.P.237.244;
2.P.238.228; 2.P.238.229; 2.P.238.230; 2.P.238.231; 2.P.238.236;
2.P.238.237; 2.P.238.238; 2.P.238.239; 2.P.238.154; 2.P.238.157;
2.P.238.166; 2.P.238.169; 2.P.238.172; 2.P.238.175; 2.P.238.240;
2.P.238.244; 2.P.239.228; 2.P.239.229; 2.P.239.230; 2.P.239.231;
2.P.239.236; 2.P.239.237; 2.P.239.238; 2.P.239.239; 2.P.239.154;
2.P.239.157; 2.P.239.166; 2.P.239.169; 2.P.239.172; 2.P.239.175;
2.P.239.240; 2.P.239.244; 2.P.154.228; 2.P.154.229; 2.P.154.230;
2.P.154.231; 2.P.154.236; 2.P.154.237; 2.P.154.238; 2.P.154.239;
2.P.154.154; 2.P.154.157; 2.P.154.166; 2.P.154.169; 2.P.154.172;
2.P.154.175; 2.P.154.240; 2.P.154.244; 2.P.157.228; 2.P.157.229;
2.P.157.230; 2.P.157.231; 2.P.157.236; 2.P.157.237; 2.P.157.238;
2.P.157.239; 2.P.157.154; 2.P.157.157; 2.P.157.166; 2.P.157.169;
2.P.157.172; 2.P.157.175; 2.P.157.240; 2.P.157.244; 2.P.166.228;
2.P.166.229; 2.P.166.230; 2.P.166.231; 2.P.166.236; 2.P.166.237;
2.P.166.238; 2.P.166.239; 2.P.166.154; 2.P.166.157; 2.P.166.166;
2.P.166.169; 2.P.166.172; 2.P.166.175; 2.P.166.240; 2.P.166.244;
2.P.169.228; 2.P.169.229; 2.P.169.230; 2.P.169.231; 2.P.169.236;
2.P.169.237; 2.P.169.238; 2.P.169.239; 2.P.169.154; 2.P.169.157;
2.P.169.166; 2.P.169.169; 2.P.169.172; 2.P.169.175; 2.P.169.240;
2.P.169.244; 2.P.172.228; 2.P.172.229; 2.P.172.230; 2.P.172.231;
2.P.172.236; 2.P.172.237; 2.P.172.238; 2.P.172.239; 2.P.172.154;
2.P.172.157; 2.P.172.166; 2.P.172.169; 2.P.172.172; 2.P.172.175;
2.P.172.240; 2.P.172.244; 2.P.175.228; 2.P.175.229; 2.P.175.230;
2.P.175.231; 2.P.175.236; 2.P.175.237; 2.P.175.238; 2.P.175.239;
2.P.175.154; 2.P.175.157; 2.P.175.166; 2.P.175.169; 2.P.175.172;
2.P.175.175; 2.P.175.240; 2.P.175.244; 2.P.240.228; 2.P.240.229;
2.P.240.230; 2.P.240.231; 2.P.240.236; 2.P.240.237; 2.P.240.238;
2.P.240.239; 2.P.240.154; 2.P.240.157; 2.P.240.166; 2.P.240.169;
2.P.240.172; 2.P.240.175; 2.P.240.240; 2.P.240.244; 2.P.244.228;
2.P.244.229; 2.P.244.230; 2.P.244.231; 2.P.244.236; 2.P.244.237;
2.P.244.238; 2.P.244.239; 2.P.244.154; 2.P.244.157; 2.P.244.166;
2.P.244.169; 2.P.244.172; 2.P.244.175; 2.P.244.240; 2.P.244.244;
Prodrugs of 2.U 2.U.228.228; 2.U.228.229; 2.U.228.230; 2.U.228.231;
2.U.228.236; 2.U.228.237; 2.U.228.238; 2.U.228.239; 2.U.228.154;
2.U.228.157; 2.U.228.166; 2.U.228.169; 2.U.228.172; 2.U.228.175;
2.U.228.240; 2.U.228.244; 2.U.229.228; 2.U.229.229; 2.U.229.230;
2.U.229.231; 2.U.229.236; 2.U.229.237; 2.U.229.238; 2.U.229.239;
2.U.229.154; 2.U.229.157; 2.U.229.166; 2.U.229.169; 2.U.229.172;
2.U.229.175; 2.U.229.240; 2.U.229.244; 2.U.230.228; 2.U.230.229;
2.U.230.230; 2.U.230.231; 2.U.230.236; 2.U.230.237; 2.U.230.238;
2.U.230.239; 2.U.230.154; 2.U.230.157; 2.U.230.166; 2.U.230.169;
2.U.230.172; 2.U.230.175; 2.U.230.240; 2.U.230.244; 2.U.231.228;
2.U.231.229; 2.U.231.230; 2.U.231.231; 2.U.231.236; 2.U.231.237;
2.U.231.238; 2.U.231.239; 2.U.231.154; 2.U.231.157; 2.U.231.166;
2.U.231.169; 2.U.231.172; 2.U.231.175; 2.U.231.240; 2.U.231.244;
2.U.236.228; 2.U.236.229; 2.U.236.230; 2.U.236.231; 2.U.236.236;
2.U.236.237; 2.U.236.238; 2.U.236.239; 2.U.236.154; 2.U.236.157;
2.U.236.166; 2.U.236.169; 2.U.236.172; 2.U.236.175; 2.U.236.240;
2.U.236.244; 2.U.237.228; 2.U.237.229; 2.U.237.230; 2.U.237.231;
2.U.237.236; 2.U.237.237; 2.U.237.238; 2.U.237.239; 2.U.237.154;
2.U.237.157; 2.U.237.166; 2.U.237.169; 2.U.237.172; 2.U.237.175;
2.U.237.240; 2.U.237.244; 2.U.238.228; 2.U.238.229; 2.U.238.230;
2.U.238.231; 2.U.238.236; 2.U.238.237; 2.U.238.238; 2.U.238.239;
2.U.238.154; 2.U.238.157; 2.U.238.166; 2.U.238.169; 2.U.238.172;
2.U.238.175; 2.U.238.240; 2.U.238.244; 2.U.239.228; 2.U.239.229;
2.U.239.230; 2.U.239.231; 2.U.239.236; 2.U.239.237; 2.U.239.238;
2.U.239.239; 2.U.239.154; 2.U.239.157; 2.U.239.166; 2.U.239.169;
2.U.239.172; 2.U.239.175; 2.U.239.240; 2.U.239.244; 2.U.154.228;
2.U.154.229; 2.U.154.230; 2.U.154.231; 2.U.154.236; 2.U.154.237;
2.U.154.238; 2.U.154.239; 2.U.154.154; 2.U.154.157; 2.U.154.166;
2.U.154.169; 2.U.154.172; 2.U.154.175; 2.U.154.240; 2.U.154.244;
2.U.157.228; 2.U.157.229; 2.U.157.230; 2.U.157.231; 2.U.157.236;
2.U.157.237; 2.U.157.238; 2.U.157.239; 2.U.157.154; 2.U.157.157;
2.U.157.166; 2.U.157.169; 2.U.157.172; 2.U.157.175; 2.U.157.240;
2.U.157.244; 2.U.166.228; 2.U.166.229; 2.U.166.230; 2.U.166.231;
2.U.166.236; 2.U.166.237; 2.U.166.238; 2.U.166.239; 2.U.166.154;
2.U.166.157; 2.U.166.166; 2.U.166.169; 2.U.166.172; 2.U.166.175;
2.U.166.240; 2.U.166.244; 2.U.169.228; 2.U.169.229; 2.U.169.230;
2.U.169.231; 2.U.169.236; 2.U.169.237; 2.U.169.238; 2.U.169.239;
2.U.169.154; 2.U.169.157; 2.U.169.166; 2.U.169.169; 2.U.169.172;
2.U.169.175; 2.U.169.240; 2.U.169.244; 2.U.172.228; 2.U.172.229;
2.U.172.230; 2.U.172.231; 2.U.172.236; 2.U.172.237; 2.U.172.238;
2.U.172.239; 2.U.172.154; 2.U.172.157; 2.U.172.166; 2.U.172.169;
2.U.172.172; 2.U.172.175; 2.U.172.240; 2.U.172.244; 2.U.175.228;
2.U.175.229; 2.U.175.230; 2.U.175.231; 2.U.175.236; 2.U.175.237;
2.U.175.238; 2.U.175.239; 2.U.175.154; 2.U.175.157; 2.U.175.166;
2.U.175.169; 2.U.175.172; 2.U.175.175; 2.U.175.240; 2.U.175.244;
2.U.240.228; 2.U.240.229; 2.U.240.230; 2.U.240.231; 2.U.240.236;
2.U.240.237; 2.U.240.238; 2.U.240.239; 2.U.240.154; 2.U.240.157;
2.U.240.166; 2.U.240.169; 2.U.240.172; 2.U.240.175; 2.U.240.240;
2.U.240.244; 2.U.244.228; 2.U.244.229; 2.U.244.230; 2.U.244.231;
2.U.244.236; 2.U.244.237; 2.U.244.238; 2.U.244.239; 2.U.244.154;
2.U.244.157; 2.U.244.166; 2.U.244.169; 2.U.244.172; 2.U.244.175;
2.U.244.240; 2.U.244.244; Prodrugs of 2.W 2.W.228.228; 2.W.228.229;
2.W.228.230; 2.W.228.231; 2.W.228.236; 2.W.228.237; 2.W.228.238;
2.W.228.239; 2.W.228.154; 2.W.228.157; 2.W.228.166; 2.W.228.169;
2.W.228.172; 2.W.228.175; 2.W.228.240; 2.W.228.244; 2.W.229.228;
2.W.229.229; 2.W.229.230; 2.W.229.231; 2.W.229.236; 2.W.229.237;
2.W.229.238; 2.W.229.239; 2.W.229.154; 2.W.229.157; 2.W.229.166;
2.W.229.169; 2.W.229.172; 2.W.229.175; 2.W.229.240; 2.W.229.244;
2.W.230.228; 2.W.230.229; 2.W.230.230; 2.W.230.231; 2.W.230.236;
2.W.230.237; 2.W.230.238; 2.W.230.239; 2.W.230.154; 2.W.230.157;
2.W.230.166; 2.W.230.169; 2.W.230.172; 2.W.230.175; 2.W.230.240;
2.W.230.244; 2.W.231.228; 2.W.231.229; 2.W.231.230; 2.W.231.231;
2.W.231.236; 2.W.231.237; 2.W.231.238; 2.W.231.239; 2.W.231.154;
2.W.231.157; 2.W.231.166; 2.W.231.169; 2.W.231.172; 2.W.231.175;
2.W.231.240; 2.W.231.244; 2.W.236.228; 2.W.236.229; 2.W.236.230;
2.W.236.231; 2.W.236.236; 2.W.236.237; 2.W.236.238; 2.W.236.239;
2.W.236.154; 2.W.236.157; 2.W.236.166; 2.W.236.169; 2.W.236.172;
2.W.236.175; 2.W.236.240; 2.W.236.244; 2.W.237.228; 2.W.237.229;
2.W.237.230; 2.W.237.231; 2.W.237.236; 2.W.237.237; 2.W.237.238;
2.W.237.239; 2.W.237.154; 2.W.237.157; 2.W.237.166; 2.W.237.169;
2.W.237.172; 2.W.237.175; 2.W.237.240; 2.W.237.244; 2.W.238.228;
2.W.238.229; 2.W.238.230; 2.W.238.231; 2.W.238.236; 2.W.238.237;
2.W.238.238; 2.W.238.239; 2.W.238.154; 2.W.238.157; 2.W.238.166;
2.W.238.169; 2.W.238.172; 2.W.238.175; 2.W.238.240; 2.W.238.244;
2.W.239.228; 2.W.239.229; 2.W.239.230; 2.W.239.231; 2.W.239.236;
2.W.239.237; 2.W.239.238; 2.W.239.239; 2.W.239.154; 2.W.239.157;
2.W.239.166; 2.W.239.169; 2.W.239.172; 2.W.239.175; 2.W.239.240;
2.W.239.244; 2.W.154.228; 2.W.154.229; 2.W.154.230; 2.W.154.231;
2.W.154.236; 2.W.154.237; 2.W.154.238; 2.W.154.239; 2.W.154.154;
2.W.154.157; 2.W.154.166; 2.W.154.169; 2.W.154.172; 2.W.154.175;
2.W.154.240; 2.W.154.244; 2.W.157.228; 2.W.157.229; 2.W.157.230;
2.W.157.231; 2.W.157.236; 2.W.157.237; 2.W.157.238; 2.W.157.239;
2.W.157.154; 2.W.157.157; 2.W.157.166; 2.W.157.169; 2.W.157.172;
2.W.157.175; 2.W.157.240; 2.W.157.244; 2.W.166.228; 2.W.166.229;
2.W.166.230; 2.W.166.231; 2.W.166.236; 2.W.166.237; 2.W.166.238;
2.W.166.239; 2.W.166.154; 2.W.166.157; 2.W.166.166; 2.W.166.169;
2.W.166.172; 2.W.166.175; 2.W.166.240; 2.W.166.244; 2.W.169.228;
2.W.169.229; 2.W.169.230; 2.W.169.231; 2.W.169.236; 2.W.169.237;
2.W.169.238; 2.W.169.239; 2.W.169.154; 2.W.169.157; 2.W.169.166;
2.W.169.169; 2.W.169.172; 2.W.169.175; 2.W.169.240; 2.W.169.244;
2.W.172.228; 2.W.172.229; 2.W.172.230; 2.W.172.231; 2.W.172.236;
2.W.172.237; 2.W.172.238; 2.W.172.239; 2.W.172.154; 2.W.172.157;
2.W.172.166; 2.W.172.169; 2.W.172.172; 2.W.172.175; 2.W.172.240;
2.W.172.244; 2.W.175.228; 2.W.175.229; 2.W.175.230; 2.W.175.231;
2.W.175.236; 2.W.175.237; 2.W.175.238; 2.W.175.239; 2.W.175.154;
2.W.175.157; 2.W.175.166; 2.W.175.169; 2.W.175.172; 2.W.175.175;
2.W.175.240; 2.W.175.244; 2.W.240.228; 2.W.240.229; 2.W.240.230;
2.W.240.231; 2.W.240.236; 2.W.240.237; 2.W.240.238; 2.W.240.239;
2.W.240.154; 2.W.240.157; 2.W.240.166; 2.W.240.169; 2.W.240.172;
2.W.240.175; 2.W.240.240; 2.W.240.244; 2.W.244.228; 2.W.244.229;
2.W.244.230; 2.W.244.231; 2.W.244.236; 2.W.244.237; 2.W.244.238;
2.W.244.239; 2.W.244.154; 2.W.244.157; 2.W.244.166; 2.W.244.169;
2.W.244.172; 2.W.244.175; 2.W.244.240; 2.W.244.244; Prodrugs of 2.Y
2.Y.228.228; 2.Y.228.229; 2.Y.228.230; 2.Y.228.231; 2.Y.228.236;
2.Y.228.237; 2.Y.228.238; 2.Y.228.239; 2.Y.228.154; 2.Y.228.157;
2.Y.228.166; 2.Y.228.169; 2.Y.228.172; 2.Y.228.175; 2.Y.228.240;
2.Y.228.244; 2.Y.229.228; 2.Y.229.229; 2.Y.229.230; 2.Y.229.231;
2.Y.229.236; 2.Y.229.237; 2.Y.229.238; 2.Y.229.239; 2.Y.229.154;
2.Y.229.157; 2.Y.229.166; 2.Y.229.169; 2.Y.229.172; 2.Y.229.175;
2.Y.229.240; 2.Y.229.244; 2.Y.230.228; 2.Y.230.229; 2.Y.230.230;
2.Y.230.231; 2.Y.230.236; 2.Y.230.237; 2.Y.230.238; 2.Y.230.239;
2.Y.230.154; 2.Y.230.157; 2.Y.230.166; 2.Y.230.169; 2.Y.230.172;
2.Y.230.175; 2.Y.230.240; 2.Y.230.244; 2.Y.231.228; 2.Y.231.229;
2.Y.231.230; 2.Y.231.231; 2.Y.231.236; 2.Y.231.237; 2.Y.231.238;
2.Y.231.239; 2.Y.231.154; 2.Y.231.157; 2.Y.231.166; 2.Y.231.169;
2.Y.231.172; 2.Y.231.175; 2.Y.231.240; 2.Y.231.244; 2.Y.236.228;
2.Y.236.229; 2.Y.236.230; 2.Y.236.231; 2.Y.236.236; 2.Y.236.237;
2.Y.236.238; 2.Y.236.239; 2.Y.236.154; 2.Y.236.157; 2.Y.236.166;
2.Y.236.169; 2.Y.236.172; 2.Y.236.175; 2.Y.236.240; 2.Y.236.244;
2.Y.237.228; 2.Y.237.229; 2.Y.237.230; 2.Y.237.231; 2.Y.237.236;
2.Y.237.237; 2.Y.237.238; 2.Y.237.239; 2.Y.237.154; 2.Y.237.157;
2.Y.237.166; 2.Y.237.169; 2.Y.237.172; 2.Y.237.175; 2.Y.237.240;
2.Y.237.244; 2.Y.238.228; 2.Y.238.229; 2.Y.238.230; 2.Y.238.231;
2.Y.238.236; 2.Y.238.237; 2.Y.238.238; 2.Y.238.239; 2.Y.238.154;
2.Y.238.157; 2.Y.238.166; 2.Y.238.169; 2.Y.238.172; 2.Y.238.175;
2.Y.238.240; 2.Y.238.244; 2.Y.239.228; 2.Y.239.229; 2.Y.239.230;
2.Y.239.231; 2.Y.239.236; 2.Y.239.237; 2.Y.239.238; 2.Y.239.239;
2.Y.239.154; 2.Y.239.157; 2.Y.239.166; 2.Y.239.169; 2.Y.239.172;
2.Y.239.175; 2.Y.239.240; 2.Y.239.244; 2.Y.154.228; 2.Y.154.229;
2.Y.154.230; 2.Y.154.231; 2.Y.154.236; 2.Y.154.237; 2.Y.154.238;
2.Y.154.239; 2.Y.154.154; 2.Y.154.157; 2.Y.154.166; 2.Y.154.169;
2.Y.154.172; 2.Y.154.175; 2.Y.154.240; 2.Y.154.244; 2.Y.157.228;
2.Y.157.229; 2.Y.157.230; 2.Y.157.231; 2.Y.157.236; 2.Y.157.237;
2.Y.157.238; 2.Y.157.239; 2.Y.157.154; 2.Y.157.157; 2.Y.157.166;
2.Y.157.169; 2.Y.157.172; 2.Y.157.175; 2.Y.157.240;
2.Y.157.244;
2.Y.166.228; 2.Y.166.229; 2.Y.166.230; 2.Y.166.231; 2.Y.166.236;
2.Y.166.237; 2.Y.166.238; 2.Y.166.239; 2.Y.166.154; 2.Y.166.157;
2.Y.166.166; 2.Y.166.169; 2.Y.166.172; 2.Y.166.175; 2.Y.166.240;
2.Y.166.244; 2.Y.169.228; 2.Y.169.229; 2.Y.169.230; 2.Y.169.231;
2.Y.169.236; 2.Y.169.237; 2.Y.169.238; 2.Y.169.239; 2.Y.169.154;
2.Y.169.157; 2.Y.169.166; 2.Y.169.169; 2.Y.169.172; 2.Y.169.175;
2.Y.169.240; 2.Y.169.244; 2.Y.172.228; 2.Y.172.229; 2.Y.172.230;
2.Y.172.231; 2.Y.172.236; 2.Y.172.237; 2.Y.172.238; 2.Y.172.239;
2.Y.172.154; 2.Y.172.157; 2.Y.172.166; 2.Y.172.169; 2.Y.172.172;
2.Y.172.175; 2.Y.172.240; 2.Y.172.244; 2.Y.175.228; 2.Y.175.229;
2.Y.175.230; 2.Y.175.231; 2.Y.175.236; 2.Y.175.237; 2.Y.175.238;
2.Y.175.239; 2.Y.175.154; 2.Y.175.157; 2.Y.175.166; 2.Y.175.169;
2.Y.175.172; 2.Y.175.175; 2.Y.175.240; 2.Y.175.244; 2.Y.240.228;
2.Y.240.229; 2.Y.240.230; 2.Y.240.231; 2.Y.240.236; 2.Y.240.237;
2.Y.240.238; 2.Y.240.239; 2.Y.240.154; 2.Y.240.157; 2.Y.240.166;
2.Y.240.169; 2.Y.240.172; 2.Y.240.175; 2.Y.240.240; 2.Y.240.244;
2.Y.244.228; 2.Y.244.229; 2.Y.244.230; 2.Y.244.231; 2.Y.244.236;
2.Y.244.237; 2.Y.244.238; 2.Y.244.239; 2.Y.244.154; 2.Y.244.157;
2.Y.244.166; 2.Y.244.169; 2.Y.244.172; 2.Y.244.175; 2.Y.244.240;
2.Y.244.244; Prodrugs of 3.B 3.B.228.228; 3.B.228.229; 3.B.228.230;
3.B.228.231; 3.B.228.236; 3.B.228.237; 3.B.228.238; 3.B.228.239;
3.B.228.154; 3.B.228.157; 3.B.228.166; 3.B.228.169; 3.B.228.172;
3.B.228.175; 3.B.228.240; 3.B.228.244; 3.B.229.228; 3.B.229.229;
3.B.229.230; 3.B.229.231; 3.B.229.236; 3.B.229.237; 3.B.229.238;
3.B.229.239; 3.B.229.154; 3.B.229.157; 3.B.229.166; 3.B.229.169;
3.B.229.172; 3.B.229.175; 3.B.229.240; 3.B.229.244; 3.B.230.228;
3.B.230.229; 3.B.230.230; 3.B.230.231; 3.B.230.236; 3.B.230.237;
3.B.230.238; 3.B.230.239; 3.B.230.154; 3.B.230.157; 3.B.230.166;
3.B.230.169; 3.B.230.172; 3.B.230.175; 3.B.230.240; 3.B.230.244;
3.B.231.228; 3.B.231.229; 3.B.231.230; 3.B.231.231; 3.B.231.236;
3.B.231.237; 3.B.231.238; 3.B.231.239; 3.B.231.154; 3.B.231.157;
3.B.231.166; 3.B.231.169; 3.B.231.172; 3.B.231.175; 3.B.231.240;
3.B.231.244; 3.B.236.228; 3.B.236.229; 3.B.236.230; 3.B.236.231;
3.B.236.236; 3.B.236.237; 3.B.236.238; 3.B.236.239; 3.B.236.154;
3.B.236.157; 3.B.236.166; 3.B.236.169; 3.B.236.172; 3.B.236.175;
3.B.236.240; 3.B.236.244; 3.B.237.228; 3.B.237.229; 3.B.237.230;
3.B.237.231; 3.B.237.236; 3.B.237.237; 3.B.237.238; 3.B.237.239;
3.B.237.154; 3.B.237.157; 3.B.237.166; 3.B.237.169; 3.B.237.172;
3.B.237.175; 3.B.237.240; 3.B.237.244; 3.B.238.228; 3.B.238.229;
3.B.238.230; 3.B.238.231; 3.B.238.236; 3.B.238.237; 3.B.238.238;
3.B.238.239; 3.B.238.154; 3.B.238.157; 3.B.238.166; 3.B.238.169;
3.B.238.172; 3.B.238.175; 3.B.238.240; 3.B.238.244; 3.B.239.228;
3.B.239.229; 3.B.239.230; 3.B.239.231; 3.B.239.236; 3.B.239.237;
3.B.239.238; 3.B.239.239; 3.B.239.154; 3.B.239.157; 3.B.239.166;
3.B.239.169; 3.B.239.172; 3.B.239.175; 3.B.239.240; 3.B.239.244;
3.B.154.228; 3.B.154.229; 3.B.154.230; 3.B.154.231; 3.B.154.236;
3.B.154.237; 3.B.154.238; 3.B.154.239; 3.B.154.154; 3.B.154.157;
3.B.154.166; 3.B.154.169; 3.B.154.172; 3.B.154.175; 3.B.154.240;
3.B.154.244; 3.B.157.228; 3.B.157.229; 3.B.157.230; 3.B.157.231;
3.B.157.236; 3.B.157.237; 3.B.157.238; 3.B.157.239; 3.B.157.154;
3.B.157.157; 3.B.157.166; 3.B.157.169; 3.B.157.172; 3.B.157.175;
3.B.157.240; 3.B.157.244; 3.B.166.228; 3.B.166.229; 3.B.166.230;
3.B.166.231; 3.B.166.236; 3.B.166.237; 3.B.166.238; 3.B.166.239;
3.B.166.154; 3.B.166.157; 3.B.166.166; 3.B.166.169; 3.B.166.172;
3.B.166.175; 3.B.166.240; 3.B.166.244; 3.B.169.228; 3.B.169.229;
3.B.169.230; 3.B.169.231; 3.B.169.236; 3.B.169.237; 3.B.169.238;
3.B.169.239; 3.B.169.154; 3.B.169.157; 3.B.169.166; 3.B.169.169;
3.B.169.172; 3.B.169.175; 3.B.169.240; 3.B.169.244; 3.B.172.228;
3.B.172.229; 3.B.172.230; 3.B.172.231; 3.B.172.236; 3.B.172.237;
3.B.172.238; 3.B.172.239; 3.B.172.154; 3.B.172.157; 3.B.172.166;
3.B.172.169; 3.B.172.172; 3.B.172.175; 3.B.172.240; 3.B.172.244;
3.B.175.228; 3.B.175.229; 3.B.175.230; 3.B.175.231; 3.B.175.236;
3.B.175.237; 3.B.175.238; 3.B.175.239; 3.B.175.154; 3.B.175.157;
3.B.175.166; 3.B.175.169; 3.B.175.172; 3.B.175.175; 3.B.175.240;
3.B.175.244; 3.B.240.228; 3.B.240.229; 3.B.240.230; 3.B.240.231;
3.B.240.236; 3.B.240.237; 3.B.240.238; 3.B.240.239; 3.B.240.154;
3.B.240.157; 3.B.240.166; 3.B.240.169; 3.B.240.172; 3.B.240.175;
3.B.240.240; 3.B.240.244; 3.B.244.228; 3.B.244.229; 3.B.244.230;
3.B.244.231; 3.B.244.236; 3.B.244.237; 3.B.244.238; 3.B.244.239;
3.B.244.154; 3.B.244.157; 3.B.244.166; 3.B.244.169; 3.B.244.172;
3.B.244.175; 3.B.244.240; 3.B.244.244; Prodrugs of 3.D 3.D.228.228;
3.D.228.229; 3.D.228.230; 3.D.228.231; 3.D.228.236; 3.D.228.237;
3.D.228.238; 3.D.228.239; 3.D.228.154; 3.D.228.157; 3.D.228.166;
3.D.228.169; 3.D.228.172; 3.D.228.175; 3.D.228.240; 3.D.228.244;
3.D.229.228; 3.D.229.229; 3.D.229.230; 3.D.229.231; 3.D.229.236;
3.D.229.237; 3.D.229.238; 3.D.229.239; 3.D.229.154; 3.D.229.157;
3.D.229.166; 3.D.229.169; 3.D.229.172; 3.D.229.175; 3.D.229.240;
3.D.229.244; 3.D.230.228; 3.D.230.229; 3.D.230.230; 3.D.230.231;
3.D.230.236; 3.D.230.237; 3.D.230.238; 3.D.230.239; 3.D.230.154;
3.D.230.157; 3.D.230.166; 3.D.230.169; 3.D.230.172; 3.D.230.175;
3.D.230.240; 3.D.230.244; 3.D.231.228; 3.D.231.229; 3.D.231.230;
3.D.231.231; 3.D.231.236; 3.D.231.237; 3.D.231.238; 3.D.231.239;
3.D.231.154; 3.D.231.157; 3.D.231.166; 3.D.231.169; 3.D.231.172;
3.D.231.175; 3.D.231.240; 3.D.231.244; 3.D.236.228; 3.D.236.229;
3.D.236.230; 3.D.236.231; 3.D.236.236; 3.D.236.237; 3.D.236.238;
3.D.236.239; 3.D.236.154; 3.D.236.157; 3.D.236.166; 3.D.236.169;
3.D.236.172; 3.D.236.175; 3.D.236.240; 3.D.236.244; 3.D.237.228;
3.D.237.229; 3.D.237.230; 3.D.237.231; 3.D.237.236; 3.D.237.237;
3.D.237.238; 3.D.237.239; 3.D.237.154; 3.D.237.157; 3.D.237.166;
3.D.237.169; 3.D.237.172; 3.D.237.175; 3.D.237.240; 3.D.237.244;
3.D.238.228; 3.D.238.229; 3.D.238.230; 3.D.238.231; 3.D.238.236;
3.D.238.237; 3.D.238.238; 3.D.238.239; 3.D.238.154; 3.D.238.157;
3.D.238.166; 3.D.238.169; 3.D.238.172; 3.D.238.175; 3.D.238.240;
3.D.238.244; 3.D.239.228; 3.D.239.229; 3.D.239.230; 3.D.239.231;
3.D.239.236; 3.D.239.237; 3.D.239.238; 3.D.239.239; 3.D.239.154;
3.D.239.157; 3.D.239.166; 3.D.239.169; 3.D.239.172; 3.D.239.175;
3.D.239.240; 3.D.239.244; 3.D.154.228; 3.D.154.229; 3.D.154.230;
3.D.154.231; 3.D.154.236; 3.D.154.237; 3.D.154.238; 3.D.154.239;
3.D.154.154; 3.D.154.157; 3.D.154.166; 3.D.154.169; 3.D.154.172;
3.D.154.175; 3.D.154.240; 3.D.154.244; 3.D.157.228; 3.D.157.229;
3.D.157.230; 3.D.157.231; 3.D.157.236; 3.D.157.237; 3.D.157.238;
3.D.157.239; 3.D.157.154; 3.D.157.157; 3.D.157.166; 3.D.157.169;
3.D.157.172; 3.D.157.175; 3.D.157.240; 3.D.157.244; 3.D.166.228;
3.D.166.229; 3.D.166.230; 3.D.166.231; 3.D.166.236; 3.D.166.237;
3.D.166.238; 3.D.166.239; 3.D.166.154; 3.D.166.157; 3.D.166.166;
3.D.166.169; 3.D.166.172; 3.D.166.175; 3.D.166.240; 3.D.166.244;
3.D.169.228; 3.D.169.229; 3.D.169.230; 3.D.169.231; 3.D.169.236;
3.D.169.237; 3.D.169.238; 3.D.169.239; 3.D.169.154; 3.D.169.157;
3.D.169.166; 3.D.169.169; 3.D.169.172; 3.D.169.175; 3.D.169.240;
3.D.169.244; 3.D.172.228; 3.D.172.229; 3.D.172.230; 3.D.172.231;
3.D.172.236; 3.D.172.237; 3.D.172.238; 3.D.172.239; 3.D.172.154;
3.D.172.157; 3.D.172.166; 3.D.172.169; 3.D.172.172; 3.D.172.175;
3.D.172.240; 3.D.172.244; 3.D.175.228; 3.D.175.229; 3.D.175.230;
3.D.175.231; 3.D.175.236; 3.D.175.237; 3.D.175.238; 3.D.175.239;
3.D.175.154; 3.D.175.157; 3.D.175.166; 3.D.175.169; 3.D.175.172;
3.D.175.175; 3.D.175.240; 3.D.175.244; 3.D.240.228; 3.D.240.229;
3.D.240.230; 3.D.240.231; 3.D.240.236; 3.D.240.237; 3.D.240.238;
3.D.240.239; 3.D.240.154; 3.D.240.157; 3.D.240.166; 3.D.240.169;
3.D.240.172; 3.D.240.175; 3.D.240.240; 3.D.240.244; 3.D.244.228;
3.D.244.229; 3.D.244.230; 3.D.244.231; 3.D.244.236; 3.D.244.237;
3.D.244.238; 3.D.244.239; 3.D.244.154; 3.D.244.157; 3.D.244.166;
3.D.244.169; 3.D.244.172; 3.D.244.175; 3.D.244.240; 3.D.244.244;
Prodrugs of 3.E 3.E.228.228; 3.E.228.229; 3.E.228.230; 3.E.228.231;
3.E.228.236; 3.E.228.237; 3.E.228.238; 3.E.228.239; 3.E.228.154;
3.E.228.157; 3.E.228.166; 3.E.228.169; 3.E.228.172; 3.E.228.175;
3.E.228.240; 3.E.228.244; 3.E.229.228; 3.E.229.229; 3.E.229.230;
3.E.229.231; 3.E.229.236; 3.E.229.237; 3.E.229.238; 3.E.229.239;
3.E.229.154; 3.E.229.157; 3.E.229.166; 3.E.229.169; 3.E.229.172;
3.E.229.175; 3.E.229.240; 3.E.229.244; 3.E.230.228; 3.E.230.229;
3.E.230.230; 3.E.230.231; 3.E.230.236; 3.E.230.237; 3.E.230.238;
3.E.230.239; 3.E.230.154; 3.E.230.157; 3.E.230.166; 3.E.230.169;
3.E.230.172; 3.E.230.175; 3.E.230.240; 3.E.230.244; 3.E.231.228;
3.E.231.229; 3.E.231.230; 3.E.231.231; 3.E.231.236; 3.E.231.237;
3.E.231.238; 3.E.231.239; 3.E.231.154; 3.E.231.157; 3.E.231.166;
3.E.231.169; 3.E.231.172; 3.E.231.175; 3.E.231.240; 3.E.231.244;
3.E.236.228; 3.E.236.229; 3.E.236.230; 3.E.236.231; 3.E.236.236;
3.E.236.237; 3.E.236.238; 3.E.236.239; 3.E.236.154; 3.E.236.157;
3.E.236.166; 3.E.236.169; 3.E.236.172; 3.E.236.175; 3.E.236.240;
3.E.236.244; 3.E.237.228; 3.E.237.229; 3.E.237.230; 3.E.237.231;
3.E.237.236; 3.E.237.237; 3.E.237.238; 3.E.237.239; 3.E.237.154;
3.E.237.157; 3.E.237.166; 3.E.237.169; 3.E.237.172; 3.E.237.175;
3.E.237.240; 3.E.237.244; 3.E.238.228; 3.E.238.229; 3.E.238.230;
3.E.238.231; 3.E.238.236; 3.E.238.237; 3.E.238.238; 3.E.238.239;
3.E.238.154; 3.E.238.157; 3.E.238.166; 3.E.238.169; 3.E.238.172;
3.E.238.175; 3.E.238.240; 3.E.238.244; 3.E.239.228; 3.E.239.229;
3.E.239.230; 3.E.239.231; 3.E.239.236; 3.E.239.237; 3.E.239.238;
3.E.239.239; 3.E.239.154; 3.E.239.157; 3.E.239.166; 3.E.239.169;
3.E.239.172; 3.E.239.175; 3.E.239.240; 3.E.239.244; 3.E.154.228;
3.E.154.229; 3.E.154.230; 3.E.154.231; 3.E.154.236; 3.E.154.237;
3.E.154.238; 3.E.154.239; 3.E.154.154; 3.E.154.157; 3.E.154.166;
3.E.154.169; 3.E.154.172; 3.E.154.175; 3.E.154.240; 3.E.154.244;
3.E.157.228; 3.E.157.229; 3.E.157.230; 3.E.157.231; 3.E.157.236;
3.E.157.237; 3.E.157.238; 3.E.157.239; 3.E.157.154; 3.E.157.157;
3.E.157.166; 3.E.157.169; 3.E.157.172; 3.E.157.175; 3.E.157.240;
3.E.157.244; 3.E.166.228; 3.E.166.229; 3.E.166.230; 3.E.166.231;
3.E.166.236; 3.E.166.237; 3.E.166.238; 3.E.166.239; 3.E.166.154;
3.E.166.157; 3.E.166.166; 3.E.166.169; 3.E.166.172; 3.E.166.175;
3.E.166.240; 3.E.166.244; 3.E.169.228; 3.E.169.229; 3.E.169.230;
3.E.169.231; 3.E.169.236; 3.E.169.237; 3.E.169.238; 3.E.169.239;
3.E.169.154; 3.E.169.157; 3.E.169.166; 3.E.169.169; 3.E.169.172;
3.E.169.175; 3.E.169.240; 3.E.169.244; 3.E.172.228; 3.E.172.229;
3.E.172.230; 3.E.172.231; 3.E.172.236; 3.E.172.237; 3.E.172.238;
3.E.172.239; 3.E.172.154; 3.E.172.157; 3.E.172.166; 3.E.172.169;
3.E.172.172; 3.E.172.175; 3.E.172.240; 3.E.172.244; 3.E.175.228;
3.E.175.229; 3.E.175.230; 3.E.175.231; 3.E.175.236; 3.E.175.237;
3.E.175.238; 3.E.175.239; 3.E.175.154; 3.E.175.157; 3.E.175.166;
3.E.175.169; 3.E.175.172; 3.E.175.175; 3.E.175.240; 3.E.175.244;
3.E.240.228; 3.E.240.229; 3.E.240.230; 3.E.240.231; 3.E.240.236;
3.E.240.237; 3.E.240.238; 3.E.240.239; 3.E.240.154; 3.E.240.157;
3.E.240.166; 3.E.240.169; 3.E.240.172; 3.E.240.175; 3.E.240.240;
3.E.240.244; 3.E.244.228; 3.E.244.229; 3.E.244.230; 3.E.244.231;
3.E.244.236; 3.E.244.237; 3.E.244.238; 3.E.244.239; 3.E.244.154;
3.E.244.157; 3.E.244.166; 3.E.244.169; 3.E.244.172; 3.E.244.175;
3.E.244.240; 3.E.244.244; Prodrugs of 3.G 3.G.228.228; 3.G.228.229;
3.G.228.230; 3.G.228.231; 3.G.228.236; 3.G.228.237; 3.G.228.238;
3.G.228.239; 3.G.228.154; 3.G.228.157; 3.G.228.166; 3.G.228.169;
3.G.228.172; 3.G.228.175; 3.G.228.240; 3.G.228.244; 3.G.229.228;
3.G.229.229; 3.G.229.230; 3.G.229.231; 3.G.229.236; 3.G.229.237;
3.G.229.238; 3.G.229.239; 3.G.229.154; 3.G.229.157; 3.G.229.166;
3.G.229.169; 3.G.229.172; 3.G.229.175; 3.G.229.240; 3.G.229.244;
3.G.230.228; 3.G.230.229; 3.G.230.230; 3.G.230.231; 3.G.230.236;
3.G.230.237; 3.G.230.238; 3.G.230.239; 3.G.230.154; 3.G.230.157;
3.G.230.166; 3.G.230.169; 3.G.230.172; 3.G.230.175; 3.G.230.240;
3.G.230.244; 3.G.231.228; 3.G.231.229; 3.G.231.230; 3.G.231.231;
3.G.231.236; 3.G.231.237; 3.G.231.238; 3.G.231.239; 3.G.231.154;
3.G.231.157; 3.G.231.166; 3.G.231.169; 3.G.231.172; 3.G.231.175;
3.G.231.240; 3.G.231.244; 3.G.236.228; 3.G.236.229; 3.G.236.230;
3.G.236.231; 3.G.236.236; 3.G.236.237; 3.G.236.238; 3.G.236.239;
3.G.236.154; 3.G.236.157; 3.G.236.166; 3.G.236.169; 3.G.236.172;
3.G.236.175; 3.G.236.240; 3.G.236.244; 3.G.237.228; 3.G.237.229;
3.G.237.230; 3.G.237.231; 3.G.237.236; 3.G.237.237; 3.G.237.238;
3.G.237.239; 3.G.237.154; 3.G.237.157; 3.G.237.166; 3.G.237.169;
3.G.237.172; 3.G.237.175; 3.G.237.240; 3.G.237.244; 3.G.238.228;
3.G.238.229; 3.G.238.230; 3.G.238.231; 3.G.238.236; 3.G.238.237;
3.G.238.238; 3.G.238.239; 3.G.238.154; 3.G.238.157; 3.G.238.166;
3.G.238.169; 3.G.238.172; 3.G.238.175; 3.G.238.240; 3.G.238.244;
3.G.239.228; 3.G.239.229; 3.G.239.230; 3.G.239.231; 3.G.239.236;
3.G.239.237; 3.G.239.238; 3.G.239.239; 3.G.239.154; 3.G.239.157;
3.G.239.166; 3.G.239.169; 3.G.239.172; 3.G.239.175; 3.G.239.240;
3.G.239.244; 3.G.154.228; 3.G.154.229; 3.G.154.230; 3.G.154.231;
3.G.154.236; 3.G.154.237; 3.G.154.238; 3.G.154.239; 3.G.154.154;
3.G.154.157; 3.G.154.166; 3.G.154.169; 3.G.154.172; 3.G.154.175;
3.G.154.240; 3.G.154.244; 3.G.157.228; 3.G.157.229; 3.G.157.230;
3.G.157.231; 3.G.157.236; 3.G.157.237; 3.G.157.238; 3.G.157.239;
3.G.157.154; 3.G.157.157; 3.G.157.166; 3.G.157.169; 3.G.157.172;
3.G.157.175; 3.G.157.240; 3.G.157.244; 3.G.166.228; 3.G.166.229;
3.G.166.230; 3.G.166.231; 3.G.166.236; 3.G.166.237; 3.G.166.238;
3.G.166.239; 3.G.166.154; 3.G.166.157; 3.G.166.166; 3.G.166.169;
3.G.166.172; 3.G.166.175; 3.G.166.240; 3.G.166.244; 3.G.169.228;
3.G.169.229; 3.G.169.230; 3.G.169.231; 3.G.169.236; 3.G.169.237;
3.G.169.238; 3.G.169.239; 3.G.169.154; 3.G.169.157; 3.G.169.166;
3.G.169.169; 3.G.169.172; 3.G.169.175; 3.G.169.240; 3.G.169.244;
3.G.172.228; 3.G.172.229; 3.G.172.230; 3.G.172.231; 3.G.172.236;
3.G.172.237; 3.G.172.238; 3.G.172.239; 3.G.172.154; 3.G.172.157;
3.G.172.166; 3.G.172.169; 3.G.172.172; 3.G.172.175; 3.G.172.240;
3.G.172.244; 3.G.175.228; 3.G.175.229; 3.G.175.230; 3.G.175.231;
3.G.175.236; 3.G.175.237; 3.G.175.238; 3.G.175.239; 3.G.175.154;
3.G.175.157; 3.G.175.166; 3.G.175.169; 3.G.175.172; 3.G.175.175;
3.G.175.240; 3.G.175.244; 3.G.240.228; 3.G.240.229; 3.G.240.230;
3.G.240.231; 3.G.240.236; 3.G.240.237; 3.G.240.238; 3.G.240.239;
3.G.240.154; 3.G.240.157; 3.G.240.166; 3.G.240.169; 3.G.240.172;
3.G.240.175; 3.G.240.240; 3.G.240.244; 3.G.244.228; 3.G.244.229;
3.G.244.230; 3.G.244.231; 3.G.244.236; 3.G.244.237; 3.G.244.238;
3.G.244.239; 3.G.244.154; 3.G.244.157; 3.G.244.166; 3.G.244.169;
3.G.244.172; 3.G.244.175; 3.G.244.240; 3.G.244.244; Prodrugs of 3.I
3.I.228.228; 3.I.228.229; 3.I.228.230; 3.I.228.231; 3.I.228.236;
3.I.228.237; 3.I.228.238; 3.I.228.239; 3.I.228.154; 3.I.228.157;
3.I.228.166; 3.I.228.169; 3.I.228.172; 3.I.228.175; 3.I.228.240;
3.I.228.244; 3.I.229.228; 3.I.229.229; 3.I.229.230; 3.I.229.231;
3.I.229.236; 3.I.229.237; 3.I.229.238; 3.I.229.239; 3.I.229.154;
3.I.229.157; 3.I.229.166; 3.I.229.169; 3.I.229.172; 3.I.229.175;
3.I.229.240; 3.I.229.244; 3.I.230.228; 3.I.230.229; 3.I.230.230;
3.I.230.231; 3.I.230.236; 3.I.230.237; 3.I.230.238; 3.I.230.239;
3.I.230.154; 3.I.230.157; 3.I.230.166; 3.I.230.169; 3.I.230.172;
3.I.230.175; 3.I.230.240; 3.I.230.244; 3.I.231.228; 3.I.231.229;
3.I.231.230; 3.I.231.231; 3.I.231.236; 3.I.231.237; 3.I.231.238;
3.I.231.239; 3.I.231.154; 3.I.231.157; 3.I.231.166; 3.I.231.169;
3.I.231.172; 3.I.231.175; 3.I.231.240; 3.I.231.244; 3.I.236.228;
3.I.236.229; 3.I.236.230; 3.I.236.231; 3.I.236.236; 3.I.236.237;
3.I.236.238; 3.I.236.239; 3.I.236.154; 3.I.236.157; 3.I.236.166;
3.I.236.169; 3.I.236.172; 3.I.236.175; 3.I.236.240; 3.I.236.244;
3.I.237.228; 3.I.237.229; 3.I.237.230; 3.I.237.231; 3.I.237.236;
3.I.237.237; 3.I.237.238; 3.I.237.239; 3.I.237.154;
3.I.237.157;
3.I.237.166; 3.I.237.169; 3.I.237.172; 3.I.237.175; 3.I.237.240;
3.I.237.244; 3.I.238.228; 3.I.238.229; 3.I.238.230; 3.I.238.231;
3.I.238.236; 3.I.238.237; 3.I.238.238; 3.I.238.239; 3.I.238.154;
3.I.238.157; 3.I.238.166; 3.I.238.169; 3.I.238.172; 3.I.238.175;
3.I.238.240; 3.I.238.244; 3.I.239.228; 3.I.239.229; 3.I.239.230;
3.I.239.231; 3.I.239.236; 3.I.239.237; 3.I.239.238; 3.I.239.239;
3.I.239.154; 3.I.239.157; 3.I.239.166; 3.I.239.169; 3.I.239.172;
3.I.239.175; 3.I.239.240; 3.I.239.244; 3.I.154.228; 3.I.154.229;
3.I.154.230; 3.I.154.231; 3.I.154.236; 3.I.154.237; 3.I.154.238;
3.I.154.239; 3.I.154.154; 3.I.154.157; 3.I.154.166; 3.I.154.169;
3.I.154.172; 3.I.154.175; 3.I.154.240; 3.I.154.244; 3.I.157.228;
3.I.157.229; 3.I.157.230; 3.I.157.231; 3.I.157.236; 3.I.157.237;
3.I.157.238; 3.I.157.239; 3.I.157.154; 3.I.157.157; 3.I.157.166;
3.I.157.169; 3.I.157.172; 3.I.157.175; 3.I.157.240; 3.I.157.244;
3.I.166.228; 3.I.166.229; 3.I.166.230; 3.I.166.231; 3.I.166.236;
3.I.166.237; 3.I.166.238; 3.I.166.239; 3.I.166.154; 3.I.166.157;
3.I.166.166; 3.I.166.169; 3.I.166.172; 3.I.166.175; 3.I.166.240;
3.I.166.244; 3.I.169.228; 3.I.169.229; 3.I.169.230; 3.I.169.231;
3.I.169.236; 3.I.169.237; 3.I.169.238; 3.I.169.239; 3.I.169.154;
3.I.169.157; 3.I.169.166; 3.I.169.169; 3.I.169.172; 3.I.169.175;
3.I.169.240; 3.I.169.244; 3.I.172.228; 3.I.172.229; 3.I.172.230;
3.I.172.231; 3.I.172.236; 3.I.172.237; 3.I.172.238; 3.I.172.239;
3.I.172.154; 3.I.172.157; 3.I.172.166; 3.I.172.169; 3.I.172.172;
3.I.172.175; 3.I.172.240; 3.I.172.244; 3.I.175.228; 3.I.175.229;
3.I.175.230; 3.I.175.231; 3.I.175.236; 3.I.175.237; 3.I.175.238;
3.I.175.239; 3.I.175.154; 3.I.175.157; 3.I.175.166; 3.I.175.169;
3.I.175.172; 3.I.175.175; 3.I.175.240; 3.I.175.244; 3.I.240.228;
3.I.240.229; 3.I.240.230; 3.I.240.231; 3.I.240.236; 3.I.240.237;
3.I.240.238; 3.I.240.239; 3.I.240.154; 3.I.240.157; 3.I.240.166;
3.I.240.169; 3.I.240.172; 3.I.240.175; 3.I.240.240; 3.I.240.244;
3.I.244.228; 3.I.244.229; 3.I.244.230; 3.I.244.231; 3.I.244.236;
3.I.244.237; 3.I.244.238; 3.I.244.239; 3.I.244.154; 3.I.244.157;
3.I.244.166; 3.I.244.169; 3.I.244.172; 3.I.244.175; 3.I.244.240;
3.I.244.244; Prodrugs of 3.J 3.J.228.228; 3.J.228.229; 3.J.228.230;
3.J.228.231; 3.J.228.236; 3.J.228.237; 3.J.228.238; 3.J.228.239;
3.J.228.154; 3.J.228.157; 3.J.228.166; 3.J.228.169; 3.J.228.172;
3.J.228.175; 3.J.228.240; 3.J.228.244; 3.J.229.228; 3.J.229.229;
3.J.229.230; 3.J.229.231; 3.J.229.236; 3.J.229.237; 3.J.229.238;
3.J.229.239; 3.J.229.154; 3.J.229.157; 3.J.229.166; 3.J.229.169;
3.J.229.172; 3.J.229.175; 3.J.229.240; 3.J.229.244; 3.J.230.228;
3.J.230.229; 3.J.230.230; 3.J.230.231; 3.J.230.236; 3.J.230.237;
3.J.230.238; 3.J.230.239; 3.J.230.154; 3.J.230.157; 3.J.230.166;
3.J.230.169; 3.J.230.172; 3.J.230.175; 3.J.230.240; 3.J.230.244;
3.J.231.228; 3.J.231.229; 3.J.231.230; 3.J.231.231; 3.J.231.236;
3.J.231.237; 3.J.231.238; 3.J.231.239; 3.J.231.154; 3.J.231.157;
3.J.231.166; 3.J.231.169; 3.J.231.172; 3.J.231.175; 3.J.231.240;
3.J.231.244; 3.J.236.228; 3.J.236.229; 3.J.236.230; 3.J.236.231;
3.J.236.236; 3.J.236.237; 3.J.236.238; 3.J.236.239; 3.J.236.154;
3.J.236.157; 3.J.236.166; 3.J.236.169; 3.J.236.172; 3.J.236.175;
3.J.236.240; 3.J.236.244; 3.J.237.228; 3.J.237.229; 3.J.237.230;
3.J.237.231; 3.J.237.236; 3.J.237.237; 3.J.237.238; 3.J.237.239;
3.J.237.154; 3.J.237.157; 3.J.237.166; 3.J.237.169; 3.J.237.172;
3.J.237.175; 3.J.237.240; 3.J.237.244; 3.J.238.228; 3.J.238.229;
3.J.238.230; 3.J.238.231; 3.J.238.236; 3.J.238.237; 3.J.238.238;
3.J.238.239; 3.J.238.154; 3.J.238.157; 3.J.238.166; 3.J.238.169;
3.J.238.172; 3.J.238.175; 3.J.238.240; 3.J.238.244; 3.J.239.228;
3.J.239.229; 3.J.239.230; 3.J.239.231; 3.J.239.236; 3.J.239.237;
3.J.239.238; 3.J.239.239; 3.J.239.154; 3.J.239.157; 3.J.239.166;
3.J.239.169; 3.J.239.172; 3.J.239.175; 3.J.239.240; 3.J.239.244;
3.J.154.228; 3.J.154.229; 3.J.154.230; 3.J.154.231; 3.J.154.236;
3.J.154.237; 3.J.154.238; 3.J.154.239; 3.J.154.154; 3.J.154.157;
3.J.154.166; 3.J.154.169; 3.J.154.172; 3.J.154.175; 3.J.154.240;
3.J.154.244; 3.J.157.228; 3.J.157.229; 3.J.157.230; 3.J.157.231;
3.J.157.236; 3.J.157.237; 3.J.157.238; 3.J.157.239; 3.J.157.154;
3.J.157.157; 3.J.157.166; 3.J.157.169; 3.J.157.172; 3.J.157.175;
3.J.157.240; 3.J.157.244; 3.J.166.228; 3.J.166.229; 3.J.166.230;
3.J.166.231; 3.J.166.236; 3.J.166.237; 3.J.166.238; 3.J.166.239;
3.J.166.154; 3.J.166.157; 3.J.166.166; 3.J.166.169; 3.J.166.172;
3.J.166.175; 3.J.166.240; 3.J.166.244; 3.J.169.228; 3.J.169.229;
3.J.169.230; 3.J.169.231; 3.J.169.236; 3.J.169.237; 3.J.169.238;
3.J.169.239; 3.J.169.154; 3.J.169.157; 3.J.169.166; 3.J.169.169;
3.J.169.172; 3.J.169.175; 3.J.169.240; 3.J.169.244; 3.J.172.228;
3.J.172.229; 3.J.172.230; 3.J.172.231; 3.J.172.236; 3.J.172.237;
3.J.172.238; 3.J.172.239; 3.J.172.154; 3.J.172.157; 3.J.172.166;
3.J.172.169; 3.J.172.172; 3.J.172.175; 3.J.172.240; 3.J.172.244;
3.J.175.228; 3.J.175.229; 3.J.175.230; 3.J.175.231; 3.J.175.236;
3.J.175.237; 3.J.175.238; 3.J.175.239; 3.J.175.154; 3.J.175.157;
3.J.175.166; 3.J.175.169; 3.J.175.172; 3.J.175.175; 3.J.175.240;
3.J.175.244; 3.J.240.228; 3.J.240.229; 3.J.240.230; 3.J.240.231;
3.J.240.236; 3.J.240.237; 3.J.240.238; 3.J.240.239; 3.J.240.154;
3.J.240.157; 3.J.240.166; 3.J.240.169; 3.J.240.172; 3.J.240.175;
3.J.240.240; 3.J.240.244; 3.J.244.228; 3.J.244.229; 3.J.244.230;
3.J.244.231; 3.J.244.236; 3.J.244.237; 3.J.244.238; 3.J.244.239;
3.J.244.154; 3.J.244.157; 3.J.244.166; 3.J.244.169; 3.J.244.172;
3.J.244.175; 3.J.244.240; 3.J.244.244; Prodrugs of 3.L 3.L.228.228;
3.L.228.229; 3.L.228.230; 3.L.228.231; 3.L.228.236; 3.L.228.237;
3.L.228.238; 3.L.228.239; 3.L.228.154; 3.L.228.157; 3.L.228.166;
3.L.228.169; 3.L.228.172; 3.L.228.175; 3.L.228.240; 3.L.228.244;
3.L.229.228; 3.L.229.229; 3.L.229.230; 3.L.229.231; 3.L.229.236;
3.L.229.237; 3.L.229.238; 3.L.229.239; 3.L.229.154; 3.L.229.157;
3.L.229.166; 3.L.229.169; 3.L.229.172; 3.L.229.175; 3.L.229.240;
3.L.229.244; 3.L.230.228; 3.L.230.229; 3.L.230.230; 3.L.230.231;
3.L.230.236; 3.L.230.237; 3.L.230.238; 3.L.230.239; 3.L.230.154;
3.L.230.157; 3.L.230.166; 3.L.230.169; 3.L.230.172; 3.L.230.175;
3.L.230.240; 3.L.230.244; 3.L.231.228; 3.L.231.229; 3.L.231.230;
3.L.231.231; 3.L.231.236; 3.L.231.237; 3.L.231.238; 3.L.231.239;
3.L.231.154; 3.L.231.157; 3.L.231.166; 3.L.231.169; 3.L.231.172;
3.L.231.175; 3.L.231.240; 3.L.231.244; 3.L.236.228; 3.L.236.229;
3.L.236.230; 3.L.236.231; 3.L.236.236; 3.L.236.237; 3.L.236.238;
3.L.236.239; 3.L.236.154; 3.L.236.157; 3.L.236.166; 3.L.236.169;
3.L.236.172; 3.L.236.175; 3.L.236.240; 3.L.236.244; 3.L.237.228;
3.L.237.229; 3.L.237.230; 3.L.237.231; 3.L.237.236; 3.L.237.237;
3.L.237.238; 3.L.237.239; 3.L.237.154; 3.L.237.157; 3.L.237.166;
3.L.237.169; 3.L.237.172; 3.L.237.175; 3.L.237.240; 3.L.237.244;
3.L.238.228; 3.L.238.229; 3.L.238.230; 3.L.238.231; 3.L.238.236;
3.L.238.237; 3.L.238.238; 3.L.238.239; 3.L.238.154; 3.L.238.157;
3.L.238.166; 3.L.238.169; 3.L.238.172; 3.L.238.175; 3.L.238.240;
3.L.238.244; 3.L.239.228; 3.L.239.229; 3.L.239.230; 3.L.239.231;
3.L.239.236; 3.L.239.237; 3.L.239.238; 3.L.239.239; 3.L.239.154;
3.L.239.157; 3.L.239.166; 3.L.239.169; 3.L.239.172; 3.L.239.175;
3.L.239.240; 3.L.239.244; 3.L.154.228; 3.L.154.229; 3.L.154.230;
3.L.154.231; 3.L.154.236; 3.L.154.237; 3.L.154.238; 3.L.154.239;
3.L.154.154; 3.L.154.157; 3.L.154.166; 3.L.154.169; 3.L.154.172;
3.L.154.175; 3.L.154.240; 3.L.154.244; 3.L.157.228; 3.L.157.229;
3.L.157.230; 3.L.157.231; 3.L.157.236; 3.L.157.237; 3.L.157.238;
3.L.157.239; 3.L.157.154; 3.L.157.157; 3.L.157.166; 3.L.157.169;
3.L.157.172; 3.L.157.175; 3.L.157.240; 3.L.157.244; 3.L.166.228;
3.L.166.229; 3.L.166.230; 3.L.166.231; 3.L.166.236; 3.L.166.237;
3.L.166.238; 3.L.166.239; 3.L.166.154; 3.L.166.157; 3.L.166.166;
3.L.166.169; 3.L.166.172; 3.L.166.175; 3.L.166.240; 3.L.166.244;
3.L.169.228; 3.L.169.229; 3.L.169.230; 3.L.169.231; 3.L.169.236;
3.L.169.237; 3.L.169.238; 3.L.169.239; 3.L.169.154; 3.L.169.157;
3.L.169.166; 3.L.169.169; 3.L.169.172; 3.L.169.175; 3.L.169.240;
3.L.169.244; 3.L.172.228; 3.L.172.229; 3.L.172.230; 3.L.172.231;
3.L.172.236; 3.L.172.237; 3.L.172.238; 3.L.172.239; 3.L.172.154;
3.L.172.157; 3.L.172.166; 3.L.172.169; 3.L.172.172; 3.L.172.175;
3.L.172.240; 3.L.172.244; 3.L.175.228; 3.L.175.229; 3.L.175.230;
3.L.175.231; 3.L.175.236; 3.L.175.237; 3.L.175.238; 3.L.175.239;
3.L.175.154; 3.L.175.157; 3.L.175.166; 3.L.175.169; 3.L.175.172;
3.L.175.175; 3.L.175.240; 3.L.175.244; 3.L.240.228; 3.L.240.229;
3.L.240.230; 3.L.240.231; 3.L.240.236; 3.L.240.237; 3.L.240.238;
3.L.240.239; 3.L.240.154; 3.L.240.157; 3.L.240.166; 3.L.240.169;
3.L.240.172; 3.L.240.175; 3.L.240.240; 3.L.240.244; 3.L.244.228;
3.L.244.229; 3.L.244.230; 3.L.244.231; 3.L.244.236; 3.L.244.237;
3.L.244.238; 3.L.244.239; 3.L.244.154; 3.L.244.157; 3.L.244.166;
3.L.244.169; 3.L.244.172; 3.L.244.175; 3.L.244.240; 3.L.244.244;
Prodrugs of 3.O 3.O.228.228; 3.O.228.229; 3.O.228.230; 3.O.228.231;
3.O.228.236; 3.O.228.237; 3.O.228.238; 3.O.228.239; 3.O.228.154;
3.O.228.157; 3.O.228.166; 3.O.228.169; 3.O.228.172; 3.O.228.175;
3.O.228.240; 3.O.228.244; 3.O.229.228; 3.O.229.229; 3.O.229.230;
3.O.229.231; 3.O.229.236; 3.O.229.237; 3.O.229.238; 3.O.229.239;
3.O.229.154; 3.O.229.157; 3.O.229.166; 3.O.229.169; 3.O.229.172;
3.O.229.175; 3.O.229.240; 3.O.229.244; 3.O.230.228; 3.O.230.229;
3.O.230.230; 3.O.230.231; 3.O.230.236; 3.O.230.237; 3.O.230.238;
3.O.230.239; 3.O.230.154; 3.O.230.157; 3.O.230.166; 3.O.230.169;
3.O.230.172; 3.O.230.175; 3.O.230.240; 3.O.230.244; 3.O.231.228;
3.O.231.229; 3.O.231.230; 3.O.231.231; 3.O.231.236; 3.O.231.237;
3.O.231.238; 3.O.231.239; 3.O.231.154; 3.O.231.157; 3.O.231.166;
3.O.231.169; 3.O.231.172; 3.O.231.175; 3.O.231.240; 3.O.231.244;
3.O.236.228; 3.O.236.229; 3.O.236.230; 3.O.236.231; 3.O.236.236;
3.O.236.237; 3.O.236.238; 3.O.236.239; 3.O.236.154; 3.O.236.157;
3.O.236.166; 3.O.236.169; 3.O.236.172; 3.O.236.175; 3.O.236.240;
3.O.236.244; 3.O.237.228; 3.O.237.229; 3.O.237.230; 3.O.237.231;
3.O.237.236; 3.O.237.237; 3.O.237.238; 3.O.237.239; 3.O.237.154;
3.O.237.157; 3.O.237.166; 3.O.237.169; 3.O.237.172; 3.O.237.175;
3.O.237.240; 3.O.237.244; 3.O.238.228; 3.O.238.229; 3.O.238.230;
3.O.238.231; 3.O.238.236; 3.O.238.237; 3.O.238.238; 3.O.238.239;
3.O.238.154; 3.O.238.157; 3.O.238.166; 3.O.238.169; 3.O.238.172;
3.O.238.175; 3.O.238.240; 3.O.238.244; 3.O.239.228; 3.O.239.229;
3.O.239.230; 3.O.239.231; 3.O.239.236; 3.O.239.237; 3.O.239.238;
3.O.239.239; 3.O.239.154; 3.O.239.157; 3.O.239.166; 3.O.239.169;
3.O.239.172; 3.O.239.175; 3.O.239.240; 3.O.239.244; 3.O.154.228;
3.O.154.229; 3.O.154.230; 3.O.154.231; 3.O.154.236; 3.O.154.237;
3.O.154.238; 3.O.154.239; 3.O.154.154; 3.O.154.157; 3.O.154.166;
3.O.154.169; 3.O.154.172; 3.O.154.175; 3.O.154.240; 3.O.154.244;
3.O.157.228; 3.O.157.229; 3.O.157.230; 3.O.157.231; 3.O.157.236;
3.O.157.237; 3.O.157.238; 3.O.157.239; 3.O.157.154; 3.O.157.157;
3.O.157.166; 3.O.157.169; 3.O.157.172; 3.O.157.175; 3.O.157.240;
3.O.157.244; 3.O.166.228; 3.O.166.229; 3.O.166.230; 3.O.166.231;
3.O.166.236; 3.O.166.237; 3.O.166.238; 3.O.166.239; 3.O.166.154;
3.O.166.157; 3.O.166.166; 3.O.166.169; 3.O.166.172; 3.O.166.175;
3.O.166.240; 3.O.166.244; 3.O.169.228; 3.O.169.229; 3.O.169.230;
3.O.169.231; 3.O.169.236; 3.O.169.237; 3.O.169.238; 3.O.169.239;
3.O.169.154; 3.O.169.157; 3.O.169.166; 3.O.169.169; 3.O.169.172;
3.O.169.175; 3.O.169.240; 3.O.169.244; 3.O.172.228; 3.O.172.229;
3.O.172.230; 3.O.172.231; 3.O.172.236; 3.O.172.237; 3.O.172.238;
3.O.172.239; 3.O.172.154; 3.O.172.157; 3.O.172.166; 3.O.172.169;
3.O.172.172; 3.O.172.175; 3.O.172.240; 3.O.172.244; 3.O.175.228;
3.O.175.229; 3.O.175.230; 3.O.175.231; 3.O.175.236; 3.O.175.237;
3.O.175.238; 3.O.175.239; 3.O.175.154; 3.O.175.157; 3.O.175.166;
3.O.175.169; 3.O.175.172; 3.O.175.175; 3.O.175.240; 3.O.175.244;
3.O.240.228; 3.O.240.229; 3.O.240.230; 3.O.240.231; 3.O.240.236;
3.O.240.237; 3.O.240.238; 3.O.240.239; 3.O.240.154; 3.O.240.157;
3.O.240.166; 3.O.240.169; 3.O.240.172; 3.O.240.175; 3.O.240.240;
3.O.240.244; 3.O.244.228; 3.O.244.229; 3.O.244.230; 3.O.244.231;
3.O.244.236; 3.O.244.237; 3.O.244.238; 3.O.244.239; 3.O.244.154;
3.O.244.157; 3.O.244.166; 3.O.244.169; 3.O.244.172; 3.O.244.175;
3.O.244.240; 3.O.244.244; Prodrugs of 3.P 3.P.228.228; 3.P.228.229;
3.P.228.230; 3.P.228.231; 3.P.228.236; 3.P.228.237; 3.P.228.238;
3.P.228.239; 3.P.228.154; 3.P.228.157; 3.P.228.166; 3.P.228.169;
3.P.228.172; 3.P.228.175; 3.P.228.240; 3.P.228.244; 3.P.229.228;
3.P.229.229; 3.P.229.230; 3.P.229.231; 3.P.229.236; 3.P.229.237;
3.P.229.238; 3.P.229.239; 3.P.229.154; 3.P.229.157; 3.P.229.166;
3.P.229.169; 3.P.229.172; 3.P.229.175; 3.P.229.240; 3.P.229.244;
3.P.230.228; 3.P.230.229; 3.P.230.230; 3.P.230.231; 3.P.230.236;
3.P.230.237; 3.P.230.238; 3.P.230.239; 3.P.230.154; 3.P.230.157;
3.P.230.166; 3.P.230.169; 3.P.230.172; 3.P.230.175; 3.P.230.240;
3.P.230.244; 3.P.231.228; 3.P.231.229; 3.P.231.230; 3.P.231.231;
3.P.231.236; 3.P.231.237; 3.P.231.238; 3.P.231.239; 3.P.231.154;
3.P.231.157; 3.P.231.166; 3.P.231.169; 3.P.231.172; 3.P.231.175;
3.P.231.240; 3.P.231.244; 3.P.236.228; 3.P.236.229; 3.P.236.230;
3.P.236.231; 3.P.236.236; 3.P.236.237; 3.P.236.238; 3.P.236.239;
3.P.236.154; 3.P.236.157; 3.P.236.166; 3.P.236.169; 3.P.236.172;
3.P.236.175; 3.P.236.240; 3.P.236.244; 3.P.237.228; 3.P.237.229;
3.P.237.230; 3.P.237.231; 3.P.237.236; 3.P.237.237; 3.P.237.238;
3.P.237.239; 3.P.237.154; 3.P.237.157; 3.P.237.166; 3.P.237.169;
3.P.237.172; 3.P.237.175; 3.P.237.240; 3.P.237.244; 3.P.238.228;
3.P.238.229; 3.P.238.230; 3.P.238.231; 3.P.238.236; 3.P.238.237;
3.P.238.238; 3.P.238.239; 3.P.238.154; 3.P.238.157; 3.P.238.166;
3.P.238.169; 3.P.238.172; 3.P.238.175; 3.P.238.240; 3.P.238.244;
3.P.239.228; 3.P.239.229; 3.P.239.230; 3.P.239.231; 3.P.239.236;
3.P.239.237; 3.P.239.238; 3.P.239.239; 3.P.239.154; 3.P.239.157;
3.P.239.166; 3.P.239.169; 3.P.239.172; 3.P.239.175; 3.P.239.240;
3.P.239.244; 3.P.154.228; 3.P.154.229; 3.P.154.230; 3.P.154.231;
3.P.154.236; 3.P.154.237; 3.P.154.238; 3.P.154.239; 3.P.154.154;
3.P.154.157; 3.P.154.166; 3.P.154.169; 3.P.154.172; 3.P.154.175;
3.P.154.240; 3.P.154.244; 3.P.157.228; 3.P.157.229; 3.P.157.230;
3.P.157.231; 3.P.157.236; 3.P.157.237; 3.P.157.238; 3.P.157.239;
3.P.157.154; 3.P.157.157; 3.P.157.166; 3.P.157.169; 3.P.157.172;
3.P.157.175; 3.P.157.240; 3.P.157.244; 3.P.166.228; 3.P.166.229;
3.P.166.230; 3.P.166.231; 3.P.166.236; 3.P.166.237; 3.P.166.238;
3.P.166.239; 3.P.166.154; 3.P.166.157; 3.P.166.166; 3.P.166.169;
3.P.166.172; 3.P.166.175; 3.P.166.240; 3.P.166.244; 3.P.169.228;
3.P.169.229; 3.P.169.230; 3.P.169.231; 3.P.169.236; 3.P.169.237;
3.P.169.238; 3.P.169.239; 3.P.169.154; 3.P.169.157; 3.P.169.166;
3.P.169.169; 3.P.169.172; 3.P.169.175; 3.P.169.240; 3.P.169.244;
3.P.172.228; 3.P.172.229; 3.P.172.230; 3.P.172.231; 3.P.172.236;
3.P.172.237; 3.P.172.238; 3.P.172.239; 3.P.172.154; 3.P.172.157;
3.P.172.166; 3.P.172.169; 3.P.172.172; 3.P.172.175; 3.P.172.240;
3.P.172.244; 3.P.175.228; 3.P.175.229; 3.P.175.230; 3.P.175.231;
3.P.175.236; 3.P.175.237; 3.P.175.238; 3.P.175.239; 3.P.175.154;
3.P.175.157; 3.P.175.166; 3.P.175.169; 3.P.175.172; 3.P.175.175;
3.P.175.240; 3.P.175.244; 3.P.240.228; 3.P.240.229; 3.P.240.230;
3.P.240.231; 3.P.240.236; 3.P.240.237; 3.P.240.238; 3.P.240.239;
3.P.240.154; 3.P.240.157; 3.P.240.166; 3.P.240.169; 3.P.240.172;
3.P.240.175; 3.P.240.240; 3.P.240.244; 3.P.244.228; 3.P.244.229;
3.P.244.230; 3.P.244.231; 3.P.244.236; 3.P.244.237; 3.P.244.238;
3.P.244.239; 3.P.244.154; 3.P.244.157; 3.P.244.166; 3.P.244.169;
3.P.244.172; 3.P.244.175; 3.P.244.240; 3.P.244.244; Prodrugs of 3.U
3.U.228.228; 3.U.228.229; 3.U.228.230; 3.U.228.231; 3.U.228.236;
3.U.228.237; 3.U.228.238; 3.U.228.239; 3.U.228.154; 3.U.228.157;
3.U.228.166; 3.U.228.169; 3.U.228.172; 3.U.228.175; 3.U.228.240;
3.U.228.244; 3.U.229.228; 3.U.229.229; 3.U.229.230;
3.U.229.231;
3.U.229.236; 3.U.229.237; 3.U.229.238; 3.U.229.239; 3.U.229.154;
3.U.229.157; 3.U.229.166; 3.U.229.169; 3.U.229.172; 3.U.229.175;
3.U.229.240; 3.U.229.244; 3.U.230.228; 3.U.230.229; 3.U.230.230;
3.U.230.231; 3.U.230.236; 3.U.230.237; 3.U.230.238; 3.U.230.239;
3.U.230.154; 3.U.230.157; 3.U.230.166; 3.U.230.169; 3.U.230.172;
3.U.230.175; 3.U.230.240; 3.U.230.244; 3.U.231.228; 3.U.231.229;
3.U.231.230; 3.U.231.231; 3.U.231.236; 3.U.231.237; 3.U.231.238;
3.U.231.239; 3.U.231.154; 3.U.231.157; 3.U.231.166; 3.U.231.169;
3.U.231.172; 3.U.231.175; 3.U.231.240; 3.U.231.244; 3.U.236.228;
3.U.236.229; 3.U.236.230; 3.U.236.231; 3.U.236.236; 3.U.236.237;
3.U.236.238; 3.U.236.239; 3.U.236.154; 3.U.236.157; 3.U.236.166;
3.U.236.169; 3.U.236.172; 3.U.236.175; 3.U.236.240; 3.U.236.244;
3.U.237.228; 3.U.237.229; 3.U.237.230; 3.U.237.231; 3.U.237.236;
3.U.237.237; 3.U.237.238; 3.U.237.239; 3.U.237.154; 3.U.237.157;
3.U.237.166; 3.U.237.169; 3.U.237.172; 3.U.237.175; 3.U.237.240;
3.U.237.244; 3.U.238.228; 3.U.238.229; 3.U.238.230; 3.U.238.231;
3.U.238.236; 3.U.238.237; 3.U.238.238; 3.U.238.239; 3.U.238.154;
3.U.238.157; 3.U.238.166; 3.U.238.169; 3.U.238.172; 3.U.238.175;
3.U.238.240; 3.U.238.244; 3.U.239.228; 3.U.239.229; 3.U.239.230;
3.U.239.231; 3.U.239.236; 3.U.239.237; 3.U.239.238; 3.U.239.239;
3.U.239.154; 3.U.239.157; 3.U.239.166; 3.U.239.169; 3.U.239.172;
3.U.239.175; 3.U.239.240; 3.U.239.244; 3.U.154.228; 3.U.154.229;
3.U.154.230; 3.U.154.231; 3.U.154.236; 3.U.154.237; 3.U.154.238;
3.U.154.239; 3.U.154.154; 3.U.154.157; 3.U.154.166; 3.U.154.169;
3.U.154.172; 3.U.154.175; 3.U.154.240; 3.U.154.244; 3.U.157.228;
3.U.157.229; 3.U.157.230; 3.U.157.231; 3.U.157.236; 3.U.157.237;
3.U.157.238; 3.U.157.239; 3.U.157.154; 3.U.157.157; 3.U.157.166;
3.U.157.169; 3.U.157.172; 3.U.157.175; 3.U.157.240; 3.U.157.244;
3.U.166.228; 3.U.166.229; 3.U.166.230; 3.U.166.231; 3.U.166.236;
3.U.166.237; 3.U.166.238; 3.U.166.239; 3.U.166.154; 3.U.166.157;
3.U.166.166; 3.U.166.169; 3.U.166.172; 3.U.166.175; 3.U.166.240;
3.U.166.244; 3.U.169.228; 3.U.169.229; 3.U.169.230; 3.U.169.231;
3.U.169.236; 3.U.169.237; 3.U.169.238; 3.U.169.239; 3.U.169.154;
3.U.169.157; 3.U.169.166; 3.U.169.169; 3.U.169.172; 3.U.169.175;
3.U.169.240; 3.U.169.244; 3.U.172.228; 3.U.172.229; 3.U.172.230;
3.U.172.231; 3.U.172.236; 3.U.172.237; 3.U.172.238; 3.U.172.239;
3.U.172.154; 3.U.172.157; 3.U.172.166; 3.U.172.169; 3.U.172.172;
3.U.172.175; 3.U.172.240; 3.U.172.244; 3.U.175.228; 3.U.175.229;
3.U.175.230; 3.U.175.231; 3.U.175.236; 3.U.175.237; 3.U.175.238;
3.U.175.239; 3.U.175.154; 3.U.175.157; 3.U.175.166; 3.U.175.169;
3.U.175.172; 3.U.175.175; 3.U.175.240; 3.U.175.244; 3.U.240.228;
3.U.240.229; 3.U.240.230; 3.U.240.231; 3.U.240.236; 3.U.240.237;
3.U.240.238; 3.U.240.239; 3.U.240.154; 3.U.240.157; 3.U.240.166;
3.U.240.169; 3.U.240.172; 3.U.240.175; 3.U.240.240; 3.U.240.244;
3.U.244.228; 3.U.244.229; 3.U.244.230; 3.U.244.231; 3.U.244.236;
3.U.244.237; 3.U.244.238; 3.U.244.239; 3.U.244.154; 3.U.244.157;
3.U.244.166; 3.U.244.169; 3.U.244.172; 3.U.244.175; 3.U.244.240;
3.U.244.244; Prodrugs of 3.W 3.W.228.228; 3.W.228.229; 3.W.228.230;
3.W.228.231; 3.W.228.236; 3.W.228.237; 3.W.228.238; 3.W.228.239;
3.W.228.154; 3.W.228.157; 3.W.228.166; 3.W.228.169; 3.W.228.172;
3.W.228.175; 3.W.228.240; 3.W.228.244; 3.W.229.228; 3.W.229.229;
3.W.229.230; 3.W.229.231; 3.W.229.236; 3.W.229.237; 3.W.229.238;
3.W.229.239; 3.W.229.154; 3.W.229.157; 3.W.229.166; 3.W.229.169;
3.W.229.172; 3.W.229.175; 3.W.229.240; 3.W.229.244; 3.W.230.228;
3.W.230.229; 3.W.230.230; 3.W.230.231; 3.W.230.236; 3.W.230.237;
3.W.230.238; 3.W.230.239; 3.W.230.154; 3.W.230.157; 3.W.230.166;
3.W.230.169; 3.W.230.172; 3.W.230.175; 3.W.230.240; 3.W.230.244;
3.W.231.228; 3.W.231.229; 3.W.231.230; 3.W.231.231; 3.W.231.236;
3.W.231.237; 3.W.231.238; 3.W.231.239; 3.W.231.154; 3.W.231.157;
3.W.231.166; 3.W.231.169; 3.W.231.172; 3.W.231.175; 3.W.231.240;
3.W.231.244; 3.W.236.228; 3.W.236.229; 3.W.236.230; 3.W.236.231;
3.W.236.236; 3.W.236.237; 3.W.236.238; 3.W.236.239; 3.W.236.154;
3.W.236.157; 3.W.236.166; 3.W.236.169; 3.W.236.172; 3.W.236.175;
3.W.236.240; 3.W.236.244; 3.W.237.228; 3.W.237.229; 3.W.237.230;
3.W.237.231; 3.W.237.236; 3.W.237.237; 3.W.237.238; 3.W.237.239;
3.W.237.154; 3.W.237.157; 3.W.237.166; 3.W.237.169; 3.W.237.172;
3.W.237.175; 3.W.237.240; 3.W.237.244; 3.W.238.228; 3.W.238.229;
3.W.238.230; 3.W.238.231; 3.W.238.236; 3.W.238.237; 3.W.238.238;
3.W.238.239; 3.W.238.154; 3.W.238.157; 3.W.238.166; 3.W.238.169;
3.W.238.172; 3.W.238.175; 3.W.238.240; 3.W.238.244; 3.W.239.228;
3.W.239.229; 3.W.239.230; 3.W.239.231; 3.W.239.236; 3.W.239.237;
3.W.239.238; 3.W.239.239; 3.W.239.154; 3.W.239.157; 3.W.239.166;
3.W.239.169; 3.W.239.172; 3.W.239.175; 3.W.239.240; 3.W.239.244;
3.W.154.228; 3.W.154.229; 3.W.154.230; 3.W.154.231; 3.W.154.236;
3.W.154.237; 3.W.154.238; 3.W.154.239; 3.W.154.154; 3.W.154.157;
3.W.154.166; 3.W.154.169; 3.W.154.172; 3.W.154.175; 3.W.154.240;
3.W.154.244; 3.W.157.228; 3.W.157.229; 3.W.157.230; 3.W.157.231;
3.W.157.236; 3.W.157.237; 3.W.157.238; 3.W.157.239; 3.W.157.154;
3.W.157.157; 3.W.157.166; 3.W.157.169; 3.W.157.172; 3.W.157.175;
3.W.157.240; 3.W.157.244; 3.W.166.228; 3.W.166.229; 3.W.166.230;
3.W.166.231; 3.W.166.236; 3.W.166.237; 3.W.166.238; 3.W.166.239;
3.W.166.154; 3.W.166.157; 3.W.166.166; 3.W.166.169; 3.W.166.172;
3.W.166.175; 3.W.166.240; 3.W.166.244; 3.W.169.228; 3.W.169.229;
3.W.169.230; 3.W.169.231; 3.W.169.236; 3.W.169.237; 3.W.169.238;
3.W.169.239; 3.W.169.154; 3.W.169.157; 3.W.169.166; 3.W.169.169;
3.W.169.172; 3.W.169.175; 3.W.169.240; 3.W.169.244; 3.W.172.228;
3.W.172.229; 3.W.172.230; 3.W.172.231; 3.W.172.236; 3.W.172.237;
3.W.172.238; 3.W.172.239; 3.W.172.154; 3.W.172.157; 3.W.172.166;
3.W.172.169; 3.W.172.172; 3.W.172.175; 3.W.172.240; 3.W.172.244;
3.W.175.228; 3.W.175.229; 3.W.175.230; 3.W.175.231; 3.W.175.236;
3.W.175.237; 3.W.175.238; 3.W.175.239; 3.W.175.154; 3.W.175.157;
3.W.175.166; 3.W.175.169; 3.W.175.172; 3.W.175.175; 3.W.175.240;
3.W.175.244; 3.W.240.228; 3.W.240.229; 3.W.240.230; 3.W.240.231;
3.W.240.236; 3.W.240.237; 3.W.240.238; 3.W.240.239; 3.W.240.154;
3.W.240.157; 3.W.240.166; 3.W.240.169; 3.W.240.172; 3.W.240.175;
3.W.240.240; 3.W.240.244; 3.W.244.228; 3.W.244.229; 3.W.244.230;
3.W.244.231; 3.W.244.236; 3.W.244.237; 3.W.244.238; 3.W.244.239;
3.W.244.154; 3.W.244.157; 3.W.244.166; 3.W.244.169; 3.W.244.172;
3.W.244.175; 3.W.244.240; 3.W.244.244; Prodrugs of 3.Y 3.Y.228.228;
3.Y.228.229; 3.Y.228.230; 3.Y.228.231; 3.Y.228.236; 3.Y.228.237;
3.Y.228.238; 3.Y.228.239; 3.Y.228.154; 3.Y.228.157; 3.Y.228.166;
3.Y.228.169; 3.Y.228.172; 3.Y.228.175; 3.Y.228.240; 3.Y.228.244;
3.Y.229.228; 3.Y.229.229; 3.Y.229.230; 3.Y.229.231; 3.Y.229.236;
3.Y.229.237; 3.Y.229.238; 3.Y.229.239; 3.Y.229.154; 3.Y.229.157;
3.Y.229.166; 3.Y.229.169; 3.Y.229.172; 3.Y.229.175; 3.Y.229.240;
3.Y.229.244; 3.Y.230.228; 3.Y.230.229; 3.Y.230.230; 3.Y.230.231;
3.Y.230.236; 3.Y.230.237; 3.Y.230.238; 3.Y.230.239; 3.Y.230.154;
3.Y.230.157; 3.Y.230.166; 3.Y.230.169; 3.Y.230.172; 3.Y.230.175;
3.Y.230.240; 3.Y.230.244; 3.Y.231.228; 3.Y.231.229; 3.Y.231.230;
3.Y.231.231; 3.Y.231.236; 3.Y.231.237; 3.Y.231.238; 3.Y.231.239;
3.Y.231.154; 3.Y.231.157; 3.Y.231.166; 3.Y.231.169; 3.Y.231.172;
3.Y.231.175; 3.Y.231.240; 3.Y.231.244; 3.Y.236.228; 3.Y.236.229;
3.Y.236.230; 3.Y.236.231; 3.Y.236.236; 3.Y.236.237; 3.Y.236.238;
3.Y.236.239; 3.Y.236.154; 3.Y.236.157; 3.Y.236.166; 3.Y.236.169;
3.Y.236.172; 3.Y.236.175; 3.Y.236.240; 3.Y.236.244; 3.Y.237.228;
3.Y.237.229; 3.Y.237.230; 3.Y.237.231; 3.Y.237.236; 3.Y.237.237;
3.Y.237.238; 3.Y.237.239; 3.Y.237.154; 3.Y.237.157; 3.Y.237.166;
3.Y.237.169; 3.Y.237.172; 3.Y.237.175; 3.Y.237.240; 3.Y.237.244;
3.Y.238.228; 3.Y.238.229; 3.Y.238.230; 3.Y.238.231; 3.Y.238.236;
3.Y.238.237; 3.Y.238.238; 3.Y.238.239; 3.Y.238.154; 3.Y.238.157;
3.Y.238.166; 3.Y.238.169; 3.Y.238.172; 3.Y.238.175; 3.Y.238.240;
3.Y.238.244; 3.Y.239.228; 3.Y.239.229; 3.Y.239.230; 3.Y.239.231;
3.Y.239.236; 3.Y.239.237; 3.Y.239.238; 3.Y.239.239; 3.Y.239.154;
3.Y.239.157; 3.Y.239.166; 3.Y.239.169; 3.Y.239.172; 3.Y.239.175;
3.Y.239.240; 3.Y.239.244; 3.Y.154.228; 3.Y.154.229; 3.Y.154.230;
3.Y.154.231; 3.Y.154.236; 3.Y.154.237; 3.Y.154.238; 3.Y.154.239;
3.Y.154.154; 3.Y.154.157; 3.Y.154.166; 3.Y.154.169; 3.Y.154.172;
3.Y.154.175; 3.Y.154.240; 3.Y.154.244; 3.Y.157.228; 3.Y.157.229;
3.Y.157.230; 3.Y.157.231; 3.Y.157.236; 3.Y.157.237; 3.Y.157.238;
3.Y.157.239; 3.Y.157.154; 3.Y.157.157; 3.Y.157.166; 3.Y.157.169;
3.Y.157.172; 3.Y.157.175; 3.Y.157.240; 3.Y.157.244; 3.Y.166.228;
3.Y.166.229; 3.Y.166.230; 3.Y.166.231; 3.Y.166.236; 3.Y.166.237;
3.Y.166.238; 3.Y.166.239; 3.Y.166.154; 3.Y.166.157; 3.Y.166.166;
3.Y.166.169; 3.Y.166.172; 3.Y.166.175; 3.Y.166.240; 3.Y.166.244;
3.Y.169.228; 3.Y.169.229; 3.Y.169.230; 3.Y.169.231; 3.Y.169.236;
3.Y.169.237; 3.Y.169.238; 3.Y.169.239; 3.Y.169.154; 3.Y.169.157;
3.Y.169.166; 3.Y.169.169; 3.Y.169.172; 3.Y.169.175; 3.Y.169.240;
3.Y.169.244; 3.Y.172.228; 3.Y.172.229; 3.Y.172.230; 3.Y.172.231;
3.Y.172.236; 3.Y.172.237; 3.Y.172.238; 3.Y.172.239; 3.Y.172.154;
3.Y.172.157; 3.Y.172.166; 3.Y.172.169; 3.Y.172.172; 3.Y.172.175;
3.Y.172.240; 3.Y.172.244; 3.Y.175.228; 3.Y.175.229; 3.Y.175.230;
3.Y.175.231; 3.Y.175.236; 3.Y.175.237; 3.Y.175.238; 3.Y.175.239;
3.Y.175.154; 3.Y.175.157; 3.Y.175.166; 3.Y.175.169; 3.Y.175.172;
3.Y.175.175; 3.Y.175.240; 3.Y.175.244; 3.Y.240.228; 3.Y.240.229;
3.Y.240.230; 3.Y.240.231; 3.Y.240.236; 3.Y.240.237; 3.Y.240.238;
3.Y.240.239; 3.Y.240.154; 3.Y.240.157; 3.Y.240.166; 3.Y.240.169;
3.Y.240.172; 3.Y.240.175; 3.Y.240.240; 3.Y.240.244; 3.Y.244.228;
3.Y.244.229; 3.Y.244.230; 3.Y.244.231; 3.Y.244.236; 3.Y.244.237;
3.Y.244.238; 3.Y.244.239; 3.Y.244.154; 3.Y.244.157; 3.Y.244.166;
3.Y.244.169; 3.Y.244.172; 3.Y.244.175; 3.Y.244.240; 3.Y.244.244;
Prodrugs of 4.B 4.B.228.228; 4.B.228.229; 4.B.228.230; 4.B.228.231;
4.B.228.236; 4.B.228.237; 4.B.228.238; 4.B.228.239; 4.B.228.154;
4.B.228.157; 4.B.228.166; 4.B.228.169; 4.B.228.172; 4.B.228.175;
4.B.228.240; 4.B.228.244; 4.B.229.228; 4.B.229.229; 4.B.229.230;
4.B.229.231; 4.B.229.236; 4.B.229.237; 4.B.229.238; 4.B.229.239;
4.B.229.154; 4.B.229.157; 4.B.229.166; 4.B.229.169; 4.B.229.172;
4.B.229.175; 4.B.229.240; 4.B.229.244; 4.B.230.228; 4.B.230.229;
4.B.230.230; 4.B.230.231; 4.B.230.236; 4.B.230.237; 4.B.230.238;
4.B.230.239; 4.B.230.154; 4.B.230.157; 4.B.230.166; 4.B.230.169;
4.B.230.172; 4.B.230.175; 4.B.230.240; 4.B.230.244; 4.B.231.228;
4.B.231.229; 4.B.231.230; 4.B.231.231; 4.B.231.236; 4.B.231.237;
4.B.231.238; 4.B.231.239; 4.B.231.154; 4.B.231.157; 4.B.231.166;
4.B.231.169; 4.B.231.172; 4.B.231.175; 4.B.231.240; 4.B.231.244;
4.B.236.228; 4.B.236.229; 4.B.236.230; 4.B.236.231; 4.B.236.236;
4.B.236.237; 4.B.236.238; 4.B.236.239; 4.B.236.154; 4.B.236.157;
4.B.236.166; 4.B.236.169; 4.B.236.172; 4.B.236.175; 4.B.236.240;
4.B.236.244; 4.B.237.228; 4.B.237.229; 4.B.237.230; 4.B.237.231;
4.B.237.236; 4.B.237.237; 4.B.237.238; 4.B.237.239; 4.B.237.154;
4.B.237.157; 4.B.237.166; 4.B.237.169; 4.B.237.172; 4.B.237.175;
4.B.237.240; 4.B.237.244; 4.B.238.228; 4.B.238.229; 4.B.238.230;
4.B.238.231; 4.B.238.236; 4.B.238.237; 4.B.238.238; 4.B.238.239;
4.B.238.154; 4.B.238.157; 4.B.238.166; 4.B.238.169; 4.B.238.172;
4.B.238.175; 4.B.238.240; 4.B.238.244; 4.B.239.228; 4.B.239.229;
4.B.239.230; 4.B.239.231; 4.B.239.236; 4.B.239.237; 4.B.239.238;
4.B.239.239; 4.B.239.154; 4.B.239.157; 4.B.239.166; 4.B.239.169;
4.B.239.172; 4.B.239.175; 4.B.239.240; 4.B.239.244; 4.B.154.228;
4.B.154.229; 4.B.154.230; 4.B.154.231; 4.B.154.236; 4.B.154.237;
4.B.154.238; 4.B.154.239; 4.B.154.154; 4.B.154.157; 4.B.154.166;
4.B.154.169; 4.B.154.172; 4.B.154.175; 4.B.154.240; 4.B.154.244;
4.B.157.228; 4.B.157.229; 4.B.157.230; 4.B.157.231; 4.B.157.236;
4.B.157.237; 4.B.157.238; 4.B.157.239; 4.B.157.154; 4.B.157.157;
4.B.157.166; 4.B.157.169; 4.B.157.172; 4.B.157.175; 4.B.157.240;
4.B.157.244; 4.B.166.228; 4.B.166.229; 4.B.166.230; 4.B.166.231;
4.B.166.236; 4.B.166.237; 4.B.166.238; 4.B.166.239; 4.B.166.154;
4.B.166.157; 4.B.166.166; 4.B.166.169; 4.B.166.172; 4.B.166.175;
4.B.166.240; 4.B.166.244; 4.B.169.228; 4.B.169.229; 4.B.169.230;
4.B.169.231; 4.B.169.236; 4.B.169.237; 4.B.169.238; 4.B.169.239;
4.B.169.154; 4.B.169.157; 4.B.169.166; 4.B.169.169; 4.B.169.172;
4.B.169.175; 4.B.169.240; 4.B.169.244; 4.B.172.228; 4.B.172.229;
4.B.172.230; 4.B.172.231; 4.B.172.236; 4.B.172.237; 4.B.172.238;
4.B.172.239; 4.B.172.154; 4.B.172.157; 4.B.172.166; 4.B.172.169;
4.B.172.172; 4.B.172.175; 4.B.172.240; 4.B.172.244; 4.B.175.228;
4.B.175.229; 4.B.175.230; 4.B.175.231; 4.B.175.236; 4.B.175.237;
4.B.175.238; 4.B.175.239; 4.B.175.154; 4.B.175.157; 4.B.175.166;
4.B.175.169; 4.B.175.172; 4.B.175.175; 4.B.175.240; 4.B.175.244;
4.B.240.228; 4.B.240.229; 4.B.240.230; 4.B.240.231; 4.B.240.236;
4.B.240.237; 4.B.240.238; 4.B.240.239; 4.B.240.154; 4.B.240.157;
4.B.240.166; 4.B.240.169; 4.B.240.172; 4.B.240.175; 4.B.240.240;
4.B.240.244; 4.B.244.228; 4.B.244.229; 4.B.244.230; 4.B.244.231;
4.B.244.236; 4.B.244.237; 4.B.244.238; 4.B.244.239; 4.B.244.154;
4.B.244.157; 4.B.244.166; 4.B.244.169; 4.B.244.172; 4.B.244.175;
4.B.244.240; 4.B.244.244; Prodrugs of 4.D 4.D.228.228; 4.D.228.229;
4.D.228.230; 4.D.228.231; 4.D.228.236; 4.D.228.237; 4.D.228.238;
4.D.228.239; 4.D.228.154; 4.D.228.157; 4.D.228.166; 4.D.228.169;
4.D.228.172; 4.D.228.175; 4.D.228.240; 4.D.228.244; 4.D.229.228;
4.D.229.229; 4.D.229.230; 4.D.229.231; 4.D.229.236; 4.D.229.237;
4.D.229.238; 4.D.229.239; 4.D.229.154; 4.D.229.157; 4.D.229.166;
4.D.229.169; 4.D.229.172; 4.D.229.175; 4.D.229.240; 4.D.229.244;
4.D.230.228; 4.D.230.229; 4.D.230.230; 4.D.230.231; 4.D.230.236;
4.D.230.237; 4.D.230.238; 4.D.230.239; 4.D.230.154; 4.D.230.157;
4.D.230.166; 4.D.230.169; 4.D.230.172; 4.D.230.175; 4.D.230.240;
4.D.230.244; 4.D.231.228; 4.D.231.229; 4.D.231.230; 4.D.231.231;
4.D.231.236; 4.D.231.237; 4.D.231.238; 4.D.231.239; 4.D.231.154;
4.D.231.157; 4.D.231.166; 4.D.231.169; 4.D.231.172; 4.D.231.175;
4.D.231.240; 4.D.231.244; 4.D.236.228; 4.D.236.229; 4.D.236.230;
4.D.236.231; 4.D.236.236; 4.D.236.237; 4.D.236.238; 4.D.236.239;
4.D.236.154; 4.D.236.157; 4.D.236.166; 4.D.236.169; 4.D.236.172;
4.D.236.175; 4.D.236.240; 4.D.236.244; 4.D.237.228; 4.D.237.229;
4.D.237.230; 4.D.237.231; 4.D.237.236; 4.D.237.237; 4.D.237.238;
4.D.237.239; 4.D.237.154; 4.D.237.157; 4.D.237.166; 4.D.237.169;
4.D.237.172; 4.D.237.175; 4.D.237.240; 4.D.237.244; 4.D.238.228;
4.D.238.229; 4.D.238.230; 4.D.238.231; 4.D.238.236; 4.D.238.237;
4.D.238.238; 4.D.238.239; 4.D.238.154; 4.D.238.157; 4.D.238.166;
4.D.238.169; 4.D.238.172; 4.D.238.175; 4.D.238.240; 4.D.238.244;
4.D.239.228; 4.D.239.229; 4.D.239.230; 4.D.239.231; 4.D.239.236;
4.D.239.237; 4.D.239.238; 4.D.239.239; 4.D.239.154; 4.D.239.157;
4.D.239.166; 4.D.239.169; 4.D.239.172; 4.D.239.175; 4.D.239.240;
4.D.239.244; 4.D.154.228; 4.D.154.229; 4.D.154.230; 4.D.154.231;
4.D.154.236; 4.D.154.237; 4.D.154.238; 4.D.154.239; 4.D.154.154;
4.D.154.157; 4.D.154.166; 4.D.154.169; 4.D.154.172; 4.D.154.175;
4.D.154.240; 4.D.154.244; 4.D.157.228; 4.D.157.229; 4.D.157.230;
4.D.157.231; 4.D.157.236; 4.D.157.237; 4.D.157.238; 4.D.157.239;
4.D.157.154; 4.D.157.157; 4.D.157.166; 4.D.157.169; 4.D.157.172;
4.D.157.175; 4.D.157.240; 4.D.157.244; 4.D.166.228; 4.D.166.229;
4.D.166.230; 4.D.166.231; 4.D.166.236; 4.D.166.237; 4.D.166.238;
4.D.166.239; 4.D.166.154; 4.D.166.157; 4.D.166.166; 4.D.166.169;
4.D.166.172; 4.D.166.175; 4.D.166.240; 4.D.166.244; 4.D.169.228;
4.D.169.229; 4.D.169.230; 4.D.169.231; 4.D.169.236; 4.D.169.237;
4.D.169.238; 4.D.169.239; 4.D.169.154; 4.D.169.157; 4.D.169.166;
4.D.169.169; 4.D.169.172; 4.D.169.175; 4.D.169.240; 4.D.169.244;
4.D.172.228; 4.D.172.229; 4.D.172.230; 4.D.172.231; 4.D.172.236;
4.D.172.237; 4.D.172.238; 4.D.172.239; 4.D.172.154; 4.D.172.157;
4.D.172.166; 4.D.172.169; 4.D.172.172; 4.D.172.175; 4.D.172.240;
4.D.172.244; 4.D.175.228; 4.D.175.229; 4.D.175.230; 4.D.175.231;
4.D.175.236; 4.D.175.237; 4.D.175.238;
4.D.175.239; 4.D.175.154; 4.D.175.157; 4.D.175.166; 4.D.175.169;
4.D.175.172; 4.D.175.175; 4.D.175.240; 4.D.175.244; 4.D.240.228;
4.D.240.229; 4.D.240.230; 4.D.240.231; 4.D.240.236; 4.D.240.237;
4.D.240.238; 4.D.240.239; 4.D.240.154; 4.D.240.157; 4.D.240.166;
4.D.240.169; 4.D.240.172; 4.D.240.175; 4.D.240.240; 4.D.240.244;
4.D.244.228; 4.D.244.229; 4.D.244.230; 4.D.244.231; 4.D.244.236;
4.D.244.237; 4.D.244.238; 4.D.244.239; 4.D.244.154; 4.D.244.157;
4.D.244.166; 4.D.244.169; 4.D.244.172; 4.D.244.175; 4.D.244.240;
4.D.244.244; Prodrugs of 4.E 4.E.228.228; 4.E.228.229; 4.E.228.230;
4.E.228.231; 4.E.228.236; 4.E.228.237; 4.E.228.238; 4.E.228.239;
4.E.228.154; 4.E.228.157; 4.E.228.166; 4.E.228.169; 4.E.228.172;
4.E.228.175; 4.E.228.240; 4.E.228.244; 4.E.229.228; 4.E.229.229;
4.E.229.230; 4.E.229.231; 4.E.229.236; 4.E.229.237; 4.E.229.238;
4.E.229.239; 4.E.229.154; 4.E.229.157; 4.E.229.166; 4.E.229.169;
4.E.229.172; 4.E.229.175; 4.E.229.240; 4.E.229.244; 4.E.230.228;
4.E.230.229; 4.E.230.230; 4.E.230.231; 4.E.230.236; 4.E.230.237;
4.E.230.238; 4.E.230.239; 4.E.230.154; 4.E.230.157; 4.E.230.166;
4.E.230.169; 4.E.230.172; 4.E.230.175; 4.E.230.240; 4.E.230.244;
4.E.231.228; 4.E.231.229; 4.E.231.230; 4.E.231.231; 4.E.231.236;
4.E.231.237; 4.E.231.238; 4.E.231.239; 4.E.231.154; 4.E.231.157;
4.E.231.166; 4.E.231.169; 4.E.231.172; 4.E.231.175; 4.E.231.240;
4.E.231.244; 4.E.236.228; 4.E.236.229; 4.E.236.230; 4.E.236.231;
4.E.236.236; 4.E.236.237; 4.E.236.238; 4.E.236.239; 4.E.236.154;
4.E.236.157; 4.E.236.166; 4.E.236.169; 4.E.236.172; 4.E.236.175;
4.E.236.240; 4.E.236.244; 4.E.237.228; 4.E.237.229; 4.E.237.230;
4.E.237.231; 4.E.237.236; 4.E.237.237; 4.E.237.238; 4.E.237.239;
4.E.237.154; 4.E.237.157; 4.E.237.166; 4.E.237.169; 4.E.237.172;
4.E.237.175; 4.E.237.240; 4.E.237.244; 4.E.238.228; 4.E.238.229;
4.E.238.230; 4.E.238.231; 4.E.238.236; 4.E.238.237; 4.E.238.238;
4.E.238.239; 4.E.238.154; 4.E.238.157; 4.E.238.166; 4.E.238.169;
4.E.238.172; 4.E.238.175; 4.E.238.240; 4.E.238.244; 4.E.239.228;
4.E.239.229; 4.E.239.230; 4.E.239.231; 4.E.239.236; 4.E.239.237;
4.E.239.238; 4.E.239.239; 4.E.239.154; 4.E.239.157; 4.E.239.166;
4.E.239.169; 4.E.239.172; 4.E.239.175; 4.E.239.240; 4.E.239.244;
4.E.154.228; 4.E.154.229; 4.E.154.230; 4.E.154.231; 4.E.154.236;
4.E.154.237; 4.E.154.238; 4.E.154.239; 4.E.154.154; 4.E.154.157;
4.E.154.166; 4.E.154.169; 4.E.154.172; 4.E.154.175; 4.E.154.240;
4.E.154.244; 4.E.157.228; 4.E.157.229; 4.E.157.230; 4.E.157.231;
4.E.157.236; 4.E.157.237; 4.E.157.238; 4.E.157.239; 4.E.157.154;
4.E.157.157; 4.E.157.166; 4.E.157.169; 4.E.157.172; 4.E.157.175;
4.E.157.240; 4.E.157.244; 4.E.166.228; 4.E.166.229; 4.E.166.230;
4.E.166.231; 4.E.166.236; 4.E.166.237; 4.E.166.238; 4.E.166.239;
4.E.166.154; 4.E.166.157; 4.E.166.166; 4.E.166.169; 4.E.166.172;
4.E.166.175; 4.E.166.240; 4.E.166.244; 4.E.169.228; 4.E.169.229;
4.E.169.230; 4.E.169.231; 4.E.169.236; 4.E.169.237; 4.E.169.238;
4.E.169.239; 4.E.169.154; 4.E.169.157; 4.E.169.166; 4.E.169.169;
4.E.169.172; 4.E.169.175; 4.E.169.240; 4.E.169.244; 4.E.172.228;
4.E.172.229; 4.E.172.230; 4.E.172.231; 4.E.172.236; 4.E.172.237;
4.E.172.238; 4.E.172.239; 4.E.172.154; 4.E.172.157; 4.E.172.166;
4.E.172.169; 4.E.172.172; 4.E.172.175; 4.E.172.240; 4.E.172.244;
4.E.175.228; 4.E.175.229; 4.E.175.230; 4.E.175.231; 4.E.175.236;
4.E.175.237; 4.E.175.238; 4.E.175.239; 4.E.175.154; 4.E.175.157;
4.E.175.166; 4.E.175.169; 4.E.175.172; 4.E.175.175; 4.E.175.240;
4.E.175.244; 4.E.240.228; 4.E.240.229; 4.E.240.230; 4.E.240.231;
4.E.240.236; 4.E.240.237; 4.E.240.238; 4.E.240.239; 4.E.240.154;
4.E.240.157; 4.E.240.166; 4.E.240.169; 4.E.240.172; 4.E.240.175;
4.E.240.240; 4.E.240.244; 4.E.244.228; 4.E.244.229; 4.E.244.230;
4.E.244.231; 4.E.244.236; 4.E.244.237; 4.E.244.238; 4.E.244.239;
4.E.244.154; 4.E.244.157; 4.E.244.166; 4.E.244.169; 4.E.244.172;
4.E.244.175; 4.E.244.240; 4.E.244.244; Prodrugs of 4.G 4.G.228.228;
4.G.228.229; 4.G.228.230; 4.G.228.231; 4.G.228.236; 4.G.228.237;
4.G.228.238; 4.G.228.239; 4.G.228.154; 4.G.228.157; 4.G.228.166;
4.G.228.169; 4.G.228.172; 4.G.228.175; 4.G.228.240; 4.G.228.244;
4.G.229.228; 4.G.229.229; 4.G.229.230; 4.G.229.231; 4.G.229.236;
4.G.229.237; 4.G.229.238; 4.G.229.239; 4.G.229.154; 4.G.229.157;
4.G.229.166; 4.G.229.169; 4.G.229.172; 4.G.229.175; 4.G.229.240;
4.G.229.244; 4.G.230.228; 4.G.230.229; 4.G.230.230; 4.G.230.231;
4.G.230.236; 4.G.230.237; 4.G.230.238; 4.G.230.239; 4.G.230.154;
4.G.230.157; 4.G.230.166; 4.G.230.169; 4.G.230.172; 4.G.230.175;
4.G.230.240; 4.G.230.244; 4.G.231.228; 4.G.231.229; 4.G.231.230;
4.G.231.231; 4.G.231.236; 4.G.231.237; 4.G.231.238; 4.G.231.239;
4.G.231.154; 4.G.231.157; 4.G.231.166; 4.G.231.169; 4.G.231.172;
4.G.231.175; 4.G.231.240; 4.G.231.244; 4.G.236.228; 4.G.236.229;
4.G.236.230; 4.G.236.231; 4.G.236.236; 4.G.236.237; 4.G.236.238;
4.G.236.239; 4.G.236.154; 4.G.236.157; 4.G.236.166; 4.G.236.169;
4.G.236.172; 4.G.236.175; 4.G.236.240; 4.G.236.244; 4.G.237.228;
4.G.237.229; 4.G.237.230; 4.G.237.231; 4.G.237.236; 4.G.237.237;
4.G.237.238; 4.G.237.239; 4.G.237.154; 4.G.237.157; 4.G.237.166;
4.G.237.169; 4.G.237.172; 4.G.237.175; 4.G.237.240; 4.G.237.244;
4.G.238.228; 4.G.238.229; 4.G.238.230; 4.G.238.231; 4.G.238.236;
4.G.238.237; 4.G.238.238; 4.G.238.239; 4.G.238.154; 4.G.238.157;
4.G.238.166; 4.G.238.169; 4.G.238.172; 4.G.238.175; 4.G.238.240;
4.G.238.244; 4.G.239.228; 4.G.239.229; 4.G.239.230; 4.G.239.231;
4.G.239.236; 4.G.239.237; 4.G.239.238; 4.G.239.239; 4.G.239.154;
4.G.239.157; 4.G.239.166; 4.G.239.169; 4.G.239.172; 4.G.239.175;
4.G.239.240; 4.G.239.244; 4.G.154.228; 4.G.154.229; 4.G.154.230;
4.G.154.231; 4.G.154.236; 4.G.154.237; 4.G.154.238; 4.G.154.239;
4.G.154.154; 4.G.154.157; 4.G.154.166; 4.G.154.169; 4.G.154.172;
4.G.154.175; 4.G.154.240; 4.G.154.244; 4.G.157.228; 4.G.157.229;
4.G.157.230; 4.G.157.231; 4.G.157.236; 4.G.157.237; 4.G.157.238;
4.G.157.239; 4.G.157.154; 4.G.157.157; 4.G.157.166; 4.G.157.169;
4.G.157.172; 4.G.157.175; 4.G.157.240; 4.G.157.244; 4.G.166.228;
4.G.166.229; 4.G.166.230; 4.G.166.231; 4.G.166.236; 4.G.166.237;
4.G.166.238; 4.G.166.239; 4.G.166.154; 4.G.166.157; 4.G.166.166;
4.G.166.169; 4.G.166.172; 4.G.166.175; 4.G.166.240; 4.G.166.244;
4.G.169.228; 4.G.169.229; 4.G.169.230; 4.G.169.231; 4.G.169.236;
4.G.169.237; 4.G.169.238; 4.G.169.239; 4.G.169.154; 4.G.169.157;
4.G.169.166; 4.G.169.169; 4.G.169.172; 4.G.169.175; 4.G.169.240;
4.G.169.244; 4.G.172.228; 4.G.172.229; 4.G.172.230; 4.G.172.231;
4.G.172.236; 4.G.172.237; 4.G.172.238; 4.G.172.239; 4.G.172.154;
4.G.172.157; 4.G.172.166; 4.G.172.169; 4.G.172.172; 4.G.172.175;
4.G.172.240; 4.G.172.244; 4.G.175.228; 4.G.175.229; 4.G.175.230;
4.G.175.231; 4.G.175.236; 4.G.175.237; 4.G.175.238; 4.G.175.239;
4.G.175.154; 4.G.175.157; 4.G.175.166; 4.G.175.169; 4.G.175.172;
4.G.175.175; 4.G.175.240; 4.G.175.244; 4.G.240.228; 4.G.240.229;
4.G.240.230; 4.G.240.231; 4.G.240.236; 4.G.240.237; 4.G.240.238;
4.G.240.239; 4.G.240.154; 4.G.240.157; 4.G.240.166; 4.G.240.169;
4.G.240.172; 4.G.240.175; 4.G.240.240; 4.G.240.244; 4.G.244.228;
4.G.244.229; 4.G.244.230; 4.G.244.231; 4.G.244.236; 4.G.244.237;
4.G.244.238; 4.G.244.239; 4.G.244.154; 4.G.244.157; 4.G.244.166;
4.G.244.169; 4.G.244.172; 4.G.244.175; 4.G.244.240; 4.G.244.244;
Prodrugs of 4.I 4.I.228.228; 4.I.228.229; 4.I.228.230; 4.I.228.231;
4.I.228.236; 4.I.228.237; 4.I.228.238; 4.I.228.239; 4.I.228.154;
4.I.228.157; 4.I.228.166; 4.I.228.169; 4.I.228.172; 4.I.228.175;
4.I.228.240; 4.I.228.244; 4.I.229.228; 4.I.229.229; 4.I.229.230;
4.I.229.231; 4.I.229.236; 4.I.229.237; 4.I.229.238; 4.I.229.239;
4.I.229.154; 4.I.229.157; 4.I.229.166; 4.I.229.169; 4.I.229.172;
4.I.229.175; 4.I.229.240; 4.I.229.244; 4.I.230.228; 4.I.230.229;
4.I.230.230; 4.I.230.231; 4.I.230.236; 4.I.230.237; 4.I.230.238;
4.I.230.239; 4.I.230.154; 4.I.230.157; 4.I.230.166; 4.I.230.169;
4.I.230.172; 4.I.230.175; 4.I.230.240; 4.I.230.244; 4.I.231.228;
4.I.231.229; 4.I.231.230; 4.I.231.231; 4.I.231.236; 4.I.231.237;
4.I.231.238; 4.I.231.239; 4.I.231.154; 4.I.231.157; 4.I.231.166;
4.I.231.169; 4.I.231.172; 4.I.231.175; 4.I.231.240; 4.I.231.244;
4.I.236.228; 4.I.236.229; 4.I.236.230; 4.I.236.231; 4.I.236.236;
4.I.236.237; 4.I.236.238; 4.I.236.239; 4.I.236.154; 4.I.236.157;
4.I.236.166; 4.I.236.169; 4.I.236.172; 4.I.236.175; 4.I.236.240;
4.I.236.244; 4.I.237.228; 4.I.237.229; 4.I.237.230; 4.I.237.231;
4.I.237.236; 4.I.237.237; 4.I.237.238; 4.I.237.239; 4.I.237.154;
4.I.237.157; 4.I.237.166; 4.I.237.169; 4.I.237.172; 4.I.237.175;
4.I.237.240; 4.I.237.244; 4.I.238.228; 4.I.238.229; 4.I.238.230;
4.I.238.231; 4.I.238.236; 4.I.238.237; 4.I.238.238; 4.I.238.239;
4.I.238.154; 4.I.238.157; 4.I.238.166; 4.I.238.169; 4.I.238.172;
4.I.238.175; 4.I.238.240; 4.I.238.244; 4.I.239.228; 4.I.239.229;
4.I.239.230; 4.I.239.231; 4.I.239.236; 4.I.239.237; 4.I.239.238;
4.I.239.239; 4.I.239.154; 4.I.239.157; 4.I.239.166; 4.I.239.169;
4.I.239.172; 4.I.239.175; 4.I.239.240; 4.I.239.244; 4.I.154.228;
4.I.154.229; 4.I.154.230; 4.I.154.231; 4.I.154.236; 4.I.154.237;
4.I.154.238; 4.I.154.239; 4.I.154.154; 4.I.154.157; 4.I.154.166;
4.I.154.169; 4.I.154.172; 4.I.154.175; 4.I.154.240; 4.I.154.244;
4.I.157.228; 4.I.157.229; 4.I.157.230; 4.I.157.231; 4.I.157.236;
4.I.157.237; 4.I.157.238; 4.I.157.239; 4.I.157.154; 4.I.157.157;
4.I.157.166; 4.I.157.169; 4.I.157.172; 4.I.157.175; 4.I.157.240;
4.I.157.244; 4.I.166.228; 4.I.166.229; 4.I.166.230; 4.I.166.231;
4.I.166.236; 4.I.166.237; 4.I.166.238; 4.I.166.239; 4.I.166.154;
4.I.166.157; 4.I.166.166; 4.I.166.169; 4.I.166.172; 4.I.166.175;
4.I.166.240; 4.I.166.244; 4.I.169.228; 4.I.169.229; 4.I.169.230;
4.I.169.231; 4.I.169.236; 4.I.169.237; 4.I.169.238; 4.I.169.239;
4.I.169.154; 4.I.169.157; 4.I.169.166; 4.I.169.169; 4.I.169.172;
4.I.169.175; 4.I.169.240; 4.I.169.244; 4.I.172.228; 4.I.172.229;
4.I.172.230; 4.I.172.231; 4.I.172.236; 4.I.172.237; 4.I.172.238;
4.I.172.239; 4.I.172.154; 4.I.172.157; 4.I.172.166; 4.I.172.169;
4.I.172.172; 4.I.172.175; 4.I.172.240; 4.I.172.244; 4.I.175.228;
4.I.175.229; 4.I.175.230; 4.I.175.231; 4.I.175.236; 4.I.175.237;
4.I.175.238; 4.I.175.239; 4.I.175.154; 4.I.175.157; 4.I.175.166;
4.I.175.169; 4.I.175.172; 4.I.175.175; 4.I.175.240; 4.I.175.244;
4.I.240.228; 4.I.240.229; 4.I.240.230; 4.I.240.231; 4.I.240.236;
4.I.240.237; 4.I.240.238; 4.I.240.239; 4.I.240.154; 4.I.240.157;
4.I.240.166; 4.I.240.169; 4.I.240.172; 4.I.240.175; 4.I.240.240;
4.I.240.244; 4.I.244.228; 4.I.244.229; 4.I.244.230; 4.I.244.231;
4.I.244.236; 4.I.244.237; 4.I.244.238; 4.I.244.239; 4.I.244.154;
4.I.244.157; 4.I.244.166; 4.I.244.169; 4.I.244.172; 4.I.244.175;
4.I.244.240; 4.I.244.244; Prodrugs of 4.J 4.J.228.228; 4.J.228.229;
4.J.228.230; 4.J.228.231; 4.J.228.236; 4.J.228.237; 4.J.228.238;
4.J.228.239; 4.J.228.154; 4.J.228.157; 4.J.228.166; 4.J.228.169;
4.J.228.172; 4.J.228.175; 4.J.228.240; 4.J.228.244; 4.J.229.228;
4.J.229.229; 4.J.229.230; 4.J.229.231; 4.J.229.236; 4.J.229.237;
4.J.229.238; 4.J.229.239; 4.J.229.154; 4.J.229.157; 4.J.229.166;
4.J.229.169; 4.J.229.172; 4.J.229.175; 4.J.229.240; 4.J.229.244;
4.J.230.228; 4.J.230.229; 4.J.230.230; 4.J.230.231; 4.J.230.236;
4.J.230.237; 4.J.230.238; 4.J.230.239; 4.J.230.154; 4.J.230.157;
4.J.230.166; 4.J.230.169; 4.J.230.172; 4.J.230.175; 4.J.230.240;
4.J.230.244; 4.J.231.228; 4.J.231.229; 4.J.231.230; 4.J.231.231;
4.J.231.236; 4.J.231.237; 4.J.231.238; 4.J.231.239; 4.J.231.154;
4.J.231.157; 4.J.231.166; 4.J.231.169; 4.J.231.172; 4.J.231.175;
4.J.231.240; 4.J.231.244; 4.J.236.228; 4.J.236.229; 4.J.236.230;
4.J.236.231; 4.J.236.236; 4.J.236.237; 4.J.236.238; 4.J.236.239;
4.J.236.154; 4.J.236.157; 4.J.236.166; 4.J.236.169; 4.J.236.172;
4.J.236.175; 4.J.236.240; 4.J.236.244; 4.J.237.228; 4.J.237.229;
4.J.237.230; 4.J.237.231; 4.J.237.236; 4.J.237.237; 4.J.237.238;
4.J.237.239; 4.J.237.154; 4.J.237.157; 4.J.237.166; 4.J.237.169;
4.J.237.172; 4.J.237.175; 4.J.237.240; 4.J.237.244; 4.J.238.228;
4.J.238.229; 4.J.238.230; 4.J.238.231; 4.J.238.236; 4.J.238.237;
4.J.238.238; 4.J.238.239; 4.J.238.154; 4.J.238.157; 4.J.238.166;
4.J.238.169; 4.J.238.172; 4.J.238.175; 4.J.238.240; 4.J.238.244;
4.J.239.228; 4.J.239.229; 4.J.239.230; 4.J.239.231; 4.J.239.236;
4.J.239.237; 4.J.239.238; 4.J.239.239; 4.J.239.154; 4.J.239.157;
4.J.239.166; 4.J.239.169; 4.J.239.172; 4.J.239.175; 4.J.239.240;
4.J.239.244; 4.J.154.228; 4.J.154.229; 4.J.154.230; 4.J.154.231;
4.J.154.236; 4.J.154.237; 4.J.154.238; 4.J.154.239; 4.J.154.154;
4.J.154.157; 4.J.154.166; 4.J.154.169; 4.J.154.172; 4.J.154.175;
4.J.154.240; 4.J.154.244; 4.J.157.228; 4.J.157.229; 4.J.157.230;
4.J.157.231; 4.J.157.236; 4.J.157.237; 4.J.157.238; 4.J.157.239;
4.J.157.154; 4.J.157.157; 4.J.157.166; 4.J.157.169; 4.J.157.172;
4.J.157.175; 4.J.157.240; 4.J.157.244; 4.J.166.228; 4.J.166.229;
4.J.166.230; 4.J.166.231; 4.J.166.236; 4.J.166.237; 4.J.166.238;
4.J.166.239; 4.J.166.154; 4.J.166.157; 4.J.166.166; 4.J.166.169;
4.J.166.172; 4.J.166.175; 4.J.166.240; 4.J.166.244; 4.J.169.228;
4.J.169.229; 4.J.169.230; 4.J.169.231; 4.J.169.236; 4.J.169.237;
4.J.169.238; 4.J.169.239; 4.J.169.154; 4.J.169.157; 4.J.169.166;
4.J.169.169; 4.J.169.172; 4.J.169.175; 4.J.169.240; 4.J.169.244;
4.J.172.228; 4.J.172.229; 4.J.172.230; 4.J.172.231; 4.J.172.236;
4.J.172.237; 4.J.172.238; 4.J.172.239; 4.J.172.154; 4.J.172.157;
4.J.172.166; 4.J.172.169; 4.J.172.172; 4.J.172.175; 4.J.172.240;
4.J.172.244; 4.J.175.228; 4.J.175.229; 4.J.175.230; 4.J.175.231;
4.J.175.236; 4.J.175.237; 4.J.175.238; 4.J.175.239; 4.J.175.154;
4.J.175.157; 4.J.175.166; 4.J.175.169; 4.J.175.172; 4.J.175.175;
4.J.175.240; 4.J.175.244; 4.J.240.228; 4.J.240.229; 4.J.240.230;
4.J.240.231; 4.J.240.236; 4.J.240.237; 4.J.240.238; 4.J.240.239;
4.J.240.154; 4.J.240.157; 4.J.240.166; 4.J.240.169; 4.J.240.172;
4.J.240.175; 4.J.240.240; 4.J.240.244; 4.J.244.228; 4.J.244.229;
4.J.244.230; 4.J.244.231; 4.J.244.236; 4.J.244.237; 4.J.244.238;
4.J.244.239; 4.J.244.154; 4.J.244.157; 4.J.244.166; 4.J.244.169;
4.J.244.172; 4.J.244.175; 4.J.244.240; 4.J.244.244; Prodrugs of 4.L
4.L.228.228; 4.L.228.229; 4.L.228.230; 4.L.228.231; 4.L.228.236;
4.L.228.237; 4.L.228.238; 4.L.228.239; 4.L.228.154; 4.L.228.157;
4.L.228.166; 4.L.228.169; 4.L.228.172; 4.L.228.175; 4.L.228.240;
4.L.228.244; 4.L.229.228; 4.L.229.229; 4.L.229.230; 4.L.229.231;
4.L.229.236; 4.L.229.237; 4.L.229.238; 4.L.229.239; 4.L.229.154;
4.L.229.157; 4.L.229.166; 4.L.229.169; 4.L.229.172; 4.L.229.175;
4.L.229.240; 4.L.229.244; 4.L.230.228; 4.L.230.229; 4.L.230.230;
4.L.230.231; 4.L.230.236; 4.L.230.237; 4.L.230.238; 4.L.230.239;
4.L.230.154; 4.L.230.157; 4.L.230.166; 4.L.230.169; 4.L.230.172;
4.L.230.175; 4.L.230.240; 4.L.230.244; 4.L.231.228; 4.L.231.229;
4.L.231.230; 4.L.231.231; 4.L.231.236; 4.L.231.237; 4.L.231.238;
4.L.231.239; 4.L.231.154; 4.L.231.157; 4.L.231.166; 4.L.231.169;
4.L.231.172; 4.L.231.175; 4.L.231.240; 4.L.231.244; 4.L.236.228;
4.L.236.229; 4.L.236.230; 4.L.236.231; 4.L.236.236; 4.L.236.237;
4.L.236.238; 4.L.236.239; 4.L.236.154; 4.L.236.157; 4.L.236.166;
4.L.236.169; 4.L.236.172; 4.L.236.175; 4.L.236.240; 4.L.236.244;
4.L.237.228; 4.L.237.229; 4.L.237.230; 4.L.237.231; 4.L.237.236;
4.L.237.237; 4.L.237.238; 4.L.237.239; 4.L.237.154; 4.L.237.157;
4.L.237.166; 4.L.237.169; 4.L.237.172; 4.L.237.175; 4.L.237.240;
4.L.237.244; 4.L.238.228; 4.L.238.229; 4.L.238.230; 4.L.238.231;
4.L.238.236; 4.L.238.237; 4.L.238.238; 4.L.238.239; 4.L.238.154;
4.L.238.157; 4.L.238.166; 4.L.238.169; 4.L.238.172; 4.L.238.175;
4.L.238.240; 4.L.238.244; 4.L.239.228; 4.L.239.229; 4.L.239.230;
4.L.239.231; 4.L.239.236; 4.L.239.237; 4.L.239.238; 4.L.239.239;
4.L.239.154; 4.L.239.157; 4.L.239.166; 4.L.239.169; 4.L.239.172;
4.L.239.175; 4.L.239.240; 4.L.239.244; 4.L.154.228; 4.L.154.229;
4.L.154.230; 4.L.154.231; 4.L.154.236; 4.L.154.237; 4.L.154.238;
4.L.154.239; 4.L.154.154; 4.L.154.157; 4.L.154.166; 4.L.154.169;
4.L.154.172; 4.L.154.175; 4.L.154.240; 4.L.154.244;
4.L.157.228;
4.L.157.229; 4.L.157.230; 4.L.157.231; 4.L.157.236; 4.L.157.237;
4.L.157.238; 4.L.157.239; 4.L.157.154; 4.L.157.157; 4.L.157.166;
4.L.157.169; 4.L.157.172; 4.L.157.175; 4.L.157.240; 4.L.157.244;
4.L.166.228; 4.L.166.229; 4.L.166.230; 4.L.166.231; 4.L.166.236;
4.L.166.237; 4.L.166.238; 4.L.166.239; 4.L.166.154; 4.L.166.157;
4.L.166.166; 4.L.166.169; 4.L.166.172; 4.L.166.175; 4.L.166.240;
4.L.166.244; 4.L.169.228; 4.L.169.229; 4.L.169.230; 4.L.169.231;
4.L.169.236; 4.L.169.237; 4.L.169.238; 4.L.169.239; 4.L.169.154;
4.L.169.157; 4.L.169.166; 4.L.169.169; 4.L.169.172; 4.L.169.175;
4.L.169.240; 4.L.169.244; 4.L.172.228; 4.L.172.229; 4.L.172.230;
4.L.172.231; 4.L.172.236; 4.L.172.237; 4.L.172.238; 4.L.172.239;
4.L.172.154; 4.L.172.157; 4.L.172.166; 4.L.172.169; 4.L.172.172;
4.L.172.175; 4.L.172.240; 4.L.172.244; 4.L.175.228; 4.L.175.229;
4.L.175.230; 4.L.175.231; 4.L.175.236; 4.L.175.237; 4.L.175.238;
4.L.175.239; 4.L.175.154; 4.L.175.157; 4.L.175.166; 4.L.175.169;
4.L.175.172; 4.L.175.175; 4.L.175.240; 4.L.175.244; 4.L.240.228;
4.L.240.229; 4.L.240.230; 4.L.240.231; 4.L.240.236; 4.L.240.237;
4.L.240.238; 4.L.240.239; 4.L.240.154; 4.L.240.157; 4.L.240.166;
4.L.240.169; 4.L.240.172; 4.L.240.175; 4.L.240.240; 4.L.240.244;
4.L.244.228; 4.L.244.229; 4.L.244.230; 4.L.244.231; 4.L.244.236;
4.L.244.237; 4.L.244.238; 4.L.244.239; 4.L.244.154; 4.L.244.157;
4.L.244.166; 4.L.244.169; 4.L.244.172; 4.L.244.175; 4.L.244.240;
4.L.244.244; Prodrugs of 4.O 4.O.228.228; 4.O.228.229; 4.O.228.230;
4.O.228.231; 4.O.228.236; 4.O.228.237; 4.O.228.238; 4.O.228.239;
4.O.228.154; 4.O.228.157; 4.O.228.166; 4.O.228.169; 4.O.228.172;
4.O.228.175; 4.O.228.240; 4.O.228.244; 4.O.229.228; 4.O.229.229;
4.O.229.230; 4.O.229.231; 4.O.229.236; 4.O.229.237; 4.O.229.238;
4.O.229.239; 4.O.229.154; 4.O.229.157; 4.O.229.166; 4.O.229.169;
4.O.229.172; 4.O.229.175; 4.O.229.240; 4.O.229.244; 4.O.230.228;
4.O.230.229; 4.O.230.230; 4.O.230.231; 4.O.230.236; 4.O.230.237;
4.O.230.238; 4.O.230.239; 4.O.230.154; 4.O.230.157; 4.O.230.166;
4.O.230.169; 4.O.230.172; 4.O.230.175; 4.O.230.240; 4.O.230.244;
4.O.231.228; 4.O.231.229; 4.O.231.230; 4.O.231.231; 4.O.231.236;
4.O.231.237; 4.O.231.238; 4.O.231.239; 4.O.231.154; 4.O.231.157;
4.O.231.166; 4.O.231.169; 4.O.231.172; 4.O.231.175; 4.O.231.240;
4.O.231.244; 4.O.236.228; 4.O.236.229; 4.O.236.230; 4.O.236.231;
4.O.236.236; 4.O.236.237; 4.O.236.238; 4.O.236.239; 4.O.236.154;
4.O.236.157; 4.O.236.166; 4.O.236.169; 4.O.236.172; 4.O.236.175;
4.O.236.240; 4.O.236.244; 4.O.237.228; 4.O.237.229; 4.O.237.230;
4.O.237.231; 4.O.237.236; 4.O.237.237; 4.O.237.238; 4.O.237.239;
4.O.237.154; 4.O.237.157; 4.O.237.166; 4.O.237.169; 4.O.237.172;
4.O.237.175; 4.O.237.240; 4.O.237.244; 4.O.238.228; 4.O.238.229;
4.O.238.230; 4.O.238.231; 4.O.238.236; 4.O.238.237; 4.O.238.238;
4.O.238.239; 4.O.238.154; 4.O.238.157; 4.O.238.166; 4.O.238.169;
4.O.238.172; 4.O.238.175; 4.O.238.240; 4.O.238.244; 4.O.239.228;
4.O.239.229; 4.O.239.230; 4.O.239.231; 4.O.239.236; 4.O.239.237;
4.O.239.238; 4.O.239.239; 4.O.239.154; 4.O.239.157; 4.O.239.166;
4.O.239.169; 4.O.239.172; 4.O.239.175; 4.O.239.240; 4.O.239.244;
4.O.154.228; 4.O.154.229; 4.O.154.230; 4.O.154.231; 4.O.154.236;
4.O.154.237; 4.O.154.238; 4.O.154.239; 4.O.154.154; 4.O.154.157;
4.O.154.166; 4.O.154.169; 4.O.154.172; 4.O.154.175; 4.O.154.240;
4.O.154.244; 4.O.157.228; 4.O.157.229; 4.O.157.230; 4.O.157.231;
4.O.157.236; 4.O.157.237; 4.O.157.238; 4.O.157.239; 4.O.157.154;
4.O.157.157; 4.O.157.166; 4.O.157.169; 4.O.157.172; 4.O.157.175;
4.O.157.240; 4.O.157.244; 4.O.166.228; 4.O.166.229; 4.O.166.230;
4.O.166.231; 4.O.166.236; 4.O.166.237; 4.O.166.238; 4.O.166.239;
4.O.166.154; 4.O.166.157; 4.O.166.166; 4.O.166.169; 4.O.166.172;
4.O.166.175; 4.O.166.240; 4.O.166.244; 4.O.169.228; 4.O.169.229;
4.O.169.230; 4.O.169.231; 4.O.169.236; 4.O.169.237; 4.O.169.238;
4.O.169.239; 4.O.169.154; 4.O.169.157; 4.O.169.166; 4.O.169.169;
4.O.169.172; 4.O.169.175; 4.O.169.240; 4.O.169.244; 4.O.172.228;
4.O.172.229; 4.O.172.230; 4.O.172.231; 4.O.172.236; 4.O.172.237;
4.O.172.238; 4.O.172.239; 4.O.172.154; 4.O.172.157; 4.O.172.166;
4.O.172.169; 4.O.172.172; 4.O.172.175; 4.O.172.240; 4.O.172.244;
4.O.175.228; 4.O.175.229; 4.O.175.230; 4.O.175.231; 4.O.175.236;
4.O.175.237; 4.O.175.238; 4.O.175.239; 4.O.175.154; 4.O.175.157;
4.O.175.166; 4.O.175.169; 4.O.175.172; 4.O.175.175; 4.O.175.240;
4.O.175.244; 4.O.240.228; 4.O.240.229; 4.O.240.230; 4.O.240.231;
4.O.240.236; 4.O.240.237; 4.O.240.238; 4.O.240.239; 4.O.240.154;
4.O.240.157; 4.O.240.166; 4.O.240.169; 4.O.240.172; 4.O.240.175;
4.O.240.240; 4.O.240.244; 4.O.244.228; 4.O.244.229; 4.O.244.230;
4.O.244.231; 4.O.244.236; 4.O.244.237; 4.O.244.238; 4.O.244.239;
4.O.244.154; 4.O.244.157; 4.O.244.166; 4.O.244.169; 4.O.244.172;
4.O.244.175; 4.O.244.240; 4.O.244.244; Prodrugs of 4.P 4.P.228.228;
4.P.228.229; 4.P.228.230; 4.P.228.231; 4.P.228.236; 4.P.228.237;
4.P.228.238; 4.P.228.239; 4.P.228.154; 4.P.228.157; 4.P.228.166;
4.P.228.169; 4.P.228.172; 4.P.228.175; 4.P.228.240; 4.P.228.244;
4.P.229.228; 4.P.229.229; 4.P.229.230; 4.P.229.231; 4.P.229.236;
4.P.229.237; 4.P.229.238; 4.P.229.239; 4.P.229.154; 4.P.229.157;
4.P.229.166; 4.P.229.169; 4.P.229.172; 4.P.229.175; 4.P.229.240;
4.P.229.244; 4.P.230.228; 4.P.230.229; 4.P.230.230; 4.P.230.231;
4.P.230.236; 4.P.230.237; 4.P.230.238; 4.P.230.239; 4.P.230.154;
4.P.230.157; 4.P.230.166; 4.P.230.169; 4.P.230.172; 4.P.230.175;
4.P.230.240; 4.P.230.244; 4.P.231.228; 4.P.231.229; 4.P.231.230;
4.P.231.231; 4.P.231.236; 4.P.231.237; 4.P.231.238; 4.P.231.239;
4.P.231.154; 4.P.231.157; 4.P.231.166; 4.P.231.169; 4.P.231.172;
4.P.231.175; 4.P.231.240; 4.P.231.244; 4.P.236.228; 4.P.236.229;
4.P.236.230; 4.P.236.231; 4.P.236.236; 4.P.236.237; 4.P.236.238;
4.P.236.239; 4.P.236.154; 4.P.236.157; 4.P.236.166; 4.P.236.169;
4.P.236.172; 4.P.236.175; 4.P.236.240; 4.P.236.244; 4.P.237.228;
4.P.237.229; 4.P.237.230; 4.P.237.231; 4.P.237.236; 4.P.237.237;
4.P.237.238; 4.P.237.239; 4.P.237.154; 4.P.237.157; 4.P.237.166;
4.P.237.169; 4.P.237.172; 4.P.237.175; 4.P.237.240; 4.P.237.244;
4.P.238.228; 4.P.238.229; 4.P.238.230; 4.P.238.231; 4.P.238.236;
4.P.238.237; 4.P.238.238; 4.P.238.239; 4.P.238.154; 4.P.238.157;
4.P.238.166; 4.P.238.169; 4.P.238.172; 4.P.238.175; 4.P.238.240;
4.P.238.244; 4.P.239.228; 4.P.239.229; 4.P.239.230; 4.P.239.231;
4.P.239.236; 4.P.239.237; 4.P.239.238; 4.P.239.239; 4.P.239.154;
4.P.239.157; 4.P.239.166; 4.P.239.169; 4.P.239.172; 4.P.239.175;
4.P.239.240; 4.P.239.244; 4.P.154.228; 4.P.154.229; 4.P.154.230;
4.P.154.231; 4.P.154.236; 4.P.154.237; 4.P.154.238; 4.P.154.239;
4.P.154.154; 4.P.154.157; 4.P.154.166; 4.P.154.169; 4.P.154.172;
4.P.154.175; 4.P.154.240; 4.P.154.244; 4.P.157.228; 4.P.157.229;
4.P.157.230; 4.P.157.231; 4.P.157.236; 4.P.157.237; 4.P.157.238;
4.P.157.239; 4.P.157.154; 4.P.157.157; 4.P.157.166; 4.P.157.169;
4.P.157.172; 4.P.157.175; 4.P.157.240; 4.P.157.244; 4.P.166.228;
4.P.166.229; 4.P.166.230; 4.P.166.231; 4.P.166.236; 4.P.166.237;
4.P.166.238; 4.P.166.239; 4.P.166.154; 4.P.166.157; 4.P.166.166;
4.P.166.169; 4.P.166.172; 4.P.166.175; 4.P.166.240; 4.P.166.244;
4.P.169.228; 4.P.169.229; 4.P.169.230; 4.P.169.231; 4.P.169.236;
4.P.169.237; 4.P.169.238; 4.P.169.239; 4.P.169.154; 4.P.169.157;
4.P.169.166; 4.P.169.169; 4.P.169.172; 4.P.169.175; 4.P.169.240;
4.P.169.244; 4.P.172.228; 4.P.172.229; 4.P.172.230; 4.P.172.231;
4.P.172.236; 4.P.172.237; 4.P.172.238; 4.P.172.239; 4.P.172.154;
4.P.172.157; 4.P.172.166; 4.P.172.169; 4.P.172.172; 4.P.172.175;
4.P.172.240; 4.P.172.244; 4.P.175.228; 4.P.175.229; 4.P.175.230;
4.P.175.231; 4.P.175.236; 4.P.175.237; 4.P.175.238; 4.P.175.239;
4.P.175.154; 4.P.175.157; 4.P.175.166; 4.P.175.169; 4.P.175.172;
4.P.175.175; 4.P.175.240; 4.P.175.244; 4.P.240.228; 4.P.240.229;
4.P.240.230; 4.P.240.231; 4.P.240.236; 4.P.240.237; 4.P.240.238;
4.P.240.239; 4.P.240.154; 4.P.240.157; 4.P.240.166; 4.P.240.169;
4.P.240.172; 4.P.240.175; 4.P.240.240; 4.P.240.244; 4.P.244.228;
4.P.244.229; 4.P.244.230; 4.P.244.231; 4.P.244.236; 4.P.244.237;
4.P.244.238; 4.P.244.239; 4.P.244.154; 4.P.244.157; 4.P.244.166;
4.P.244.169; 4.P.244.172; 4.P.244.175; 4.P.244.240; 4.P.244.244;
Prodrugs of 4.U 4.U.228.228; 4.U.228.229; 4.U.228.230; 4.U.228.231;
4.U.228.236; 4.U.228.237; 4.U.228.238; 4.U.228.239; 4.U.228.154;
4.U.228.157; 4.U.228.166; 4.U.228.169; 4.U.228.172; 4.U.228.175;
4.U.228.240; 4.U.228.244; 4.U.229.228; 4.U.229.229; 4.U.229.230;
4.U.229.231; 4.U.229.236; 4.U.229.237; 4.U.229.238; 4.U.229.239;
4.U.229.154; 4.U.229.157; 4.U.229.166; 4.U.229.169; 4.U.229.172;
4.U.229.175; 4.U.229.240; 4.U.229.244; 4.U.230.228; 4.U.230.229;
4.U.230.230; 4.U.230.231; 4.U.230.236; 4.U.230.237; 4.U.230.238;
4.U.230.239; 4.U.230.154; 4.U.230.157; 4.U.230.166; 4.U.230.169;
4.U.230.172; 4.U.230.175; 4.U.230.240; 4.U.230.244; 4.U.231.228;
4.U.231.229; 4.U.231.230; 4.U.231.231; 4.U.231.236; 4.U.231.237;
4.U.231.238; 4.U.231.239; 4.U.231.154; 4.U.231.157; 4.U.231.166;
4.U.231.169; 4.U.231.172; 4.U.231.175; 4.U.231.240; 4.U.231.244;
4.U.236.228; 4.U.236.229; 4.U.236.230; 4.U.236.231; 4.U.236.236;
4.U.236.237; 4.U.236.238; 4.U.236.239; 4.U.236.154; 4.U.236.157;
4.U.236.166; 4.U.236.169; 4.U.236.172; 4.U.236.175; 4.U.236.240;
4.U.236.244; 4.U.237.228; 4.U.237.229; 4.U.237.230; 4.U.237.231;
4.U.237.236; 4.U.237.237; 4.U.237.238; 4.U.237.239; 4.U.237.154;
4.U.237.157; 4.U.237.166; 4.U.237.169; 4.U.237.172; 4.U.237.175;
4.U.237.240; 4.U.237.244; 4.U.238.228; 4.U.238.229; 4.U.238.230;
4.U.238.231; 4.U.238.236; 4.U.238.237; 4.U.238.238; 4.U.238.239;
4.U.238.154; 4.U.238.157; 4.U.238.166; 4.U.238.169; 4.U.238.172;
4.U.238.175; 4.U.238.240; 4.U.238.244; 4.U.239.228; 4.U.239.229;
4.U.239.230; 4.U.239.231; 4.U.239.236; 4.U.239.237; 4.U.239.238;
4.U.239.239; 4.U.239.154; 4.U.239.157; 4.U.239.166; 4.U.239.169;
4.U.239.172; 4.U.239.175; 4.U.239.240; 4.U.239.244; 4.U.154.228;
4.U.154.229; 4.U.154.230; 4.U.154.231; 4.U.154.236; 4.U.154.237;
4.U.154.238; 4.U.154.239; 4.U.154.154; 4.U.154.157; 4.U.154.166;
4.U.154.169; 4.U.154.172; 4.U.154.175; 4.U.154.240; 4.U.154.244;
4.U.157.228; 4.U.157.229; 4.U.157.230; 4.U.157.231; 4.U.157.236;
4.U.157.237; 4.U.157.238; 4.U.157.239; 4.U.157.154; 4.U.157.157;
4.U.157.166; 4.U.157.169; 4.U.157.172; 4.U.157.175; 4.U.157.240;
4.U.157.244; 4.U.166.228; 4.U.166.229; 4.U.166.230; 4.U.166.231;
4.U.166.236; 4.U.166.237; 4.U.166.238; 4.U.166.239; 4.U.166.154;
4.U.166.157; 4.U.166.166; 4.U.166.169; 4.U.166.172; 4.U.166.175;
4.U.166.240; 4.U.166.244; 4.U.169.228; 4.U.169.229; 4.U.169.230;
4.U.169.231; 4.U.169.236; 4.U.169.237; 4.U.169.238; 4.U.169.239;
4.U.169.154; 4.U.169.157; 4.U.169.166; 4.U.169.169; 4.U.169.172;
4.U.169.175; 4.U.169.240; 4.U.169.244; 4.U.172.228; 4.U.172.229;
4.U.172.230; 4.U.172.231; 4.U.172.236; 4.U.172.237; 4.U.172.238;
4.U.172.239; 4.U.172.154; 4.U.172.157; 4.U.172.166; 4.U.172.169;
4.U.172.172; 4.U.172.175; 4.U.172.240; 4.U.172.244; 4.U.175.228;
4.U.175.229; 4.U.175.230; 4.U.175.231; 4.U.175.236; 4.U.175.237;
4.U.175.238; 4.U.175.239; 4.U.175.154; 4.U.175.157; 4.U.175.166;
4.U.175.169; 4.U.175.172; 4.U.175.175; 4.U.175.240; 4.U.175.244;
4.U.240.228; 4.U.240.229; 4.U.240.230; 4.U.240.231; 4.U.240.236;
4.U.240.237; 4.U.240.238; 4.U.240.239; 4.U.240.154; 4.U.240.157;
4.U.240.166; 4.U.240.169; 4.U.240.172; 4.U.240.175; 4.U.240.240;
4.U.240.244; 4.U.244.228; 4.U.244.229; 4.U.244.230; 4.U.244.231;
4.U.244.236; 4.U.244.237; 4.U.244.238; 4.U.244.239; 4.U.244.154;
4.U.244.157; 4.U.244.166; 4.U.244.169; 4.U.244.172; 4.U.244.175;
4.U.244.240; 4.U.244.244; Prodrugs of 4.W 4.W.228.228; 4.W.228.229;
4.W.228.230; 4.W.228.231; 4.W.228.236; 4.W.228.237; 4.W.228.238;
4.W.228.239; 4.W.228.154; 4.W.228.157; 4.W.228.166; 4.W.228.169;
4.W.228.172; 4.W.228.175; 4.W.228.240; 4.W.228.244; 4.W.229.228;
4.W.229.229; 4.W.229.230; 4.W.229.231; 4.W.229.236; 4.W.229.237;
4.W.229.238; 4.W.229.239; 4.W.229.154; 4.W.229.157; 4.W.229.166;
4.W.229.169; 4.W.229.172; 4.W.229.175; 4.W.229.240; 4.W.229.244;
4.W.230.228; 4.W.230.229; 4.W.230.230; 4.W.230.231; 4.W.230.236;
4.W.230.237; 4.W.230.238; 4.W.230.239; 4.W.230.154; 4.W.230.157;
4.W.230.166; 4.W.230.169; 4.W.230.172; 4.W.230.175; 4.W.230.240;
4.W.230.244; 4.W.231.228; 4.W.231.229; 4.W.231.230; 4.W.231.231;
4.W.231.236; 4.W.231.237; 4.W.231.238; 4.W.231.239; 4.W.231.154;
4.W.231.157; 4.W.231.166; 4.W.231.169; 4.W.231.172; 4.W.231.175;
4.W.231.240; 4.W.231.244; 4.W.236.228; 4.W.236.229; 4.W.236.230;
4.W.236.231; 4.W.236.236; 4.W.236.237; 4.W.236.238; 4.W.236.239;
4.W.236.154; 4.W.236.157; 4.W.236.166; 4.W.236.169; 4.W.236.172;
4.W.236.175; 4.W.236.240; 4.W.236.244; 4.W.237.228; 4.W.237.229;
4.W.237.230; 4.W.237.231; 4.W.237.236; 4.W.237.237; 4.W.237.238;
4.W.237.239; 4.W.237.154; 4.W.237.157; 4.W.237.166; 4.W.237.169;
4.W.237.172; 4.W.237.175; 4.W.237.240; 4.W.237.244; 4.W.238.228;
4.W.238.229; 4.W.238.230; 4.W.238.231; 4.W.238.236; 4.W.238.237;
4.W.238.238; 4.W.238.239; 4.W.238.154; 4.W.238.157; 4.W.238.166;
4.W.238.169; 4.W.238.172; 4.W.238.175; 4.W.238.240; 4.W.238.244;
4.W.239.228; 4.W.239.229; 4.W.239.230; 4.W.239.231; 4.W.239.236;
4.W.239.237; 4.W.239.238; 4.W.239.239; 4.W.239.154; 4.W.239.157;
4.W.239.166; 4.W.239.169; 4.W.239.172; 4.W.239.175; 4.W.239.240;
4.W.239.244; 4.W.154.228; 4.W.154.229; 4.W.154.230; 4.W.154.231;
4.W.154.236; 4.W.154.237; 4.W.154.238; 4.W.154.239; 4.W.154.154;
4.W.154.157; 4.W.154.166; 4.W.154.169; 4.W.154.172; 4.W.154.175;
4.W.154.240; 4.W.154.244; 4.W.157.228; 4.W.157.229; 4.W.157.230;
4.W.157.231; 4.W.157.236; 4.W.157.237; 4.W.157.238; 4.W.157.239;
4.W.157.154; 4.W.157.157; 4.W.157.166; 4.W.157.169; 4.W.157.172;
4.W.157.175; 4.W.157.240; 4.W.157.244; 4.W.166.228; 4.W.166.229;
4.W.166.230; 4.W.166.231; 4.W.166.236; 4.W.166.237; 4.W.166.238;
4.W.166.239; 4.W.166.154; 4.W.166.157; 4.W.166.166; 4.W.166.169;
4.W.166.172; 4.W.166.175; 4.W.166.240; 4.W.166.244; 4.W.169.228;
4.W.169.229; 4.W.169.230; 4.W.169.231; 4.W.169.236; 4.W.169.237;
4.W.169.238; 4.W.169.239; 4.W.169.154; 4.W.169.157; 4.W.169.166;
4.W.169.169; 4.W.169.172; 4.W.169.175; 4.W.169.240; 4.W.169.244;
4.W.172.228; 4.W.172.229; 4.W.172.230; 4.W.172.231; 4.W.172.236;
4.W.172.237; 4.W.172.238; 4.W.172.239; 4.W.172.154; 4.W.172.157;
4.W.172.166; 4.W.172.169; 4.W.172.172; 4.W.172.175; 4.W.172.240;
4.W.172.244; 4.W.175.228; 4.W.175.229; 4.W.175.230; 4.W.175.231;
4.W.175.236; 4.W.175.237; 4.W.175.238; 4.W.175.239; 4.W.175.154;
4.W.175.157; 4.W.175.166; 4.W.175.169; 4.W.175.172; 4.W.175.175;
4.W.175.240; 4.W.175.244; 4.W.240.228; 4.W.240.229; 4.W.240.230;
4.W.240.231; 4.W.240.236; 4.W.240.237; 4.W.240.238; 4.W.240.239;
4.W.240.154; 4.W.240.157; 4.W.240.166; 4.W.240.169; 4.W.240.172;
4.W.240.175; 4.W.240.240; 4.W.240.244; 4.W.244.228; 4.W.244.229;
4.W.244.230; 4.W.244.231; 4.W.244.236; 4.W.244.237; 4.W.244.238;
4.W.244.239; 4.W.244.154; 4.W.244.157; 4.W.244.166; 4.W.244.169;
4.W.244.172; 4.W.244.175; 4.W.244.240; 4.W.244.244; Prodrugs of 4.Y
4.Y.228.228; 4.Y.228.229; 4.Y.228.230; 4.Y.228.231; 4.Y.228.236;
4.Y.228.237; 4.Y.228.238; 4.Y.228.239; 4.Y.228.154; 4.Y.228.157;
4.Y.228.166; 4.Y.228.169; 4.Y.228.172; 4.Y.228.175; 4.Y.228.240;
4.Y.228.244; 4.Y.229.228; 4.Y.229.229; 4.Y.229.230; 4.Y.229.231;
4.Y.229.236; 4.Y.229.237; 4.Y.229.238; 4.Y.229.239; 4.Y.229.154;
4.Y.229.157; 4.Y.229.166; 4.Y.229.169; 4.Y.229.172; 4.Y.229.175;
4.Y.229.240; 4.Y.229.244; 4.Y.230.228; 4.Y.230.229; 4.Y.230.230;
4.Y.230.231; 4.Y.230.236; 4.Y.230.237; 4.Y.230.238; 4.Y.230.239;
4.Y.230.154; 4.Y.230.157; 4.Y.230.166; 4.Y.230.169; 4.Y.230.172;
4.Y.230.175; 4.Y.230.240; 4.Y.230.244; 4.Y.231.228; 4.Y.231.229;
4.Y.231.230; 4.Y.231.231; 4.Y.231.236; 4.Y.231.237; 4.Y.231.238;
4.Y.231.239; 4.Y.231.154; 4.Y.231.157; 4.Y.231.166; 4.Y.231.169;
4.Y.231.172; 4.Y.231.175; 4.Y.231.240; 4.Y.231.244; 4.Y.236.228;
4.Y.236.229; 4.Y.236.230; 4.Y.236.231; 4.Y.236.236; 4.Y.236.237;
4.Y.236.238; 4.Y.236.239; 4.Y.236.154; 4.Y.236.157;
4.Y.236.166;
4.Y.236.169; 4.Y.236.172; 4.Y.236.175; 4.Y.236.240; 4.Y.236.244;
4.Y.237.228; 4.Y.237.229; 4.Y.237.230; 4.Y.237.231; 4.Y.237.236;
4.Y.237.237; 4.Y.237.238; 4.Y.237.239; 4.Y.237.154; 4.Y.237.157;
4.Y.237.166; 4.Y.237.169; 4.Y.237.172; 4.Y.237.175; 4.Y.237.240;
4.Y.237.244; 4.Y.238.228; 4.Y.238.229; 4.Y.238.230; 4.Y.238.231;
4.Y.238.236; 4.Y.238.237; 4.Y.238.238; 4.Y.238.239; 4.Y.238.154;
4.Y.238.157; 4.Y.238.166; 4.Y.238.169; 4.Y.238.172; 4.Y.238.175;
4.Y.238.240; 4.Y.238.244; 4.Y.239.228; 4.Y.239.229; 4.Y.239.230;
4.Y.239.231; 4.Y.239.236; 4.Y.239.237; 4.Y.239.238; 4.Y.239.239;
4.Y.239.154; 4.Y.239.157; 4.Y.239.166; 4.Y.239.169; 4.Y.239.172;
4.Y.239.175; 4.Y.239.240; 4.Y.239.244; 4.Y.154.228; 4.Y.154.229;
4.Y.154.230; 4.Y.154.231; 4.Y.154.236; 4.Y.154.237; 4.Y.154.238;
4.Y.154.239; 4.Y.154.154; 4.Y.154.157; 4.Y.154.166; 4.Y.154.169;
4.Y.154.172; 4.Y.154.175; 4.Y.154.240; 4.Y.154.244; 4.Y.157.228;
4.Y.157.229; 4.Y.157.230; 4.Y.157.231; 4.Y.157.236; 4.Y.157.237;
4.Y.157.238; 4.Y.157.239; 4.Y.157.154; 4.Y.157.157; 4.Y.157.166;
4.Y.157.169; 4.Y.157.172; 4.Y.157.175; 4.Y.157.240; 4.Y.157.244;
4.Y.166.228; 4.Y.166.229; 4.Y.166.230; 4.Y.166.231; 4.Y.166.236;
4.Y.166.237; 4.Y.166.238; 4.Y.166.239; 4.Y.166.154; 4.Y.166.157;
4.Y.166.166; 4.Y.166.169; 4.Y.166.172; 4.Y.166.175; 4.Y.166.240;
4.Y.166.244; 4.Y.169.228; 4.Y.169.229; 4.Y.169.230; 4.Y.169.231;
4.Y.169.236; 4.Y.169.237; 4.Y.169.238; 4.Y.169.239; 4.Y.169.154;
4.Y.169.157; 4.Y.169.166; 4.Y.169.169; 4.Y.169.172; 4.Y.169.175;
4.Y.169.240; 4.Y.169.244; 4.Y.172.228; 4.Y.172.229; 4.Y.172.230;
4.Y.172.231; 4.Y.172.236; 4.Y.172.237; 4.Y.172.238; 4.Y.172.239;
4.Y.172.154; 4.Y.172.157; 4.Y.172.166; 4.Y.172.169; 4.Y.172.172;
4.Y.172.175; 4.Y.172.240; 4.Y.172.244; 4.Y.175.228; 4.Y.175.229;
4.Y.175.230; 4.Y.175.231; 4.Y.175.236; 4.Y.175.237; 4.Y.175.238;
4.Y.175.239; 4.Y.175.154; 4.Y.175.157; 4.Y.175.166; 4.Y.175.169;
4.Y.175.172; 4.Y.175.175; 4.Y.175.240; 4.Y.175.244; 4.Y.240.228;
4.Y.240.229; 4.Y.240.230; 4.Y.240.231; 4.Y.240.236; 4.Y.240.237;
4.Y.240.238; 4.Y.240.239; 4.Y.240.154; 4.Y.240.157; 4.Y.240.166;
4.Y.240.169; 4.Y.240.172; 4.Y.240.175; 4.Y.240.240; 4.Y.240.244;
4.Y.244.228; 4.Y.244.229; 4.Y.244.230; 4.Y.244.231; 4.Y.244.236;
4.Y.244.237; 4.Y.244.238; 4.Y.244.239; 4.Y.244.154; 4.Y.244.157;
4.Y.244.166; 4.Y.244.169; 4.Y.244.172; 4.Y.244.175; 4.Y.244.240;
4.Y.244.244; Prodrugs of 5.B 5.B.228.228; 5.B.228.229; 5.B.228.230;
5.B.228.231; 5.B.228.236; 5.B.228.237; 5.B.228.238; 5.B.228.239;
5.B.228.154; 5.B.228.157; 5.B.228.166; 5.B.228.169; 5.B.228.172;
5.B.228.175; 5.B.228.240; 5.B.228.244; 5.B.229.228; 5.B.229.229;
5.B.229.230; 5.B.229.231; 5.B.229.236; 5.B.229.237; 5.B.229.238;
5.B.229.239; 5.B.229.154; 5.B.229.157; 5.B.229.166; 5.B.229.169;
5.B.229.172; 5.B.229.175; 5.B.229.240; 5.B.229.244; 5.B.230.228;
5.B.230.229; 5.B.230.230; 5.B.230.231; 5.B.230.236; 5.B.230.237;
5.B.230.238; 5.B.230.239; 5.B.230.154; 5.B.230.157; 5.B.230.166;
5.B.230.169; 5.B.230.172; 5.B.230.175; 5.B.230.240; 5.B.230.244;
5.B.231.228; 5.B.231.229; 5.B.231.230; 5.B.231.231; 5.B.231.236;
5.B.231.237; 5.B.231.238; 5.B.231.239; 5.B.231.154; 5.B.231.157;
5.B.231.166; 5.B.231.169; 5.B.231.172; 5.B.231.175; 5.B.231.240;
5.B.231.244; 5.B.236.228; 5.B.236.229; 5.B.236.230; 5.B.236.231;
5.B.236.236; 5.B.236.237; 5.B.236.238; 5.B.236.239; 5.B.236.154;
5.B.236.157; 5.B.236.166; 5.B.236.169; 5.B.236.172; 5.B.236.175;
5.B.236.240; 5.B.236.244; 5.B.237.228; 5.B.237.229; 5.B.237.230;
5.B.237.231; 5.B.237.236; 5.B.237.237; 5.B.237.238; 5.B.237.239;
5.B.237.154; 5.B.237.157; 5.B.237.166; 5.B.237.169; 5.B.237.172;
5.B.237.175; 5.B.237.240; 5.B.237.244; 5.B.238.228; 5.B.238.229;
5.B.238.230; 5.B.238.231; 5.B.238.236; 5.B.238.237; 5.B.238.238;
5.B.238.239; 5.B.238.154; 5.B.238.157; 5.B.238.166; 5.B.238.169;
5.B.238.172; 5.B.238.175; 5.B.238.240; 5.B.238.244; 5.B.239.228;
5.B.239.229; 5.B.239.230; 5.B.239.231; 5.B.239.236; 5.B.239.237;
5.B.239.238; 5.B.239.239; 5.B.239.154; 5.B.239.157; 5.B.239.166;
5.B.239.169; 5.B.239.172; 5.B.239.175; 5.B.239.240; 5.B.239.244;
5.B.154.228; 5.B.154.229; 5.B.154.230; 5.B.154.231; 5.B.154.236;
5.B.154.237; 5.B.154.238; 5.B.154.239; 5.B.154.154; 5.B.154.157;
5.B.154.166; 5.B.154.169; 5.B.154.172; 5.B.154.175; 5.B.154.240;
5.B.154.244; 5.B.157.228; 5.B.157.229; 5.B.157.230; 5.B.157.231;
5.B.157.236; 5.B.157.237; 5.B.157.238; 5.B.157.239; 5.B.157.154;
5.B.157.157; 5.B.157.166; 5.B.157.169; 5.B.157.172; 5.B.157.175;
5.B.157.240; 5.B.157.244; 5.B.166.228; 5.B.166.229; 5.B.166.230;
5.B.166.231; 5.B.166.236; 5.B.166.237; 5.B.166.238; 5.B.166.239;
5.B.166.154; 5.B.166.157; 5.B.166.166; 5.B.166.169; 5.B.166.172;
5.B.166.175; 5.B.166.240; 5.B.166.244; 5.B.169.228; 5.B.169.229;
5.B.169.230; 5.B.169.231; 5.B.169.236; 5.B.169.237; 5.B.169.238;
5.B.169.239; 5.B.169.154; 5.B.169.157; 5.B.169.166; 5.B.169.169;
5.B.169.172; 5.B.169.175; 5.B.169.240; 5.B.169.244; 5.B.172.228;
5.B.172.229; 5.B.172.230; 5.B.172.231; 5.B.172.236; 5.B.172.237;
5.B.172.238; 5.B.172.239; 5.B.172.154; 5.B.172.157; 5.B.172.166;
5.B.172.169; 5.B.172.172; 5.B.172.175; 5.B.172.240; 5.B.172.244;
5.B.175.228; 5.B.175.229; 5.B.175.230; 5.B.175.231; 5.B.175.236;
5.B.175.237; 5.B.175.238; 5.B.175.239; 5.B.175.154; 5.B.175.157;
5.B.175.166; 5.B.175.169; 5.B.175.172; 5.B.175.175; 5.B.175.240;
5.B.175.244; 5.B.240.228; 5.B.240.229; 5.B.240.230; 5.B.240.231;
5.B.240.236; 5.B.240.237; 5.B.240.238; 5.B.240.239; 5.B.240.154;
5.B.240.157; 5.B.240.166; 5.B.240.169; 5.B.240.172; 5.B.240.175;
5.B.240.240; 5.B.240.244; 5.B.244.228; 5.B.244.229; 5.B.244.230;
5.B.244.231; 5.B.244.236; 5.B.244.237; 5.B.244.238; 5.B.244.239;
5.B.244.154; 5.B.244.157; 5.B.244.166; 5.B.244.169; 5.B.244.172;
5.B.244.175; 5.B.244.240; 5.B.244.244; Prodrugs of 5.D 5.D.228.228;
5.D.228.229; 5.D.228.230; 5.D.228.231; 5.D.228.236; 5.D.228.237;
5.D.228.238; 5.D.228.239; 5.D.228.154; 5.D.228.157; 5.D.228.166;
5.D.228.169; 5.D.228.172; 5.D.228.175; 5.D.228.240; 5.D.228.244;
5.D.229.228; 5.D.229.229; 5.D.229.230; 5.D.229.231; 5.D.229.236;
5.D.229.237; 5.D.229.238; 5.D.229.239; 5.D.229.154; 5.D.229.157;
5.D.229.166; 5.D.229.169; 5.D.229.172; 5.D.229.175; 5.D.229.240;
5.D.229.244; 5.D.230.228; 5.D.230.229; 5.D.230.230; 5.D.230.231;
5.D.230.236; 5.D.230.237; 5.D.230.238; 5.D.230.239; 5.D.230.154;
5.D.230.157; 5.D.230.166; 5.D.230.169; 5.D.230.172; 5.D.230.175;
5.D.230.240; 5.D.230.244; 5.D.231.228; 5.D.231.229; 5.D.231.230;
5.D.231.231; 5.D.231.236; 5.D.231.237; 5.D.231.238; 5.D.231.239;
5.D.231.154; 5.D.231.157; 5.D.231.166; 5.D.231.169; 5.D.231.172;
5.D.231.175; 5.D.231.240; 5.D.231.244; 5.D.236.228; 5.D.236.229;
5.D.236.230; 5.D.236.231; 5.D.236.236; 5.D.236.237; 5.D.236.238;
5.D.236.239; 5.D.236.154; 5.D.236.157; 5.D.236.166; 5.D.236.169;
5.D.236.172; 5.D.236.175; 5.D.236.240; 5.D.236.244; 5.D.237.228;
5.D.237.229; 5.D.237.230; 5.D.237.231; 5.D.237.236; 5.D.237.237;
5.D.237.238; 5.D.237.239; 5.D.237.154; 5.D.237.157; 5.D.237.166;
5.D.237.169; 5.D.237.172; 5.D.237.175; 5.D.237.240; 5.D.237.244;
5.D.238.228; 5.D.238.229; 5.D.238.230; 5.D.238.231; 5.D.238.236;
5.D.238.237; 5.D.238.238; 5.D.238.239; 5.D.238.154; 5.D.238.157;
5.D.238.166; 5.D.238.169; 5.D.238.172; 5.D.238.175; 5.D.238.240;
5.D.238.244; 5.D.239.228; 5.D.239.229; 5.D.239.230; 5.D.239.231;
5.D.239.236; 5.D.239.237; 5.D.239.238; 5.D.239.239; 5.D.239.154;
5.D.239.157; 5.D.239.166; 5.D.239.169; 5.D.239.172; 5.D.239.175;
5.D.239.240; 5.D.239.244; 5.D.154.228; 5.D.154.229; 5.D.154.230;
5.D.154.231; 5.D.154.236; 5.D.154.237; 5.D.154.238; 5.D.154.239;
5.D.154.154; 5.D.154.157; 5.D.154.166; 5.D.154.169; 5.D.154.172;
5.D.154.175; 5.D.154.240; 5.D.154.244; 5.D.157.228; 5.D.157.229;
5.D.157.230; 5.D.157.231; 5.D.157.236; 5.D.157.237; 5.D.157.238;
5.D.157.239; 5.D.157.154; 5.D.157.157; 5.D.157.166; 5.D.157.169;
5.D.157.172; 5.D.157.175; 5.D.157.240; 5.D.157.244; 5.D.166.228;
5.D.166.229; 5.D.166.230; 5.D.166.231; 5.D.166.236; 5.D.166.237;
5.D.166.238; 5.D.166.239; 5.D.166.154; 5.D.166.157; 5.D.166.166;
5.D.166.169; 5.D.166.172; 5.D.166.175; 5.D.166.240; 5.D.166.244;
5.D.169.228; 5.D.169.229; 5.D.169.230; 5.D.169.231; 5.D.169.236;
5.D.169.237; 5.D.169.238; 5.D.169.239; 5.D.169.154; 5.D.169.157;
5.D.169.166; 5.D.169.169; 5.D.169.172; 5.D.169.175; 5.D.169.240;
5.D.169.244; 5.D.172.228; 5.D.172.229; 5.D.172.230; 5.D.172.231;
5.D.172.236; 5.D.172.237; 5.D.172.238; 5.D.172.239; 5.D.172.154;
5.D.172.157; 5.D.172.166; 5.D.172.169; 5.D.172.172; 5.D.172.175;
5.D.172.240; 5.D.172.244; 5.D.175.228; 5.D.175.229; 5.D.175.230;
5.D.175.231; 5.D.175.236; 5.D.175.237; 5.D.175.238; 5.D.175.239;
5.D.175.154; 5.D.175.157; 5.D.175.166; 5.D.175.169; 5.D.175.172;
5.D.175.175; 5.D.175.240; 5.D.175.244; 5.D.240.228; 5.D.240.229;
5.D.240.230; 5.D.240.231; 5.D.240.236; 5.D.240.237; 5.D.240.238;
5.D.240.239; 5.D.240.154; 5.D.240.157; 5.D.240.166; 5.D.240.169;
5.D.240.172; 5.D.240.175; 5.D.240.240; 5.D.240.244; 5.D.244.228;
5.D.244.229; 5.D.244.230; 5.D.244.231; 5.D.244.236; 5.D.244.237;
5.D.244.238; 5.D.244.239; 5.D.244.154; 5.D.244.157; 5.D.244.166;
5.D.244.169; 5.D.244.172; 5.D.244.175; 5.D.244.240; 5.D.244.244;
Prodrugs of 5.E 5.E.228.228; 5.E.228.229; 5.E.228.230; 5.E.228.231;
5.E.228.236; 5.E.228.237; 5.E.228.238; 5.E.228.239; 5.E.228.154;
5.E.228.157; 5.E.228.166; 5.E.228.169; 5.E.228.172; 5.E.228.175;
5.E.228.240; 5.E.228.244; 5.E.229.228; 5.E.229.229; 5.E.229.230;
5.E.229.231; 5.E.229.236; 5.E.229.237; 5.E.229.238; 5.E.229.239;
5.E.229.154; 5.E.229.157; 5.E.229.166; 5.E.229.169; 5.E.229.172;
5.E.229.175; 5.E.229.240; 5.E.229.244; 5.E.230.228; 5.E.230.229;
5.E.230.230; 5.E.230.231; 5.E.230.236; 5.E.230.237; 5.E.230.238;
5.E.230.239; 5.E.230.154; 5.E.230.157; 5.E.230.166; 5.E.230.169;
5.E.230.172; 5.E.230.175; 5.E.230.240; 5.E.230.244; 5.E.231.228;
5.E.231.229; 5.E.231.230; 5.E.231.231; 5.E.231.236; 5.E.231.237;
5.E.231.238; 5.E.231.239; 5.E.231.154; 5.E.231.157; 5.E.231.166;
5.E.231.169; 5.E.231.172; 5.E.231.175; 5.E.231.240; 5.E.231.244;
5.E.236.228; 5.E.236.229; 5.E.236.230; 5.E.236.231; 5.E.236.236;
5.E.236.237; 5.E.236.238; 5.E.236.239; 5.E.236.154; 5.E.236.157;
5.E.236.166; 5.E.236.169; 5.E.236.172; 5.E.236.175; 5.E.236.240;
5.E.236.244; 5.E.237.228; 5.E.237.229; 5.E.237.230; 5.E.237.231;
5.E.237.236; 5.E.237.237; 5.E.237.238; 5.E.237.239; 5.E.237.154;
5.E.237.157; 5.E.237.166; 5.E.237.169; 5.E.237.172; 5.E.237.175;
5.E.237.240; 5.E.237.244; 5.E.238.228; 5.E.238.229; 5.E.238.230;
5.E.238.231; 5.E.238.236; 5.E.238.237; 5.E.238.238; 5.E.238.239;
5.E.238.154; 5.E.238.157; 5.E.238.166; 5.E.238.169; 5.E.238.172;
5.E.238.175; 5.E.238.240; 5.E.238.244; 5.E.239.228; 5.E.239.229;
5.E.239.230; 5.E.239.231; 5.E.239.236; 5.E.239.237; 5.E.239.238;
5.E.239.239; 5.E.239.154; 5.E.239.157; 5.E.239.166; 5.E.239.169;
5.E.239.172; 5.E.239.175; 5.E.239.240; 5.E.239.244; 5.E.154.228;
5.E.154.229; 5.E.154.230; 5.E.154.231; 5.E.154.236; 5.E.154.237;
5.E.154.238; 5.E.154.239; 5.E.154.154; 5.E.154.157; 5.E.154.166;
5.E.154.169; 5.E.154.172; 5.E.154.175; 5.E.154.240; 5.E.154.244;
5.E.157.228; 5.E.157.229; 5.E.157.230; 5.E.157.231; 5.E.157.236;
5.E.157.237; 5.E.157.238; 5.E.157.239; 5.E.157.154; 5.E.157.157;
5.E.157.166; 5.E.157.169; 5.E.157.172; 5.E.157.175; 5.E.157.240;
5.E.157.244; 5.E.166.228; 5.E.166.229; 5.E.166.230; 5.E.166.231;
5.E.166.236; 5.E.166.237; 5.E.166.238; 5.E.166.239; 5.E.166.154;
5.E.166.157; 5.E.166.166; 5.E.166.169; 5.E.166.172; 5.E.166.175;
5.E.166.240; 5.E.166.244; 5.E.169.228; 5.E.169.229; 5.E.169.230;
5.E.169.231; 5.E.169.236; 5.E.169.237; 5.E.169.238; 5.E.169.239;
5.E.169.154; 5.E.169.157; 5.E.169.166; 5.E.169.169; 5.E.169.172;
5.E.169.175; 5.E.169.240; 5.E.169.244; 5.E.172.228; 5.E.172.229;
5.E.172.230; 5.E.172.231; 5.E.172.236; 5.E.172.237; 5.E.172.238;
5.E.172.239; 5.E.172.154; 5.E.172.157; 5.E.172.166; 5.E.172.169;
5.E.172.172; 5.E.172.175; 5.E.172.240; 5.E.172.244; 5.E.175.228;
5.E.175.229; 5.E.175.230; 5.E.175.231; 5.E.175.236; 5.E.175.237;
5.E.175.238; 5.E.175.239; 5.E.175.154; 5.E.175.157; 5.E.175.166;
5.E.175.169; 5.E.175.172; 5.E.175.175; 5.E.175.240; 5.E.175.244;
5.E.240.228; 5.E.240.229; 5.E.240.230; 5.E.240.231; 5.E.240.236;
5.E.240.237; 5.E.240.238; 5.E.240.239; 5.E.240.154; 5.E.240.157;
5.E.240.166; 5.E.240.169; 5.E.240.172; 5.E.240.175; 5.E.240.240;
5.E.240.244; 5.E.244.228; 5.E.244.229; 5.E.244.230; 5.E.244.231;
5.E.244.236; 5.E.244.237; 5.E.244.238; 5.E.244.239; 5.E.244.154;
5.E.244.157; 5.E.244.166; 5.E.244.169; 5.E.244.172; 5.E.244.175;
5.E.244.240; 5.E.244.244; Prodrugs of 5.G 5.G.228.228; 5.G.228.229;
5.G.228.230; 5.G.228.231; 5.G.228.236; 5.G.228.237; 5.G.228.238;
5.G.228.239; 5.G.228.154; 5.G.228.157; 5.G.228.166; 5.G.228.169;
5.G.228.172; 5.G.228.175; 5.G.228.240; 5.G.228.244; 5.G.229.228;
5.G.229.229; 5.G.229.230; 5.G.229.231; 5.G.229.236; 5.G.229.237;
5.G.229.238; 5.G.229.239; 5.G.229.154; 5.G.229.157; 5.G.229.166;
5.G.229.169; 5.G.229.172; 5.G.229.175; 5.G.229.240; 5.G.229.244;
5.G.230.228; 5.G.230.229; 5.G.230.230; 5.G.230.231; 5.G.230.236;
5.G.230.237; 5.G.230.238; 5.G.230.239; 5.G.230.154; 5.G.230.157;
5.G.230.166; 5.G.230.169; 5.G.230.172; 5.G.230.175; 5.G.230.240;
5.G.230.244; 5.G.231.228; 5.G.231.229; 5.G.231.230; 5.G.231.231;
5.G.231.236; 5.G.231.237; 5.G.231.238; 5.G.231.239; 5.G.231.154;
5.G.231.157; 5.G.231.166; 5.G.231.169; 5.G.231.172; 5.G.231.175;
5.G.231.240; 5.G.231.244; 5.G.236.228; 5.G.236.229; 5.G.236.230;
5.G.236.231; 5.G.236.236; 5.G.236.237; 5.G.236.238; 5.G.236.239;
5.G.236.154; 5.G.236.157; 5.G.236.166; 5.G.236.169; 5.G.236.172;
5.G.236.175; 5.G.236.240; 5.G.236.244; 5.G.237.228; 5.G.237.229;
5.G.237.230; 5.G.237.231; 5.G.237.236; 5.G.237.237; 5.G.237.238;
5.G.237.239; 5.G.237.154; 5.G.237.157; 5.G.237.166; 5.G.237.169;
5.G.237.172; 5.G.237.175; 5.G.237.240; 5.G.237.244; 5.G.238.228;
5.G.238.229; 5.G.238.230; 5.G.238.231; 5.G.238.236; 5.G.238.237;
5.G.238.238; 5.G.238.239; 5.G.238.154; 5.G.238.157; 5.G.238.166;
5.G.238.169; 5.G.238.172; 5.G.238.175; 5.G.238.240; 5.G.238.244;
5.G.239.228; 5.G.239.229; 5.G.239.230; 5.G.239.231; 5.G.239.236;
5.G.239.237; 5.G.239.238; 5.G.239.239; 5.G.239.154; 5.G.239.157;
5.G.239.166; 5.G.239.169; 5.G.239.172; 5.G.239.175; 5.G.239.240;
5.G.239.244; 5.G.154.228; 5.G.154.229; 5.G.154.230; 5.G.154.231;
5.G.154.236; 5.G.154.237; 5.G.154.238; 5.G.154.239; 5.G.154.154;
5.G.154.157; 5.G.154.166; 5.G.154.169; 5.G.154.172; 5.G.154.175;
5.G.154.240; 5.G.154.244; 5.G.157.228; 5.G.157.229; 5.G.157.230;
5.G.157.231; 5.G.157.236; 5.G.157.237; 5.G.157.238; 5.G.157.239;
5.G.157.154; 5.G.157.157; 5.G.157.166; 5.G.157.169; 5.G.157.172;
5.G.157.175; 5.G.157.240; 5.G.157.244; 5.G.166.228; 5.G.166.229;
5.G.166.230; 5.G.166.231; 5.G.166.236; 5.G.166.237; 5.G.166.238;
5.G.166.239; 5.G.166.154; 5.G.166.157; 5.G.166.166; 5.G.166.169;
5.G.166.172; 5.G.166.175; 5.G.166.240; 5.G.166.244; 5.G.169.228;
5.G.169.229; 5.G.169.230; 5.G.169.231; 5.G.169.236; 5.G.169.237;
5.G.169.238; 5.G.169.239; 5.G.169.154; 5.G.169.157; 5.G.169.166;
5.G.169.169; 5.G.169.172; 5.G.169.175; 5.G.169.240; 5.G.169.244;
5.G.172.228; 5.G.172.229; 5.G.172.230; 5.G.172.231; 5.G.172.236;
5.G.172.237; 5.G.172.238; 5.G.172.239; 5.G.172.154; 5.G.172.157;
5.G.172.166; 5.G.172.169; 5.G.172.172; 5.G.172.175; 5.G.172.240;
5.G.172.244; 5.G.175.228; 5.G.175.229; 5.G.175.230; 5.G.175.231;
5.G.175.236; 5.G.175.237; 5.G.175.238; 5.G.175.239; 5.G.175.154;
5.G.175.157; 5.G.175.166; 5.G.175.169; 5.G.175.172; 5.G.175.175;
5.G.175.240; 5.G.175.244; 5.G.240.228; 5.G.240.229; 5.G.240.230;
5.G.240.231; 5.G.240.236; 5.G.240.237; 5.G.240.238; 5.G.240.239;
5.G.240.154; 5.G.240.157; 5.G.240.166; 5.G.240.169; 5.G.240.172;
5.G.240.175; 5.G.240.240; 5.G.240.244; 5.G.244.228; 5.G.244.229;
5.G.244.230; 5.G.244.231; 5.G.244.236; 5.G.244.237; 5.G.244.238;
5.G.244.239; 5.G.244.154; 5.G.244.157; 5.G.244.166; 5.G.244.169;
5.G.244.172; 5.G.244.175; 5.G.244.240; 5.G.244.244; Prodrugs of 5.I
5.I.228.228; 5.I.228.229; 5.I.228.230; 5.I.228.231;
5.I.228.236;
5.I.228.237; 5.I.228.238; 5.I.228.239; 5.I.228.154; 5.I.228.157;
5.I.228.166; 5.I.228.169; 5.I.228.172; 5.I.228.175; 5.I.228.240;
5.I.228.244; 5.I.229.228; 5.I.229.229; 5.I.229.230; 5.I.229.231;
5.I.229.236; 5.I.229.237; 5.I.229.238; 5.I.229.239; 5.I.229.154;
5.I.229.157; 5.I.229.166; 5.I.229.169; 5.I.229.172; 5.I.229.175;
5.I.229.240; 5.I.229.244; 5.I.230.228; 5.I.230.229; 5.I.230.230;
5.I.230.231; 5.I.230.236; 5.I.230.237; 5.I.230.238; 5.I.230.239;
5.I.230.154; 5.I.230.157; 5.I.230.166; 5.I.230.169; 5.I.230.172;
5.I.230.175; 5.I.230.240; 5.I.230.244; 5.I.231.228; 5.I.231.229;
5.I.231.230; 5.I.231.231; 5.I.231.236; 5.I.231.237; 5.I.231.238;
5.I.231.239; 5.I.231.154; 5.I.231.157; 5.I.231.166; 5.I.231.169;
5.I.231.172; 5.I.231.175; 5.I.231.240; 5.I.231.244; 5.I.236.228;
5.I.236.229; 5.I.236.230; 5.I.236.231; 5.I.236.236; 5.I.236.237;
5.I.236.238; 5.I.236.239; 5.I.236.154; 5.I.236.157; 5.I.236.166;
5.I.236.169; 5.I.236.172; 5.I.236.175; 5.I.236.240; 5.I.236.244;
5.I.237.228; 5.I.237.229; 5.I.237.230; 5.I.237.231; 5.I.237.236;
5.I.237.237; 5.I.237.238; 5.I.237.239; 5.I.237.154; 5.I.237.157;
5.I.237.166; 5.I.237.169; 5.I.237.172; 5.I.237.175; 5.I.237.240;
5.I.237.244; 5.I.238.228; 5.I.238.229; 5.I.238.230; 5.I.238.231;
5.I.238.236; 5.I.238.237; 5.I.238.238; 5.I.238.239; 5.I.238.154;
5.I.238.157; 5.I.238.166; 5.I.238.169; 5.I.238.172; 5.I.238.175;
5.I.238.240; 5.I.238.244; 5.I.239.228; 5.I.239.229; 5.I.239.230;
5.I.239.231; 5.I.239.236; 5.I.239.237; 5.I.239.238; 5.I.239.239;
5.I.239.154; 5.I.239.157; 5.I.239.166; 5.I.239.169; 5.I.239.172;
5.I.239.175; 5.I.239.240; 5.I.239.244; 5.I.154.228; 5.I.154.229;
5.I.154.230; 5.I.154.231; 5.I.154.236; 5.I.154.237; 5.I.154.238;
5.I.154.239; 5.I.154.154; 5.I.154.157; 5.I.154.166; 5.I.154.169;
5.I.154.172; 5.I.154.175; 5.I.154.240; 5.I.154.244; 5.I.157.228;
5.I.157.229; 5.I.157.230; 5.I.157.231; 5.I.157.236; 5.I.157.237;
5.I.157.238; 5.I.157.239; 5.I.157.154; 5.I.157.157; 5.I.157.166;
5.I.157.169; 5.I.157.172; 5.I.157.175; 5.I.157.240; 5.I.157.244;
5.I.166.228; 5.I.166.229; 5.I.166.230; 5.I.166.231; 5.I.166.236;
5.I.166.237; 5.I.166.238; 5.I.166.239; 5.I.166.154; 5.I.166.157;
5.I.166.166; 5.I.166.169; 5.I.166.172; 5.I.166.175; 5.I.166.240;
5.I.166.244; 5.I.169.228; 5.I.169.229; 5.I.169.230; 5.I.169.231;
5.I.169.236; 5.I.169.237; 5.I.169.238; 5.I.169.239; 5.I.169.154;
5.I.169.157; 5.I.169.166; 5.I.169.169; 5.I.169.172; 5.I.169.175;
5.I.169.240; 5.I.169.244; 5.I.172.228; 5.I.172.229; 5.I.172.230;
5.I.172.231; 5.I.172.236; 5.I.172.237; 5.I.172.238; 5.I.172.239;
5.I.172.154; 5.I.172.157; 5.I.172.166; 5.I.172.169; 5.I.172.172;
5.I.172.175; 5.I.172.240; 5.I.172.244; 5.I.175.228; 5.I.175.229;
5.I.175.230; 5.I.175.231; 5.I.175.236; 5.I.175.237; 5.I.175.238;
5.I.175.239; 5.I.175.154; 5.I.175.157; 5.I.175.166; 5.I.175.169;
5.I.175.172; 5.I.175.175; 5.I.175.240; 5.I.175.244; 5.I.240.228;
5.I.240.229; 5.I.240.230; 5.I.240.231; 5.I.240.236; 5.I.240.237;
5.I.240.238; 5.I.240.239; 5.I.240.154; 5.I.240.157; 5.I.240.166;
5.I.240.169; 5.I.240.172; 5.I.240.175; 5.I.240.240; 5.I.240.244;
5.I.244.228; 5.I.244.229; 5.I.244.230; 5.I.244.231; 5.I.244.236;
5.I.244.237; 5.I.244.238; 5.I.244.239; 5.I.244.154; 5.I.244.157;
5.I.244.166; 5.I.244.169; 5.I.244.172; 5.I.244.175; 5.I.244.240;
5.I.244.244; Prodrugs of 5.J 5.J.228.228; 5.J.228.229; 5.J.228.230;
5.J.228.231; 5.J.228.236; 5.J.228.237; 5.J.228.238; 5.J.228.239;
5.J.228.154; 5.J.228.157; 5.J.228.166; 5.J.228.169; 5.J.228.172;
5.J.228.175; 5.J.228.240; 5.J.228.244; 5.J.229.228; 5.J.229.229;
5.J.229.230; 5.J.229.231; 5.J.229.236; 5.J.229.237; 5.J.229.238;
5.J.229.239; 5.J.229.154; 5.J.229.157; 5.J.229.166; 5.J.229.169;
5.J.229.172; 5.J.229.175; 5.J.229.240; 5.J.229.244; 5.J.230.228;
5.J.230.229; 5.J.230.230; 5.J.230.231; 5.J.230.236; 5.J.230.237;
5.J.230.238; 5.J.230.239; 5.J.230.154; 5.J.230.157; 5.J.230.166;
5.J.230.169; 5.J.230.172; 5.J.230.175; 5.J.230.240; 5.J.230.244;
5.J.231.228; 5.J.231.229; 5.J.231.230; 5.J.231.231; 5.J.231.236;
5.J.231.237; 5.J.231.238; 5.J.231.239; 5.J.231.154; 5.J.231.157;
5.J.231.166; 5.J.231.169; 5.J.231.172; 5.J.231.175; 5.J.231.240;
5.J.231.244; 5.J.236.228; 5.J.236.229; 5.J.236.230; 5.J.236.231;
5.J.236.236; 5.J.236.237; 5.J.236.238; 5.J.236.239; 5.J.236.154;
5.J.236.157; 5.J.236.166; 5.J.236.169; 5.J.236.172; 5.J.236.175;
5.J.236.240; 5.J.236.244; 5.J.237.228; 5.J.237.229; 5.J.237.230;
5.J.237.231; 5.J.237.236; 5.J.237.237; 5.J.237.238; 5.J.237.239;
5.J.237.154; 5.J.237.157; 5.J.237.166; 5.J.237.169; 5.J.237.172;
5.J.237.175; 5.J.237.240; 5.J.237.244; 5.J.238.228; 5.J.238.229;
5.J.238.230; 5.J.238.231; 5.J.238.236; 5.J.238.237; 5.J.238.238;
5.J.238.239; 5.J.238.154; 5.J.238.157; 5.J.238.166; 5.J.238.169;
5.J.238.172; 5.J.238.175; 5.J.238.240; 5.J.238.244; 5.J.239.228;
5.J.239.229; 5.J.239.230; 5.J.239.231; 5.J.239.236; 5.J.239.237;
5.J.239.238; 5.J.239.239; 5.J.239.154; 5.J.239.157; 5.J.239.166;
5.J.239.169; 5.J.239.172; 5.J.239.175; 5.J.239.240; 5.J.239.244;
5.J.154.228; 5.J.154.229; 5.J.154.230; 5.J.154.231; 5.J.154.236;
5.J.154.237; 5.J.154.238; 5.J.154.239; 5.J.154.154; 5.J.154.157;
5.J.154.166; 5.J.154.169; 5.J.154.172; 5.J.154.175; 5.J.154.240;
5.J.154.244; 5.J.157.228; 5.J.157.229; 5.J.157.230; 5.J.157.231;
5.J.157.236; 5.J.157.237; 5.J.157.238; 5.J.157.239; 5.J.157.154;
5.J.157.157; 5.J.157.166; 5.J.157.169; 5.J.157.172; 5.J.157.175;
5.J.157.240; 5.J.157.244; 5.J.166.228; 5.J.166.229; 5.J.166.230;
5.J.166.231; 5.J.166.236; 5.J.166.237; 5.J.166.238; 5.J.166.239;
5.J.166.154; 5.J.166.157; 5.J.166.166; 5.J.166.169; 5.J.166.172;
5.J.166.175; 5.J.166.240; 5.J.166.244; 5.J.169.228; 5.J.169.229;
5.J.169.230; 5.J.169.231; 5.J.169.236; 5.J.169.237; 5.J.169.238;
5.J.169.239; 5.J.169.154; 5.J.169.157; 5.J.169.166; 5.J.169.169;
5.J.169.172; 5.J.169.175; 5.J.169.240; 5.J.169.244; 5.J.172.228;
5.J.172.229; 5.J.172.230; 5.J.172.231; 5.J.172.236; 5.J.172.237;
5.J.172.238; 5.J.172.239; 5.J.172.154; 5.J.172.157; 5.J.172.166;
5.J.172.169; 5.J.172.172; 5.J.172.175; 5.J.172.240; 5.J.172.244;
5.J.175.228; 5.J.175.229; 5.J.175.230; 5.J.175.231; 5.J.175.236;
5.J.175.237; 5.J.175.238; 5.J.175.239; 5.J.175.154; 5.J.175.157;
5.J.175.166; 5.J.175.169; 5.J.175.172; 5.J.175.175; 5.J.175.240;
5.J.175.244; 5.J.240.228; 5.J.240.229; 5.J.240.230; 5.J.240.231;
5.J.240.236; 5.J.240.237; 5.J.240.238; 5.J.240.239; 5.J.240.154;
5.J.240.157; 5.J.240.166; 5.J.240.169; 5.J.240.172; 5.J.240.175;
5.J.240.240; 5.J.240.244; 5.J.244.228; 5.J.244.229; 5.J.244.230;
5.J.244.231; 5.J.244.236; 5.J.244.237; 5.J.244.238; 5.J.244.239;
5.J.244.154; 5.J.244.157; 5.J.244.166; 5.J.244.169; 5.J.244.172;
5.J.244.175; 5.J.244.240; 5.J.244.244; Prodrugs of 5.L 5.L.228.228;
5.L.228.229; 5.L.228.230; 5.L.228.231; 5.L.228.236; 5.L.228.237;
5.L.228.238; 5.L.228.239; 5.L.228.154; 5.L.228.157; 5.L.228.166;
5.L.228.169; 5.L.228.172; 5.L.228.175; 5.L.228.240; 5.L.228.244;
5.L.229.228; 5.L.229.229; 5.L.229.230; 5.L.229.231; 5.L.229.236;
5.L.229.237; 5.L.229.238; 5.L.229.239; 5.L.229.154; 5.L.229.157;
5.L.229.166; 5.L.229.169; 5.L.229.172; 5.L.229.175; 5.L.229.240;
5.L.229.244; 5.L.230.228; 5.L.230.229; 5.L.230.230; 5.L.230.231;
5.L.230.236; 5.L.230.237; 5.L.230.238; 5.L.230.239; 5.L.230.154;
5.L.230.157; 5.L.230.166; 5.L.230.169; 5.L.230.172; 5.L.230.175;
5.L.230.240; 5.L.230.244; 5.L.231.228; 5.L.231.229; 5.L.231.230;
5.L.231.231; 5.L.231.236; 5.L.231.237; 5.L.231.238; 5.L.231.239;
5.L.231.154; 5.L.231.157; 5.L.231.166; 5.L.231.169; 5.L.231.172;
5.L.231.175; 5.L.231.240; 5.L.231.244; 5.L.236.228; 5.L.236.229;
5.L.236.230; 5.L.236.231; 5.L.236.236; 5.L.236.237; 5.L.236.238;
5.L.236.239; 5.L.236.154; 5.L.236.157; 5.L.236.166; 5.L.236.169;
5.L.236.172; 5.L.236.175; 5.L.236.240; 5.L.236.244; 5.L.237.228;
5.L.237.229; 5.L.237.230; 5.L.237.231; 5.L.237.236; 5.L.237.237;
5.L.237.238; 5.L.237.239; 5.L.237.154; 5.L.237.157; 5.L.237.166;
5.L.237.169; 5.L.237.172; 5.L.237.175; 5.L.237.240; 5.L.237.244;
5.L.238.228; 5.L.238.229; 5.L.238.230; 5.L.238.231; 5.L.238.236;
5.L.238.237; 5.L.238.238; 5.L.238.239; 5.L.238.154; 5.L.238.157;
5.L.238.166; 5.L.238.169; 5.L.238.172; 5.L.238.175; 5.L.238.240;
5.L.238.244; 5.L.239.228; 5.L.239.229; 5.L.239.230; 5.L.239.231;
5.L.239.236; 5.L.239.237; 5.L.239.238; 5.L.239.239; 5.L.239.154;
5.L.239.157; 5.L.239.166; 5.L.239.169; 5.L.239.172; 5.L.239.175;
5.L.239.240; 5.L.239.244; 5.L.154.228; 5.L.154.229; 5.L.154.230;
5.L.154.231; 5.L.154.236; 5.L.154.237; 5.L.154.238; 5.L.154.239;
5.L.154.154; 5.L.154.157; 5.L.154.166; 5.L.154.169; 5.L.154.172;
5.L.154.175; 5.L.154.240; 5.L.154.244; 5.L.157.228; 5.L.157.229;
5.L.157.230; 5.L.157.231; 5.L.157.236; 5.L.157.237; 5.L.157.238;
5.L.157.239; 5.L.157.154; 5.L.157.157; 5.L.157.166; 5.L.157.169;
5.L.157.172; 5.L.157.175; 5.L.157.240; 5.L.157.244; 5.L.166.228;
5.L.166.229; 5.L.166.230; 5.L.166.231; 5.L.166.236; 5.L.166.237;
5.L.166.238; 5.L.166.239; 5.L.166.154; 5.L.166.157; 5.L.166.166;
5.L.166.169; 5.L.166.172; 5.L.166.175; 5.L.166.240; 5.L.166.244;
5.L.169.228; 5.L.169.229; 5.L.169.230; 5.L.169.231; 5.L.169.236;
5.L.169.237; 5.L.169.238; 5.L.169.239; 5.L.169.154; 5.L.169.157;
5.L.169.166; 5.L.169.169; 5.L.169.172; 5.L.169.175; 5.L.169.240;
5.L.169.244; 5.L.172.228; 5.L.172.229; 5.L.172.230; 5.L.172.231;
5.L.172.236; 5.L.172.237; 5.L.172.238; 5.L.172.239; 5.L.172.154;
5.L.172.157; 5.L.172.166; 5.L.172.169; 5.L.172.172; 5.L.172.175;
5.L.172.240; 5.L.172.244; 5.L.175.228; 5.L.175.229; 5.L.175.230;
5.L.175.231; 5.L.175.236; 5.L.175.237; 5.L.175.238; 5.L.175.239;
5.L.175.154; 5.L.175.157; 5.L.175.166; 5.L.175.169; 5.L.175.172;
5.L.175.175; 5.L.175.240; 5.L.175.244; 5.L.240.228; 5.L.240.229;
5.L.240.230; 5.L.240.231; 5.L.240.236; 5.L.240.237; 5.L.240.238;
5.L.240.239; 5.L.240.154; 5.L.240.157; 5.L.240.166; 5.L.240.169;
5.L.240.172; 5.L.240.175; 5.L.240.240; 5.L.240.244; 5.L.244.228;
5.L.244.229; 5.L.244.230; 5.L.244.231; 5.L.244.236; 5.L.244.237;
5.L.244.238; 5.L.244.239; 5.L.244.154; 5.L.244.157; 5.L.244.166;
5.L.244.169; 5.L.244.172; 5.L.244.175; 5.L.244.240; 5.L.244.244;
Prodrugs of 5.O 5.O.228.228; 5.O.228.229; 5.O.228.230; 5.O.228.231;
5.O.228.236; 5.O.228.237; 5.O.228.238; 5.O.228.239; 5.O.228.154;
5.O.228.157; 5.O.228.166; 5.O.228.169; 5.O.228.172; 5.O.228.175;
5.O.228.240; 5.O.228.244; 5.O.229.228; 5.O.229.229; 5.O.229.230;
5.O.229.231; 5.O.229.236; 5.O.229.237; 5.O.229.238; 5.O.229.239;
5.O.229.154; 5.O.229.157; 5.O.229.166; 5.O.229.169; 5.O.229.172;
5.O.229.175; 5.O.229.240; 5.O.229.244; 5.O.230.228; 5.O.230.229;
5.O.230.230; 5.O.230.231; 5.O.230.236; 5.O.230.237; 5.O.230.238;
5.O.230.239; 5.O.230.154; 5.O.230.157; 5.O.230.166; 5.O.230.169;
5.O.230.172; 5.O.230.175; 5.O.230.240; 5.O.230.244; 5.O.231.228;
5.O.231.229; 5.O.231.230; 5.O.231.231; 5.O.231.236; 5.O.231.237;
5.O.231.238; 5.O.231.239; 5.O.231.154; 5.O.231.157; 5.O.231.166;
5.O.231.169; 5.O.231.172; 5.O.231.175; 5.O.231.240; 5.O.231.244;
5.O.236.228; 5.O.236.229; 5.O.236.230; 5.O.236.231; 5.O.236.236;
5.O.236.237; 5.O.236.238; 5.O.236.239; 5.O.236.154; 5.O.236.157;
5.O.236.166; 5.O.236.169; 5.O.236.172; 5.O.236.175; 5.O.236.240;
5.O.236.244; 5.O.237.228; 5.O.237.229; 5.O.237.230; 5.O.237.231;
5.O.237.236; 5.O.237.237; 5.O.237.238; 5.O.237.239; 5.O.237.154;
5.O.237.157; 5.O.237.166; 5.O.237.169; 5.O.237.172; 5.O.237.175;
5.O.237.240; 5.O.237.244; 5.O.238.228; 5.O.238.229; 5.O.238.230;
5.O.238.231; 5.O.238.236; 5.O.238.237; 5.O.238.238; 5.O.238.239;
5.O.238.154; 5.O.238.157; 5.O.238.166; 5.O.238.169; 5.O.238.172;
5.O.238.175; 5.O.238.240; 5.O.238.244; 5.O.239.228; 5.O.239.229;
5.O.239.230; 5.O.239.231; 5.O.239.236; 5.O.239.237; 5.O.239.238;
5.O.239.239; 5.O.239.154; 5.O.239.157; 5.O.239.166; 5.O.239.169;
5.O.239.172; 5.O.239.175; 5.O.239.240; 5.O.239.244; 5.O.154.228;
5.O.154.229; 5.O.154.230; 5.O.154.231; 5.O.154.236; 5.O.154.237;
5.O.154.238; 5.O.154.239; 5.O.154.154; 5.O.154.157; 5.O.154.166;
5.O.154.169; 5.O.154.172; 5.O.154.175; 5.O.154.240; 5.O.154.244;
5.O.157.228; 5.O.157.229; 5.O.157.230; 5.O.157.231; 5.O.157.236;
5.O.157.237; 5.O.157.238; 5.O.157.239; 5.O.157.154; 5.O.157.157;
5.O.157.166; 5.O.157.169; 5.O.157.172; 5.O.157.175; 5.O.157.240;
5.O.157.244; 5.O.166.228; 5.O.166.229; 5.O.166.230; 5.O.166.231;
5.O.166.236; 5.O.166.237; 5.O.166.238; 5.O.166.239; 5.O.166.154;
5.O.166.157; 5.O.166.166; 5.O.166.169; 5.O.166.172; 5.O.166.175;
5.O.166.240; 5.O.166.244; 5.O.169.228; 5.O.169.229; 5.O.169.230;
5.O.169.231; 5.O.169.236; 5.O.169.237; 5.O.169.238; 5.O.169.239;
5.O.169.154; 5.O.169.157; 5.O.169.166; 5.O.169.169; 5.O.169.172;
5.O.169.175; 5.O.169.240; 5.O.169.244; 5.O.172.228; 5.O.172.229;
5.O.172.230; 5.O.172.231; 5.O.172.236; 5.O.172.237; 5.O.172.238;
5.O.172.239; 5.O.172.154; 5.O.172.157; 5.O.172.166; 5.O.172.169;
5.O.172.172; 5.O.172.175; 5.O.172.240; 5.O.172.244; 5.O.175.228;
5.O.175.229; 5.O.175.230; 5.O.175.231; 5.O.175.236; 5.O.175.237;
5.O.175.238; 5.O.175.239; 5.O.175.154; 5.O.175.157; 5.O.175.166;
5.O.175.169; 5.O.175.172; 5.O.175.175; 5.O.175.240; 5.O.175.244;
5.O.240.228; 5.O.240.229; 5.O.240.230; 5.O.240.231; 5.O.240.236;
5.O.240.237; 5.O.240.238; 5.O.240.239; 5.O.240.154; 5.O.240.157;
5.O.240.166; 5.O.240.169; 5.O.240.172; 5.O.240.175; 5.O.240.240;
5.O.240.244; 5.O.244.228; 5.O.244.229; 5.O.244.230; 5.O.244.231;
5.O.244.236; 5.O.244.237; 5.O.244.238; 5.O.244.239; 5.O.244.154;
5.O.244.157; 5.O.244.166; 5.O.244.169; 5.O.244.172; 5.O.244.175;
5.O.244.240; 5.O.244.244; Prodrugs of 5.P 5.P.228.228; 5.P.228.229;
5.P.228.230; 5.P.228.231; 5.P.228.236; 5.P.228.237; 5.P.228.238;
5.P.228.239; 5.P.228.154; 5.P.228.157; 5.P.228.166; 5.P.228.169;
5.P.228.172; 5.P.228.175; 5.P.228.240; 5.P.228.244; 5.P.229.228;
5.P.229.229; 5.P.229.230; 5.P.229.231; 5.P.229.236; 5.P.229.237;
5.P.229.238; 5.P.229.239; 5.P.229.154; 5.P.229.157; 5.P.229.166;
5.P.229.169; 5.P.229.172; 5.P.229.175; 5.P.229.240; 5.P.229.244;
5.P.230.228; 5.P.230.229; 5.P.230.230; 5.P.230.231; 5.P.230.236;
5.P.230.237; 5.P.230.238; 5.P.230.239; 5.P.230.154; 5.P.230.157;
5.P.230.166; 5.P.230.169; 5.P.230.172; 5.P.230.175; 5.P.230.240;
5.P.230.244; 5.P.231.228; 5.P.231.229; 5.P.231.230; 5.P.231.231;
5.P.231.236; 5.P.231.237; 5.P.231.238; 5.P.231.239; 5.P.231.154;
5.P.231.157; 5.P.231.166; 5.P.231.169; 5.P.231.172; 5.P.231.175;
5.P.231.240; 5.P.231.244; 5.P.236.228; 5.P.236.229; 5.P.236.230;
5.P.236.231; 5.P.236.236; 5.P.236.237; 5.P.236.238; 5.P.236.239;
5.P.236.154; 5.P.236.157; 5.P.236.166; 5.P.236.169; 5.P.236.172;
5.P.236.175; 5.P.236.240; 5.P.236.244; 5.P.237.228; 5.P.237.229;
5.P.237.230; 5.P.237.231; 5.P.237.236; 5.P.237.237; 5.P.237.238;
5.P.237.239; 5.P.237.154; 5.P.237.157; 5.P.237.166; 5.P.237.169;
5.P.237.172; 5.P.237.175; 5.P.237.240; 5.P.237.244; 5.P.238.228;
5.P.238.229; 5.P.238.230; 5.P.238.231; 5.P.238.236; 5.P.238.237;
5.P.238.238; 5.P.238.239; 5.P.238.154; 5.P.238.157; 5.P.238.166;
5.P.238.169; 5.P.238.172; 5.P.238.175; 5.P.238.240; 5.P.238.244;
5.P.239.228; 5.P.239.229; 5.P.239.230; 5.P.239.231; 5.P.239.236;
5.P.239.237; 5.P.239.238; 5.P.239.239; 5.P.239.154; 5.P.239.157;
5.P.239.166; 5.P.239.169; 5.P.239.172; 5.P.239.175; 5.P.239.240;
5.P.239.244; 5.P.154.228; 5.P.154.229; 5.P.154.230; 5.P.154.231;
5.P.154.236; 5.P.154.237; 5.P.154.238; 5.P.154.239; 5.P.154.154;
5.P.154.157; 5.P.154.166; 5.P.154.169; 5.P.154.172; 5.P.154.175;
5.P.154.240; 5.P.154.244; 5.P.157.228; 5.P.157.229; 5.P.157.230;
5.P.157.231; 5.P.157.236; 5.P.157.237; 5.P.157.238; 5.P.157.239;
5.P.157.154; 5.P.157.157; 5.P.157.166; 5.P.157.169; 5.P.157.172;
5.P.157.175; 5.P.157.240; 5.P.157.244; 5.P.166.228; 5.P.166.229;
5.P.166.230; 5.P.166.231; 5.P.166.236; 5.P.166.237; 5.P.166.238;
5.P.166.239; 5.P.166.154; 5.P.166.157; 5.P.166.166; 5.P.166.169;
5.P.166.172; 5.P.166.175; 5.P.166.240; 5.P.166.244; 5.P.169.228;
5.P.169.229; 5.P.169.230; 5.P.169.231; 5.P.169.236; 5.P.169.237;
5.P.169.238; 5.P.169.239; 5.P.169.154; 5.P.169.157; 5.P.169.166;
5.P.169.169; 5.P.169.172; 5.P.169.175; 5.P.169.240; 5.P.169.244;
5.P.172.228; 5.P.172.229; 5.P.172.230; 5.P.172.231; 5.P.172.236;
5.P.172.237; 5.P.172.238; 5.P.172.239;
5.P.172.154; 5.P.172.157; 5.P.172.166; 5.P.172.169; 5.P.172.172;
5.P.172.175; 5.P.172.240; 5.P.172.244; 5.P.175.228; 5.P.175.229;
5.P.175.230; 5.P.175.231; 5.P.175.236; 5.P.175.237; 5.P.175.238;
5.P.175.239; 5.P.175.154; 5.P.175.157; 5.P.175.166; 5.P.175.169;
5.P.175.172; 5.P.175.175; 5.P.175.240; 5.P.175.244; 5.P.240.228;
5.P.240.229; 5.P.240.230; 5.P.240.231; 5.P.240.236; 5.P.240.237;
5.P.240.238; 5.P.240.239; 5.P.240.154; 5.P.240.157; 5.P.240.166;
5.P.240.169; 5.P.240.172; 5.P.240.175; 5.P.240.240; 5.P.240.244;
5.P.244.228; 5.P.244.229; 5.P.244.230; 5.P.244.231; 5.P.244.236;
5.P.244.237; 5.P.244.238; 5.P.244.239; 5.P.244.154; 5.P.244.157;
5.P.244.166; 5.P.244.169; 5.P.244.172; 5.P.244.175; 5.P.244.240;
5.P.244.244; Prodrugs of 5.U 5.U.228.228; 5.U.228.229; 5.U.228.230;
5.U.228.231; 5.U.228.236; 5.U.228.237; 5.U.228.238; 5.U.228.239;
5.U.228.154; 5.U.228.157; 5.U.228.166; 5.U.228.169; 5.U.228.172;
5.U.228.175; 5.U.228.240; 5.U.228.244; 5.U.229.228; 5.U.229.229;
5.U.229.230; 5.U.229.231; 5.U.229.236; 5.U.229.237; 5.U.229.238;
5.U.229.239; 5.U.229.154; 5.U.229.157; 5.U.229.166; 5.U.229.169;
5.U.229.172; 5.U.229.175; 5.U.229.240; 5.U.229.244; 5.U.230.228;
5.U.230.229; 5.U.230.230; 5.U.230.231; 5.U.230.236; 5.U.230.237;
5.U.230.238; 5.U.230.239; 5.U.230.154; 5.U.230.157; 5.U.230.166;
5.U.230.169; 5.U.230.172; 5.U.230.175; 5.U.230.240; 5.U.230.244;
5.U.231.228; 5.U.231.229; 5.U.231.230; 5.U.231.231; 5.U.231.236;
5.U.231.237; 5.U.231.238; 5.U.231.239; 5.U.231.154; 5.U.231.157;
5.U.231.166; 5.U.231.169; 5.U.231.172; 5.U.231.175; 5.U.231.240;
5.U.231.244; 5.U.236.228; 5.U.236.229; 5.U.236.230; 5.U.236.231;
5.U.236.236; 5.U.236.237; 5.U.236.238; 5.U.236.239; 5.U.236.154;
5.U.236.157; 5.U.236.166; 5.U.236.169; 5.U.236.172; 5.U.236.175;
5.U.236.240; 5.U.236.244; 5.U.237.228; 5.U.237.229; 5.U.237.230;
5.U.237.231; 5.U.237.236; 5.U.237.237; 5.U.237.238; 5.U.237.239;
5.U.237.154; 5.U.237.157; 5.U.237.166; 5.U.237.169; 5.U.237.172;
5.U.237.175; 5.U.237.240; 5.U.237.244; 5.U.238.228; 5.U.238.229;
5.U.238.230; 5.U.238.231; 5.U.238.236; 5.U.238.237; 5.U.238.238;
5.U.238.239; 5.U.238.154; 5.U.238.157; 5.U.238.166; 5.U.238.169;
5.U.238.172; 5.U.238.175; 5.U.238.240; 5.U.238.244; 5.U.239.228;
5.U.239.229; 5.U.239.230; 5.U.239.231; 5.U.239.236; 5.U.239.237;
5.U.239.238; 5.U.239.239; 5.U.239.154; 5.U.239.157; 5.U.239.166;
5.U.239.169; 5.U.239.172; 5.U.239.175; 5.U.239.240; 5.U.239.244;
5.U.154.228; 5.U.154.229; 5.U.154.230; 5.U.154.231; 5.U.154.236;
5.U.154.237; 5.U.154.238; 5.U.154.239; 5.U.154.154; 5.U.154.157;
5.U.154.166; 5.U.154.169; 5.U.154.172; 5.U.154.175; 5.U.154.240;
5.U.154.244; 5.U.157.228; 5.U.157.229; 5.U.157.230; 5.U.157.231;
5.U.157.236; 5.U.157.237; 5.U.157.238; 5.U.157.239; 5.U.157.154;
5.U.157.157; 5.U.157.166; 5.U.157.169; 5.U.157.172; 5.U.157.175;
5.U.157.240; 5.U.157.244; 5.U.166.228; 5.U.166.229; 5.U.166.230;
5.U.166.231; 5.U.166.236; 5.U.166.237; 5.U.166.238; 5.U.166.239;
5.U.166.154; 5.U.166.157; 5.U.166.166; 5.U.166.169; 5.U.166.172;
5.U.166.175; 5.U.166.240; 5.U.166.244; 5.U.169.228; 5.U.169.229;
5.U.169.230; 5.U.169.231; 5.U.169.236; 5.U.169.237; 5.U.169.238;
5.U.169.239; 5.U.169.154; 5.U.169.157; 5.U.169.166; 5.U.169.169;
5.U.169.172; 5.U.169.175; 5.U.169.240; 5.U.169.244; 5.U.172.228;
5.U.172.229; 5.U.172.230; 5.U.172.231; 5.U.172.236; 5.U.172.237;
5.U.172.238; 5.U.172.239; 5.U.172.154; 5.U.172.157; 5.U.172.166;
5.U.172.169; 5.U.172.172; 5.U.172.175; 5.U.172.240; 5.U.172.244;
5.U.175.228; 5.U.175.229; 5.U.175.230; 5.U.175.231; 5.U.175.236;
5.U.175.237; 5.U.175.238; 5.U.175.239; 5.U.175.154; 5.U.175.157;
5.U.175.166; 5.U.175.169; 5.U.175.172; 5.U.175.175; 5.U.175.240;
5.U.175.244; 5.U.240.228; 5.U.240.229; 5.U.240.230; 5.U.240.231;
5.U.240.236; 5.U.240.237; 5.U.240.238; 5.U.240.239; 5.U.240.154;
5.U.240.157; 5.U.240.166; 5.U.240.169; 5.U.240.172; 5.U.240.175;
5.U.240.240; 5.U.240.244; 5.U.244.228; 5.U.244.229; 5.U.244.230;
5.U.244.231; 5.U.244.236; 5.U.244.237; 5.U.244.238; 5.U.244.239;
5.U.244.154; 5.U.244.157; 5.U.244.166; 5.U.244.169; 5.U.244.172;
5.U.244.175; 5.U.244.240; 5.U.244.244; Prodrugs of 5.W 5.W.228.228;
5.W.228.229; 5.W.228.230; 5.W.228.231; 5.W.228.236; 5.W.228.237;
5.W.228.238; 5.W.228.239; 5.W.228.154; 5.W.228.157; 5.W.228.166;
5.W.228.169; 5.W.228.172; 5.W.228.175; 5.W.228.240; 5.W.228.244;
5.W.229.228; 5.W.229.229; 5.W.229.230; 5.W.229.231; 5.W.229.236;
5.W.229.237; 5.W.229.238; 5.W.229.239; 5.W.229.154; 5.W.229.157;
5.W.229.166; 5.W.229.169; 5.W.229.172; 5.W.229.175; 5.W.229.240;
5.W.229.244; 5.W.230.228; 5.W.230.229; 5.W.230.230; 5.W.230.231;
5.W.230.236; 5.W.230.237; 5.W.230.238; 5.W.230.239; 5.W.230.154;
5.W.230.157; 5.W.230.166; 5.W.230.169; 5.W.230.172; 5.W.230.175;
5.W.230.240; 5.W.230.244; 5.W.231.228; 5.W.231.229; 5.W.231.230;
5.W.231.231; 5.W.231.236; 5.W.231.237; 5.W.231.238; 5.W.231.239;
5.W.231.154; 5.W.231.157; 5.W.231.166; 5.W.231.169; 5.W.231.172;
5.W.231.175; 5.W.231.240; 5.W.231.244; 5.W.236.228; 5.W.236.229;
5.W.236.230; 5.W.236.231; 5.W.236.236; 5.W.236.237; 5.W.236.238;
5.W.236.239; 5.W.236.154; 5.W.236.157; 5.W.236.166; 5.W.236.169;
5.W.236.172; 5.W.236.175; 5.W.236.240; 5.W.236.244; 5.W.237.228;
5.W.237.229; 5.W.237.230; 5.W.237.231; 5.W.237.236; 5.W.237.237;
5.W.237.238; 5.W.237.239; 5.W.237.154; 5.W.237.157; 5.W.237.166;
5.W.237.169; 5.W.237.172; 5.W.237.175; 5.W.237.240; 5.W.237.244;
5.W.238.228; 5.W.238.229; 5.W.238.230; 5.W.238.231; 5.W.238.236;
5.W.238.237; 5.W.238.238; 5.W.238.239; 5.W.238.154; 5.W.238.157;
5.W.238.166; 5.W.238.169; 5.W.238.172; 5.W.238.175; 5.W.238.240;
5.W.238.244; 5.W.239.228; 5.W.239.229; 5.W.239.230; 5.W.239.231;
5.W.239.236; 5.W.239.237; 5.W.239.238; 5.W.239.239; 5.W.239.154;
5.W.239.157; 5.W.239.166; 5.W.239.169; 5.W.239.172; 5.W.239.175;
5.W.239.240; 5.W.239.244; 5.W.154.228; 5.W.154.229; 5.W.154.230;
5.W.154.231; 5.W.154.236; 5.W.154.237; 5.W.154.238; 5.W.154.239;
5.W.154.154; 5.W.154.157; 5.W.154.166; 5.W.154.169; 5.W.154.172;
5.W.154.175; 5.W.154.240; 5.W.154.244; 5.W.157.228; 5.W.157.229;
5.W.157.230; 5.W.157.231; 5.W.157.236; 5.W.157.237; 5.W.157.238;
5.W.157.239; 5.W.157.154; 5.W.157.157; 5.W.157.166; 5.W.157.169;
5.W.157.172; 5.W.157.175; 5.W.157.240; 5.W.157.244; 5.W.166.228;
5.W.166.229; 5.W.166.230; 5.W.166.231; 5.W.166.236; 5.W.166.237;
5.W.166.238; 5.W.166.239; 5.W.166.154; 5.W.166.157; 5.W.166.166;
5.W.166.169; 5.W.166.172; 5.W.166.175; 5.W.166.240; 5.W.166.244;
5.W.169.228; 5.W.169.229; 5.W.169.230; 5.W.169.231; 5.W.169.236;
5.W.169.237; 5.W.169.238; 5.W.169.239; 5.W.169.154; 5.W.169.157;
5.W.169.166; 5.W.169.169; 5.W.169.172; 5.W.169.175; 5.W.169.240;
5.W.169.244; 5.W.172.228; 5.W.172.229; 5.W.172.230; 5.W.172.231;
5.W.172.236; 5.W.172.237; 5.W.172.238; 5.W.172.239; 5.W.172.154;
5.W.172.157; 5.W.172.166; 5.W.172.169; 5.W.172.172; 5.W.172.175;
5.W.172.240; 5.W.172.244; 5.W.175.228; 5.W.175.229; 5.W.175.230;
5.W.175.231; 5.W.175.236; 5.W.175.237; 5.W.175.238; 5.W.175.239;
5.W.175.154; 5.W.175.157; 5.W.175.166; 5.W.175.169; 5.W.175.172;
5.W.175.175; 5.W.175.240; 5.W.175.244; 5.W.240.228; 5.W.240.229;
5.W.240.230; 5.W.240.231; 5.W.240.236; 5.W.240.237; 5.W.240.238;
5.W.240.239; 5.W.240.154; 5.W.240.157; 5.W.240.166; 5.W.240.169;
5.W.240.172; 5.W.240.175; 5.W.240.240; 5.W.240.244; 5.W.244.228;
5.W.244.229; 5.W.244.230; 5.W.244.231; 5.W.244.236; 5.W.244.237;
5.W.244.238; 5.W.244.239; 5.W.244.154; 5.W.244.157; 5.W.244.166;
5.W.244.169; 5.W.244.172; 5.W.244.175; 5.W.244.240; 5.W.244.244;
Prodrugs of 5.Y 5.Y.228.228; 5.Y.228.229; 5.Y.228.230; 5.Y.228.231;
5.Y.228.236; 5.Y.228.237; 5.Y.228.238; 5.Y.228.239; 5.Y.228.154;
5.Y.228.157; 5.Y.228.166; 5.Y.228.169; 5.Y.228.172; 5.Y.228.175;
5.Y.228.240; 5.Y.228.244; 5.Y.229.228; 5.Y.229.229; 5.Y.229.230;
5.Y.229.231; 5.Y.229.236; 5.Y.229.237; 5.Y.229.238; 5.Y.229.239;
5.Y.229.154; 5.Y.229.157; 5.Y.229.166; 5.Y.229.169; 5.Y.229.172;
5.Y.229.175; 5.Y.229.240; 5.Y.229.244; 5.Y.230.228; 5.Y.230.229;
5.Y.230.230; 5.Y.230.231; 5.Y.230.236; 5.Y.230.237; 5.Y.230.238;
5.Y.230.239; 5.Y.230.154; 5.Y.230.157; 5.Y.230.166; 5.Y.230.169;
5.Y.230.172; 5.Y.230.175; 5.Y.230.240; 5.Y.230.244; 5.Y.231.228;
5.Y.231.229; 5.Y.231.230; 5.Y.231.231; 5.Y.231.236; 5.Y.231.237;
5.Y.231.238; 5.Y.231.239; 5.Y.231.154; 5.Y.231.157; 5.Y.231.166;
5.Y.231.169; 5.Y.231.172; 5.Y.231.175; 5.Y.231.240; 5.Y.231.244;
5.Y.236.228; 5.Y.236.229; 5.Y.236.230; 5.Y.236.231; 5.Y.236.236;
5.Y.236.237; 5.Y.236.238; 5.Y.236.239; 5.Y.236.154; 5.Y.236.157;
5.Y.236.166; 5.Y.236.169; 5.Y.236.172; 5.Y.236.175; 5.Y.236.240;
5.Y.236.244; 5.Y.237.228; 5.Y.237.229; 5.Y.237.230; 5.Y.237.231;
5.Y.237.236; 5.Y.237.237; 5.Y.237.238; 5.Y.237.239; 5.Y.237.154;
5.Y.237.157; 5.Y.237.166; 5.Y.237.169; 5.Y.237.172; 5.Y.237.175;
5.Y.237.240; 5.Y.237.244; 5.Y.238.228; 5.Y.238.229; 5.Y.238.230;
5.Y.238.231; 5.Y.238.236; 5.Y.238.237; 5.Y.238.238; 5.Y.238.239;
5.Y.238.154; 5.Y.238.157; 5.Y.238.166; 5.Y.238.169; 5.Y.238.172;
5.Y.238.175; 5.Y.238.240; 5.Y.238.244; 5.Y.239.228; 5.Y.239.229;
5.Y.239.230; 5.Y.239.231; 5.Y.239.236; 5.Y.239.237; 5.Y.239.238;
5.Y.239.239; 5.Y.239.154; 5.Y.239.157; 5.Y.239.166; 5.Y.239.169;
5.Y.239.172; 5.Y.239.175; 5.Y.239.240; 5.Y.239.244; 5.Y.154.228;
5.Y.154.229; 5.Y.154.230; 5.Y.154.231; 5.Y.154.236; 5.Y.154.237;
5.Y.154.238; 5.Y.154.239; 5.Y.154.154; 5.Y.154.157; 5.Y.154.166;
5.Y.154.169; 5.Y.154.172; 5.Y.154.175; 5.Y.154.240; 5.Y.154.244;
5.Y.157.228; 5.Y.157.229; 5.Y.157.230; 5.Y.157.231; 5.Y.157.236;
5.Y.157.237; 5.Y.157.238; 5.Y.157.239; 5.Y.157.154; 5.Y.157.157;
5.Y.157.166; 5.Y.157.169; 5.Y.157.172; 5.Y.157.175; 5.Y.157.240;
5.Y.157.244; 5.Y.166.228; 5.Y.166.229; 5.Y.166.230; 5.Y.166.231;
5.Y.166.236; 5.Y.166.237; 5.Y.166.238; 5.Y.166.239; 5.Y.166.154;
5.Y.166.157; 5.Y.166.166; 5.Y.166.169; 5.Y.166.172; 5.Y.166.175;
5.Y.166.240; 5.Y.166.244; 5.Y.169.228; 5.Y.169.229; 5.Y.169.230;
5.Y.169.231; 5.Y.169.236; 5.Y.169.237; 5.Y.169.238; 5.Y.169.239;
5.Y.169.154; 5.Y.169.157; 5.Y.169.166; 5.Y.169.169; 5.Y.169.172;
5.Y.169.175; 5.Y.169.240; 5.Y.169.244; 5.Y.172.228; 5.Y.172.229;
5.Y.172.230; 5.Y.172.231; 5.Y.172.236; 5.Y.172.237; 5.Y.172.238;
5.Y.172.239; 5.Y.172.154; 5.Y.172.157; 5.Y.172.166; 5.Y.172.169;
5.Y.172.172; 5.Y.172.175; 5.Y.172.240; 5.Y.172.244; 5.Y.175.228;
5.Y.175.229; 5.Y.175.230; 5.Y.175.231; 5.Y.175.236; 5.Y.175.237;
5.Y.175.238; 5.Y.175.239; 5.Y.175.154; 5.Y.175.157; 5.Y.175.166;
5.Y.175.169; 5.Y.175.172; 5.Y.175.175; 5.Y.175.240; 5.Y.175.244;
5.Y.240.228; 5.Y.240.229; 5.Y.240.230; 5.Y.240.231; 5.Y.240.236;
5.Y.240.237; 5.Y.240.238; 5.Y.240.239; 5.Y.240.154; 5.Y.240.157;
5.Y.240.166; 5.Y.240.169; 5.Y.240.172; 5.Y.240.175; 5.Y.240.240;
5.Y.240.244; 5.Y.244.228; 5.Y.244.229; 5.Y.244.230; 5.Y.244.231;
5.Y.244.236; 5.Y.244.237; 5.Y.244.238; 5.Y.244.239; 5.Y.244.154;
5.Y.244.157; 5.Y.244.166; 5.Y.244.169; 5.Y.244.172; 5.Y.244.175;
5.Y.244.240; 5.Y.244.244; Prodrugs of 6.B 6.B.228.228; 6.B.228.229;
6.B.228.230; 6.B.228.231; 6.B.228.236; 6.B.228.237; 6.B.228.238;
6.B.228.239; 6.B.228.154; 6.B.228.157; 6.B.228.166; 6.B.228.169;
6.B.228.172; 6.B.228.175; 6.B.228.240; 6.B.228.244; 6.B.229.228;
6.B.229.229; 6.B.229.230; 6.B.229.231; 6.B.229.236; 6.B.229.237;
6.B.229.238; 6.B.229.239; 6.B.229.154; 6.B.229.157; 6.B.229.166;
6.B.229.169; 6.B.229.172; 6.B.229.175; 6.B.229.240; 6.B.229.244;
6.B.230.228; 6.B.230.229; 6.B.230.230; 6.B.230.231; 6.B.230.236;
6.B.230.237; 6.B.230.238; 6.B.230.239; 6.B.230.154; 6.B.230.157;
6.B.230.166; 6.B.230.169; 6.B.230.172; 6.B.230.175; 6.B.230.240;
6.B.230.244; 6.B.231.228; 6.B.231.229; 6.B.231.230; 6.B.231.231;
6.B.231.236; 6.B.231.237; 6.B.231.238; 6.B.231.239; 6.B.231.154;
6.B.231.157; 6.B.231.166; 6.B.231.169; 6.B.231.172; 6.B.231.175;
6.B.231.240; 6.B.231.244; 6.B.236.228; 6.B.236.229; 6.B.236.230;
6.B.236.231; 6.B.236.236; 6.B.236.237; 6.B.236.238; 6.B.236.239;
6.B.236.154; 6.B.236.157; 6.B.236.166; 6.B.236.169; 6.B.236.172;
6.B.236.175; 6.B.236.240; 6.B.236.244; 6.B.237.228; 6.B.237.229;
6.B.237.230; 6.B.237.231; 6.B.237.236; 6.B.237.237; 6.B.237.238;
6.B.237.239; 6.B.237.154; 6.B.237.157; 6.B.237.166; 6.B.237.169;
6.B.237.172; 6.B.237.175; 6.B.237.240; 6.B.237.244; 6.B.238.228;
6.B.238.229; 6.B.238.230; 6.B.238.231; 6.B.238.236; 6.B.238.237;
6.B.238.238; 6.B.238.239; 6.B.238.154; 6.B.238.157; 6.B.238.166;
6.B.238.169; 6.B.238.172; 6.B.238.175; 6.B.238.240; 6.B.238.244;
6.B.239.228; 6.B.239.229; 6.B.239.230; 6.B.239.231; 6.B.239.236;
6.B.239.237; 6.B.239.238; 6.B.239.239; 6.B.239.154; 6.B.239.157;
6.B.239.166; 6.B.239.169; 6.B.239.172; 6.B.239.175; 6.B.239.240;
6.B.239.244; 6.B.154.228; 6.B.154.229; 6.B.154.230; 6.B.154.231;
6.B.154.236; 6.B.154.237; 6.B.154.238; 6.B.154.239; 6.B.154.154;
6.B.154.157; 6.B.154.166; 6.B.154.169; 6.B.154.172; 6.B.154.175;
6.B.154.240; 6.B.154.244; 6.B.157.228; 6.B.157.229; 6.B.157.230;
6.B.157.231; 6.B.157.236; 6.B.157.237; 6.B.157.238; 6.B.157.239;
6.B.157.154; 6.B.157.157; 6.B.157.166; 6.B.157.169; 6.B.157.172;
6.B.157.175; 6.B.157.240; 6.B.157.244; 6.B.166.228; 6.B.166.229;
6.B.166.230; 6.B.166.231; 6.B.166.236; 6.B.166.237; 6.B.166.238;
6.B.166.239; 6.B.166.154; 6.B.166.157; 6.B.166.166; 6.B.166.169;
6.B.166.172; 6.B.166.175; 6.B.166.240; 6.B.166.244; 6.B.169.228;
6.B.169.229; 6.B.169.230; 6.B.169.231; 6.B.169.236; 6.B.169.237;
6.B.169.238; 6.B.169.239; 6.B.169.154; 6.B.169.157; 6.B.169.166;
6.B.169.169; 6.B.169.172; 6.B.169.175; 6.B.169.240; 6.B.169.244;
6.B.172.228; 6.B.172.229; 6.B.172.230; 6.B.172.231; 6.B.172.236;
6.B.172.237; 6.B.172.238; 6.B.172.239; 6.B.172.154; 6.B.172.157;
6.B.172.166; 6.B.172.169; 6.B.172.172; 6.B.172.175; 6.B.172.240;
6.B.172.244; 6.B.175.228; 6.B.175.229; 6.B.175.230; 6.B.175.231;
6.B.175.236; 6.B.175.237; 6.B.175.238; 6.B.175.239; 6.B.175.154;
6.B.175.157; 6.B.175.166; 6.B.175.169; 6.B.175.172; 6.B.175.175;
6.B.175.240; 6.B.175.244; 6.B.240.228; 6.B.240.229; 6.B.240.230;
6.B.240.231; 6.B.240.236; 6.B.240.237; 6.B.240.238; 6.B.240.239;
6.B.240.154; 6.B.240.157; 6.B.240.166; 6.B.240.169; 6.B.240.172;
6.B.240.175; 6.B.240.240; 6.B.240.244; 6.B.244.228; 6.B.244.229;
6.B.244.230; 6.B.244.231; 6.B.244.236; 6.B.244.237; 6.B.244.238;
6.B.244.239; 6.B.244.154; 6.B.244.157; 6.B.244.166; 6.B.244.169;
6.B.244.172; 6.B.244.175; 6.B.244.240; 6.B.244.244; Prodrugs of 6.D
6.D.228.228; 6.D.228.229; 6.D.228.230; 6.D.228.231; 6.D.228.236;
6.D.228.237; 6.D.228.238; 6.D.228.239; 6.D.228.154; 6.D.228.157;
6.D.228.166; 6.D.228.169; 6.D.228.172; 6.D.228.175; 6.D.228.240;
6.D.228.244; 6.D.229.228; 6.D.229.229; 6.D.229.230; 6.D.229.231;
6.D.229.236; 6.D.229.237; 6.D.229.238; 6.D.229.239; 6.D.229.154;
6.D.229.157; 6.D.229.166; 6.D.229.169; 6.D.229.172; 6.D.229.175;
6.D.229.240; 6.D.229.244; 6.D.230.228; 6.D.230.229; 6.D.230.230;
6.D.230.231; 6.D.230.236; 6.D.230.237; 6.D.230.238; 6.D.230.239;
6.D.230.154; 6.D.230.157; 6.D.230.166; 6.D.230.169; 6.D.230.172;
6.D.230.175; 6.D.230.240; 6.D.230.244; 6.D.231.228; 6.D.231.229;
6.D.231.230; 6.D.231.231; 6.D.231.236; 6.D.231.237; 6.D.231.238;
6.D.231.239; 6.D.231.154; 6.D.231.157; 6.D.231.166; 6.D.231.169;
6.D.231.172; 6.D.231.175; 6.D.231.240; 6.D.231.244; 6.D.236.228;
6.D.236.229; 6.D.236.230; 6.D.236.231; 6.D.236.236; 6.D.236.237;
6.D.236.238; 6.D.236.239; 6.D.236.154; 6.D.236.157; 6.D.236.166;
6.D.236.169; 6.D.236.172; 6.D.236.175; 6.D.236.240; 6.D.236.244;
6.D.237.228; 6.D.237.229; 6.D.237.230; 6.D.237.231; 6.D.237.236;
6.D.237.237; 6.D.237.238; 6.D.237.239; 6.D.237.154; 6.D.237.157;
6.D.237.166; 6.D.237.169; 6.D.237.172; 6.D.237.175; 6.D.237.240;
6.D.237.244; 6.D.238.228; 6.D.238.229; 6.D.238.230; 6.D.238.231;
6.D.238.236; 6.D.238.237; 6.D.238.238; 6.D.238.239; 6.D.238.154;
6.D.238.157; 6.D.238.166; 6.D.238.169; 6.D.238.172; 6.D.238.175;
6.D.238.240; 6.D.238.244; 6.D.239.228; 6.D.239.229; 6.D.239.230;
6.D.239.231; 6.D.239.236; 6.D.239.237; 6.D.239.238; 6.D.239.239;
6.D.239.154; 6.D.239.157; 6.D.239.166; 6.D.239.169; 6.D.239.172;
6.D.239.175; 6.D.239.240; 6.D.239.244; 6.D.154.228;
6.D.154.229;
6.D.154.230; 6.D.154.231; 6.D.154.236; 6.D.154.237; 6.D.154.238;
6.D.154.239; 6.D.154.154; 6.D.154.157; 6.D.154.166; 6.D.154.169;
6.D.154.172; 6.D.154.175; 6.D.154.240; 6.D.154.244; 6.D.157.228;
6.D.157.229; 6.D.157.230; 6.D.157.231; 6.D.157.236; 6.D.157.237;
6.D.157.238; 6.D.157.239; 6.D.157.154; 6.D.157.157; 6.D.157.166;
6.D.157.169; 6.D.157.172; 6.D.157.175; 6.D.157.240; 6.D.157.244;
6.D.166.228; 6.D.166.229; 6.D.166.230; 6.D.166.231; 6.D.166.236;
6.D.166.237; 6.D.166.238; 6.D.166.239; 6.D.166.154; 6.D.166.157;
6.D.166.166; 6.D.166.169; 6.D.166.172; 6.D.166.175; 6.D.166.240;
6.D.166.244; 6.D.169.228; 6.D.169.229; 6.D.169.230; 6.D.169.231;
6.D.169.236; 6.D.169.237; 6.D.169.238; 6.D.169.239; 6.D.169.154;
6.D.169.157; 6.D.169.166; 6.D.169.169; 6.D.169.172; 6.D.169.175;
6.D.169.240; 6.D.169.244; 6.D.172.228; 6.D.172.229; 6.D.172.230;
6.D.172.231; 6.D.172.236; 6.D.172.237; 6.D.172.238; 6.D.172.239;
6.D.172.154; 6.D.172.157; 6.D.172.166; 6.D.172.169; 6.D.172.172;
6.D.172.175; 6.D.172.240; 6.D.172.244; 6.D.175.228; 6.D.175.229;
6.D.175.230; 6.D.175.231; 6.D.175.236; 6.D.175.237; 6.D.175.238;
6.D.175.239; 6.D.175.154; 6.D.175.157; 6.D.175.166; 6.D.175.169;
6.D.175.172; 6.D.175.175; 6.D.175.240; 6.D.175.244; 6.D.240.228;
6.D.240.229; 6.D.240.230; 6.D.240.231; 6.D.240.236; 6.D.240.237;
6.D.240.238; 6.D.240.239; 6.D.240.154; 6.D.240.157; 6.D.240.166;
6.D.240.169; 6.D.240.172; 6.D.240.175; 6.D.240.240; 6.D.240.244;
6.D.244.228; 6.D.244.229; 6.D.244.230; 6.D.244.231; 6.D.244.236;
6.D.244.237; 6.D.244.238; 6.D.244.239; 6.D.244.154; 6.D.244.157;
6.D.244.166; 6.D.244.169; 6.D.244.172; 6.D.244.175; 6.D.244.240;
6.D.244.244; Prodrugs of 6.E 6.E.228.228; 6.E.228.229; 6.E.228.230;
6.E.228.231; 6.E.228.236; 6.E.228.237; 6.E.228.238; 6.E.228.239;
6.E.228.154; 6.E.228.157; 6.E.228.166; 6.E.228.169; 6.E.228.172;
6.E.228.175; 6.E.228.240; 6.E.228.244; 6.E.229.228; 6.E.229.229;
6.E.229.230; 6.E.229.231; 6.E.229.236; 6.E.229.237; 6.E.229.238;
6.E.229.239; 6.E.229.154; 6.E.229.157; 6.E.229.166; 6.E.229.169;
6.E.229.172; 6.E.229.175; 6.E.229.240; 6.E.229.244; 6.E.230.228;
6.E.230.229; 6.E.230.230; 6.E.230.231; 6.E.230.236; 6.E.230.237;
6.E.230.238; 6.E.230.239; 6.E.230.154; 6.E.230.157; 6.E.230.166;
6.E.230.169; 6.E.230.172; 6.E.230.175; 6.E.230.240; 6.E.230.244;
6.E.231.228; 6.E.231.229; 6.E.231.230; 6.E.231.231; 6.E.231.236;
6.E.231.237; 6.E.231.238; 6.E.231.239; 6.E.231.154; 6.E.231.157;
6.E.231.166; 6.E.231.169; 6.E.231.172; 6.E.231.175; 6.E.231.240;
6.E.231.244; 6.E.236.228; 6.E.236.229; 6.E.236.230; 6.E.236.231;
6.E.236.236; 6.E.236.237; 6.E.236.238; 6.E.236.239; 6.E.236.154;
6.E.236.157; 6.E.236.166; 6.E.236.169; 6.E.236.172; 6.E.236.175;
6.E.236.240; 6.E.236.244; 6.E.237.228; 6.E.237.229; 6.E.237.230;
6.E.237.231; 6.E.237.236; 6.E.237.237; 6.E.237.238; 6.E.237.239;
6.E.237.154; 6.E.237.157; 6.E.237.166; 6.E.237.169; 6.E.237.172;
6.E.237.175; 6.E.237.240; 6.E.237.244; 6.E.238.228; 6.E.238.229;
6.E.238.230; 6.E.238.231; 6.E.238.236; 6.E.238.237; 6.E.238.238;
6.E.238.239; 6.E.238.154; 6.E.238.157; 6.E.238.166; 6.E.238.169;
6.E.238.172; 6.E.238.175; 6.E.238.240; 6.E.238.244; 6.E.239.228;
6.E.239.229; 6.E.239.230; 6.E.239.231; 6.E.239.236; 6.E.239.237;
6.E.239.238; 6.E.239.239; 6.E.239.154; 6.E.239.157; 6.E.239.166;
6.E.239.169; 6.E.239.172; 6.E.239.175; 6.E.239.240; 6.E.239.244;
6.E.154.228; 6.E.154.229; 6.E.154.230; 6.E.154.231; 6.E.154.236;
6.E.154.237; 6.E.154.238; 6.E.154.239; 6.E.154.154; 6.E.154.157;
6.E.154.166; 6.E.154.169; 6.E.154.172; 6.E.154.175; 6.E.154.240;
6.E.154.244; 6.E.157.228; 6.E.157.229; 6.E.157.230; 6.E.157.231;
6.E.157.236; 6.E.157.237; 6.E.157.238; 6.E.157.239; 6.E.157.154;
6.E.157.157; 6.E.157.166; 6.E.157.169; 6.E.157.172; 6.E.157.175;
6.E.157.240; 6.E.157.244; 6.E.166.228; 6.E.166.229; 6.E.166.230;
6.E.166.231; 6.E.166.236; 6.E.166.237; 6.E.166.238; 6.E.166.239;
6.E.166.154; 6.E.166.157; 6.E.166.166; 6.E.166.169; 6.E.166.172;
6.E.166.175; 6.E.166.240; 6.E.166.244; 6.E.169.228; 6.E.169.229;
6.E.169.230; 6.E.169.231; 6.E.169.236; 6.E.169.237; 6.E.169.238;
6.E.169.239; 6.E.169.154; 6.E.169.157; 6.E.169.166; 6.E.169.169;
6.E.169.172; 6.E.169.175; 6.E.169.240; 6.E.169.244; 6.E.172.228;
6.E.172.229; 6.E.172.230; 6.E.172.231; 6.E.172.236; 6.E.172.237;
6.E.172.238; 6.E.172.239; 6.E.172.154; 6.E.172.157; 6.E.172.166;
6.E.172.169; 6.E.172.172; 6.E.172.175; 6.E.172.240; 6.E.172.244;
6.E.175.228; 6.E.175.229; 6.E.175.230; 6.E.175.231; 6.E.175.236;
6.E.175.237; 6.E.175.238; 6.E.175.239; 6.E.175.154; 6.E.175.157;
6.E.175.166; 6.E.175.169; 6.E.175.172; 6.E.175.175; 6.E.175.240;
6.E.175.244; 6.E.240.228; 6.E.240.229; 6.E.240.230; 6.E.240.231;
6.E.240.236; 6.E.240.237; 6.E.240.238; 6.E.240.239; 6.E.240.154;
6.E.240.157; 6.E.240.166; 6.E.240.169; 6.E.240.172; 6.E.240.175;
6.E.240.240; 6.E.240.244; 6.E.244.228; 6.E.244.229; 6.E.244.230;
6.E.244.231; 6.E.244.236; 6.E.244.237; 6.E.244.238; 6.E.244.239;
6.E.244.154; 6.E.244.157; 6.E.244.166; 6.E.244.169; 6.E.244.172;
6.E.244.175; 6.E.244.240; 6.E.244.244; Prodrugs of 6.G 6.G.228.228;
6.G.228.229; 6.G.228.230; 6.G.228.231; 6.G.228.236; 6.G.228.237;
6.G.228.238; 6.G.228.239; 6.G.228.154; 6.G.228.157; 6.G.228.166;
6.G.228.169; 6.G.228.172; 6.G.228.175; 6.G.228.240; 6.G.228.244;
6.G.229.228; 6.G.229.229; 6.G.229.230; 6.G.229.231; 6.G.229.236;
6.G.229.237; 6.G.229.238; 6.G.229.239; 6.G.229.154; 6.G.229.157;
6.G.229.166; 6.G.229.169; 6.G.229.172; 6.G.229.175; 6.G.229.240;
6.G.229.244; 6.G.230.228; 6.G.230.229; 6.G.230.230; 6.G.230.231;
6.G.230.236; 6.G.230.237; 6.G.230.238; 6.G.230.239; 6.G.230.154;
6.G.230.157; 6.G.230.166; 6.G.230.169; 6.G.230.172; 6.G.230.175;
6.G.230.240; 6.G.230.244; 6.G.231.228; 6.G.231.229; 6.G.231.230;
6.G.231.231; 6.G.231.236; 6.G.231.237; 6.G.231.238; 6.G.231.239;
6.G.231.154; 6.G.231.157; 6.G.231.166; 6.G.231.169; 6.G.231.172;
6.G.231.175; 6.G.231.240; 6.G.231.244; 6.G.236.228; 6.G.236.229;
6.G.236.230; 6.G.236.231; 6.G.236.236; 6.G.236.237; 6.G.236.238;
6.G.236.239; 6.G.236.154; 6.G.236.157; 6.G.236.166; 6.G.236.169;
6.G.236.172; 6.G.236.175; 6.G.236.240; 6.G.236.244; 6.G.237.228;
6.G.237.229; 6.G.237.230; 6.G.237.231; 6.G.237.236; 6.G.237.237;
6.G.237.238; 6.G.237.239; 6.G.237.154; 6.G.237.157; 6.G.237.166;
6.G.237.169; 6.G.237.172; 6.G.237.175; 6.G.237.240; 6.G.237.244;
6.G.238.228; 6.G.238.229; 6.G.238.230; 6.G.238.231; 6.G.238.236;
6.G.238.237; 6.G.238.238; 6.G.238.239; 6.G.238.154; 6.G.238.157;
6.G.238.166; 6.G.238.169; 6.G.238.172; 6.G.238.175; 6.G.238.240;
6.G.238.244; 6.G.239.228; 6.G.239.229; 6.G.239.230; 6.G.239.231;
6.G.239.236; 6.G.239.237; 6.G.239.238; 6.G.239.239; 6.G.239.154;
6.G.239.157; 6.G.239.166; 6.G.239.169; 6.G.239.172; 6.G.239.175;
6.G.239.240; 6.G.239.244; 6.G.154.228; 6.G.154.229; 6.G.154.230;
6.G.154.231; 6.G.154.236; 6.G.154.237; 6.G.154.238; 6.G.154.239;
6.G.154.154; 6.G.154.157; 6.G.154.166; 6.G.154.169; 6.G.154.172;
6.G.154.175; 6.G.154.240; 6.G.154.244; 6.G.157.228; 6.G.157.229;
6.G.157.230; 6.G.157.231; 6.G.157.236; 6.G.157.237; 6.G.157.238;
6.G.157.239; 6.G.157.154; 6.G.157.157; 6.G.157.166; 6.G.157.169;
6.G.157.172; 6.G.157.175; 6.G.157.240; 6.G.157.244; 6.G.166.228;
6.G.166.229; 6.G.166.230; 6.G.166.231; 6.G.166.236; 6.G.166.237;
6.G.166.238; 6.G.166.239; 6.G.166.154; 6.G.166.157; 6.G.166.166;
6.G.166.169; 6.G.166.172; 6.G.166.175; 6.G.166.240; 6.G.166.244;
6.G.169.228; 6.G.169.229; 6.G.169.230; 6.G.169.231; 6.G.169.236;
6.G.169.237; 6.G.169.238; 6.G.169.239; 6.G.169.154; 6.G.169.157;
6.G.169.166; 6.G.169.169; 6.G.169.172; 6.G.169.175; 6.G.169.240;
6.G.169.244; 6.G.172.228; 6.G.172.229; 6.G.172.230; 6.G.172.231;
6.G.172.236; 6.G.172.237; 6.G.172.238; 6.G.172.239; 6.G.172.154;
6.G.172.157; 6.G.172.166; 6.G.172.169; 6.G.172.172; 6.G.172.175;
6.G.172.240; 6.G.172.244; 6.G.175.228; 6.G.175.229; 6.G.175.230;
6.G.175.231; 6.G.175.236; 6.G.175.237; 6.G.175.238; 6.G.175.239;
6.G.175.154; 6.G.175.157; 6.G.175.166; 6.G.175.169; 6.G.175.172;
6.G.175.175; 6.G.175.240; 6.G.175.244; 6.G.240.228; 6.G.240.229;
6.G.240.230; 6.G.240.231; 6.G.240.236; 6.G.240.237; 6.G.240.238;
6.G.240.239; 6.G.240.154; 6.G.240.157; 6.G.240.166; 6.G.240.169;
6.G.240.172; 6.G.240.175; 6.G.240.240; 6.G.240.244; 6.G.244.228;
6.G.244.229; 6.G.244.230; 6.G.244.231; 6.G.244.236; 6.G.244.237;
6.G.244.238; 6.G.244.239; 6.G.244.154; 6.G.244.157; 6.G.244.166;
6.G.244.169; 6.G.244.172; 6.G.244.175; 6.G.244.240; 6.G.244.244;
Prodrugs of 6.I 6.I.228.228; 6.I.228.229; 6.I.228.230; 6.I.228.231;
6.I.228.236; 6.I.228.237; 6.I.228.238; 6.I.228.239; 6.I.228.154;
6.I.228.157; 6.I.228.166; 6.I.228.169; 6.I.228.172; 6.I.228.175;
6.I.228.240; 6.I.228.244; 6.I.229.228; 6.I.229.229; 6.I.229.230;
6.I.229.231; 6.I.229.236; 6.I.229.237; 6.I.229.238; 6.I.229.239;
6.I.229.154; 6.I.229.157; 6.I.229.166; 6.I.229.169; 6.I.229.172;
6.I.229.175; 6.I.229.240; 6.I.229.244; 6.I.230.228; 6.I.230.229;
6.I.230.230; 6.I.230.231; 6.I.230.236; 6.I.230.237; 6.I.230.238;
6.I.230.239; 6.I.230.154; 6.I.230.157; 6.I.230.166; 6.I.230.169;
6.I.230.172; 6.I.230.175; 6.I.230.240; 6.I.230.244; 6.I.231.228;
6.I.231.229; 6.I.231.230; 6.I.231.231; 6.I.231.236; 6.I.231.237;
6.I.231.238; 6.I.231.239; 6.I.231.154; 6.I.231.157; 6.I.231.166;
6.I.231.169; 6.I.231.172; 6.I.231.175; 6.I.231.240; 6.I.231.244;
6.I.236.228; 6.I.236.229; 6.I.236.230; 6.I.236.231; 6.I.236.236;
6.I.236.237; 6.I.236.238; 6.I.236.239; 6.I.236.154; 6.I.236.157;
6.I.236.166; 6.I.236.169; 6.I.236.172; 6.I.236.175; 6.I.236.240;
6.I.236.244; 6.I.237.228; 6.I.237.229; 6.I.237.230; 6.I.237.231;
6.I.237.236; 6.I.237.237; 6.I.237.238; 6.I.237.239; 6.I.237.154;
6.I.237.157; 6.I.237.166; 6.I.237.169; 6.I.237.172; 6.I.237.175;
6.I.237.240; 6.I.237.244; 6.I.238.228; 6.I.238.229; 6.I.238.230;
6.I.238.231; 6.I.238.236; 6.I.238.237; 6.I.238.238; 6.I.238.239;
6.I.238.154; 6.I.238.157; 6.I.238.166; 6.I.238.169; 6.I.238.172;
6.I.238.175; 6.I.238.240; 6.I.238.244; 6.I.239.228; 6.I.239.229;
6.I.239.230; 6.I.239.231; 6.I.239.236; 6.I.239.237; 6.I.239.238;
6.I.239.239; 6.I.239.154; 6.I.239.157; 6.I.239.166; 6.I.239.169;
6.I.239.172; 6.I.239.175; 6.I.239.240; 6.I.239.244; 6.I.154.228;
6.I.154.229; 6.I.154.230; 6.I.154.231; 6.I.154.236; 6.I.154.237;
6.I.154.238; 6.I.154.239; 6.I.154.154; 6.I.154.157; 6.I.154.166;
6.I.154.169; 6.I.154.172; 6.I.154.175; 6.I.154.240; 6.I.154.244;
6.I.157.228; 6.I.157.229; 6.I.157.230; 6.I.157.231; 6.I.157.236;
6.I.157.237; 6.I.157.238; 6.I.157.239; 6.I.157.154; 6.I.157.157;
6.I.157.166; 6.I.157.169; 6.I.157.172; 6.I.157.175; 6.I.157.240;
6.I.157.244; 6.I.166.228; 6.I.166.229; 6.I.166.230; 6.I.166.231;
6.I.166.236; 6.I.166.237; 6.I.166.238; 6.I.166.239; 6.I.166.154;
6.I.166.157; 6.I.166.166; 6.I.166.169; 6.I.166.172; 6.I.166.175;
6.I.166.240; 6.I.166.244; 6.I.169.228; 6.I.169.229; 6.I.169.230;
6.I.169.231; 6.I.169.236; 6.I.169.237; 6.I.169.238; 6.I.169.239;
6.I.169.154; 6.I.169.157; 6.I.169.166; 6.I.169.169; 6.I.169.172;
6.I.169.175; 6.I.169.240; 6.I.169.244; 6.I.172.228; 6.I.172.229;
6.I.172.230; 6.I.172.231; 6.I.172.236; 6.I.172.237; 6.I.172.238;
6.I.172.239; 6.I.172.154; 6.I.172.157; 6.I.172.166; 6.I.172.169;
6.I.172.172; 6.I.172.175; 6.I.172.240; 6.I.172.244; 6.I.175.228;
6.I.175.229; 6.I.175.230; 6.I.175.231; 6.I.175.236; 6.I.175.237;
6.I.175.238; 6.I.175.239; 6.I.175.154; 6.I.175.157; 6.I.175.166;
6.I.175.169; 6.I.175.172; 6.I.175.175; 6.I.175.240; 6.I.175.244;
6.I.240.228; 6.I.240.229; 6.I.240.230; 6.I.240.231; 6.I.240.236;
6.I.240.237; 6.I.240.238; 6.I.240.239; 6.I.240.154; 6.I.240.157;
6.I.240.166; 6.I.240.169; 6.I.240.172; 6.I.240.175; 6.I.240.240;
6.I.240.244; 6.I.244.228; 6.I.244.229; 6.I.244.230; 6.I.244.231;
6.I.244.236; 6.I.244.237; 6.I.244.238; 6.I.244.239; 6.I.244.154;
6.I.244.157; 6.I.244.166; 6.I.244.169; 6.I.244.172; 6.I.244.175;
6.I.244.240; 6.I.244.244; Prodrugs of 6.J 6.J.228.228; 6.J.228.229;
6.J.228.230; 6.J.228.231; 6.J.228.236; 6.J.228.237; 6.J.228.238;
6.J.228.239; 6.J.228.154; 6.J.228.157; 6.J.228.166; 6.J.228.169;
6.J.228.172; 6.J.228.175; 6.J.228.240; 6.J.228.244; 6.J.229.228;
6.J.229.229; 6.J.229.230; 6.J.229.231; 6.J.229.236; 6.J.229.237;
6.J.229.238; 6.J.229.239; 6.J.229.154; 6.J.229.157; 6.J.229.166;
6.J.229.169; 6.J.229.172; 6.J.229.175; 6.J.229.240; 6.J.229.244;
6.J.230.228; 6.J.230.229; 6.J.230.230; 6.J.230.231; 6.J.230.236;
6.J.230.237; 6.J.230.238; 6.J.230.239; 6.J.230.154; 6.J.230.157;
6.J.230.166; 6.J.230.169; 6.J.230.172; 6.J.230.175; 6.J.230.240;
6.J.230.244; 6.J.231.228; 6.J.231.229; 6.J.231.230; 6.J.231.231;
6.J.231.236; 6.J.231.237; 6.J.231.238; 6.J.231.239; 6.J.231.154;
6.J.231.157; 6.J.231.166; 6.J.231.169; 6.J.231.172; 6.J.231.175;
6.J.231.240; 6.J.231.244; 6.J.236.228; 6.J.236.229; 6.J.236.230;
6.J.236.231; 6.J.236.236; 6.J.236.237; 6.J.236.238; 6.J.236.239;
6.J.236.154; 6.J.236.157; 6.J.236.166; 6.J.236.169; 6.J.236.172;
6.J.236.175; 6.J.236.240; 6.J.236.244; 6.J.237.228; 6.J.237.229;
6.J.237.230; 6.J.237.231; 6.J.237.236; 6.J.237.237; 6.J.237.238;
6.J.237.239; 6.J.237.154; 6.J.237.157; 6.J.237.166; 6.J.237.169;
6.J.237.172; 6.J.237.175; 6.J.237.240; 6.J.237.244; 6.J.238.228;
6.J.238.229; 6.J.238.230; 6.J.238.231; 6.J.238.236; 6.J.238.237;
6.J.238.238; 6.J.238.239; 6.J.238.154; 6.J.238.157; 6.J.238.166;
6.J.238.169; 6.J.238.172; 6.J.238.175; 6.J.238.240; 6.J.238.244;
6.J.239.228; 6.J.239.229; 6.J.239.230; 6.J.239.231; 6.J.239.236;
6.J.239.237; 6.J.239.238; 6.J.239.239; 6.J.239.154; 6.J.239.157;
6.J.239.166; 6.J.239.169; 6.J.239.172; 6.J.239.175; 6.J.239.240;
6.J.239.244; 6.J.154.228; 6.J.154.229; 6.J.154.230; 6.J.154.231;
6.J.154.236; 6.J.154.237; 6.J.154.238; 6.J.154.239; 6.J.154.154;
6.J.154.157; 6.J.154.166; 6.J.154.169; 6.J.154.172; 6.J.154.175;
6.J.154.240; 6.J.154.244; 6.J.157.228; 6.J.157.229; 6.J.157.230;
6.J.157.231; 6.J.157.236; 6.J.157.237; 6.J.157.238; 6.J.157.239;
6.J.157.154; 6.J.157.157; 6.J.157.166; 6.J.157.169; 6.J.157.172;
6.J.157.175; 6.J.157.240; 6.J.157.244; 6.J.166.228; 6.J.166.229;
6.J.166.230; 6.J.166.231; 6.J.166.236; 6.J.166.237; 6.J.166.238;
6.J.166.239; 6.J.166.154; 6.J.166.157; 6.J.166.166; 6.J.166.169;
6.J.166.172; 6.J.166.175; 6.J.166.240; 6.J.166.244; 6.J.169.228;
6.J.169.229; 6.J.169.230; 6.J.169.231; 6.J.169.236; 6.J.169.237;
6.J.169.238; 6.J.169.239; 6.J.169.154; 6.J.169.157; 6.J.169.166;
6.J.169.169; 6.J.169.172; 6.J.169.175; 6.J.169.240; 6.J.169.244;
6.J.172.228; 6.J.172.229; 6.J.172.230; 6.J.172.231; 6.J.172.236;
6.J.172.237; 6.J.172.238; 6.J.172.239; 6.J.172.154; 6.J.172.157;
6.J.172.166; 6.J.172.169; 6.J.172.172; 6.J.172.175; 6.J.172.240;
6.J.172.244; 6.J.175.228; 6.J.175.229; 6.J.175.230; 6.J.175.231;
6.J.175.236; 6.J.175.237; 6.J.175.238; 6.J.175.239; 6.J.175.154;
6.J.175.157; 6.J.175.166; 6.J.175.169; 6.J.175.172; 6.J.175.175;
6.J.175.240; 6.J.175.244; 6.J.240.228; 6.J.240.229; 6.J.240.230;
6.J.240.231; 6.J.240.236; 6.J.240.237; 6.J.240.238; 6.J.240.239;
6.J.240.154; 6.J.240.157; 6.J.240.166; 6.J.240.169; 6.J.240.172;
6.J.240.175; 6.J.240.240; 6.J.240.244; 6.J.244.228; 6.J.244.229;
6.J.244.230; 6.J.244.231; 6.J.244.236; 6.J.244.237; 6.J.244.238;
6.J.244.239; 6.J.244.154; 6.J.244.157; 6.J.244.166; 6.J.244.169;
6.J.244.172; 6.J.244.175; 6.J.244.240; 6.J.244.244; Prodrugs of 6.L
6.L.228.228; 6.L.228.229; 6.L.228.230; 6.L.228.231; 6.L.228.236;
6.L.228.237; 6.L.228.238; 6.L.228.239; 6.L.228.154; 6.L.228.157;
6.L.228.166; 6.L.228.169; 6.L.228.172; 6.L.228.175; 6.L.228.240;
6.L.228.244; 6.L.229.228; 6.L.229.229; 6.L.229.230; 6.L.229.231;
6.L.229.236; 6.L.229.237; 6.L.229.238; 6.L.229.239; 6.L.229.154;
6.L.229.157; 6.L.229.166; 6.L.229.169; 6.L.229.172; 6.L.229.175;
6.L.229.240; 6.L.229.244; 6.L.230.228; 6.L.230.229; 6.L.230.230;
6.L.230.231; 6.L.230.236; 6.L.230.237; 6.L.230.238; 6.L.230.239;
6.L.230.154; 6.L.230.157; 6.L.230.166; 6.L.230.169; 6.L.230.172;
6.L.230.175; 6.L.230.240; 6.L.230.244; 6.L.231.228; 6.L.231.229;
6.L.231.230; 6.L.231.231; 6.L.231.236; 6.L.231.237; 6.L.231.238;
6.L.231.239; 6.L.231.154; 6.L.231.157; 6.L.231.166;
6.L.231.169;
6.L.231.172; 6.L.231.175; 6.L.231.240; 6.L.231.244; 6.L.236.228;
6.L.236.229; 6.L.236.230; 6.L.236.231; 6.L.236.236; 6.L.236.237;
6.L.236.238; 6.L.236.239; 6.L.236.154; 6.L.236.157; 6.L.236.166;
6.L.236.169; 6.L.236.172; 6.L.236.175; 6.L.236.240; 6.L.236.244;
6.L.237.228; 6.L.237.229; 6.L.237.230; 6.L.237.231; 6.L.237.236;
6.L.237.237; 6.L.237.238; 6.L.237.239; 6.L.237.154; 6.L.237.157;
6.L.237.166; 6.L.237.169; 6.L.237.172; 6.L.237.175; 6.L.237.240;
6.L.237.244; 6.L.238.228; 6.L.238.229; 6.L.238.230; 6.L.238.231;
6.L.238.236; 6.L.238.237; 6.L.238.238; 6.L.238.239; 6.L.238.154;
6.L.238.157; 6.L.238.166; 6.L.238.169; 6.L.238.172; 6.L.238.175;
6.L.238.240; 6.L.238.244; 6.L.239.228; 6.L.239.229; 6.L.239.230;
6.L.239.231; 6.L.239.236; 6.L.239.237; 6.L.239.238; 6.L.239.239;
6.L.239.154; 6.L.239.157; 6.L.239.166; 6.L.239.169; 6.L.239.172;
6.L.239.175; 6.L.239.240; 6.L.239.244; 6.L.154.228; 6.L.154.229;
6.L.154.230; 6.L.154.231; 6.L.154.236; 6.L.154.237; 6.L.154.238;
6.L.154.239; 6.L.154.154; 6.L.154.157; 6.L.154.166; 6.L.154.169;
6.L.154.172; 6.L.154.175; 6.L.154.240; 6.L.154.244; 6.L.157.228;
6.L.157.229; 6.L.157.230; 6.L.157.231; 6.L.157.236; 6.L.157.237;
6.L.157.238; 6.L.157.239; 6.L.157.154; 6.L.157.157; 6.L.157.166;
6.L.157.169; 6.L.157.172; 6.L.157.175; 6.L.157.240; 6.L.157.244;
6.L.166.228; 6.L.166.229; 6.L.166.230; 6.L.166.231; 6.L.166.236;
6.L.166.237; 6.L.166.238; 6.L.166.239; 6.L.166.154; 6.L.166.157;
6.L.166.166; 6.L.166.169; 6.L.166.172; 6.L.166.175; 6.L.166.240;
6.L.166.244; 6.L.169.228; 6.L.169.229; 6.L.169.230; 6.L.169.231;
6.L.169.236; 6.L.169.237; 6.L.169.238; 6.L.169.239; 6.L.169.154;
6.L.169.157; 6.L.169.166; 6.L.169.169; 6.L.169.172; 6.L.169.175;
6.L.169.240; 6.L.169.244; 6.L.172.228; 6.L.172.229; 6.L.172.230;
6.L.172.231; 6.L.172.236; 6.L.172.237; 6.L.172.238; 6.L.172.239;
6.L.172.154; 6.L.172.157; 6.L.172.166; 6.L.172.169; 6.L.172.172;
6.L.172.175; 6.L.172.240; 6.L.172.244; 6.L.175.228; 6.L.175.229;
6.L.175.230; 6.L.175.231; 6.L.175.236; 6.L.175.237; 6.L.175.238;
6.L.175.239; 6.L.175.154; 6.L.175.157; 6.L.175.166; 6.L.175.169;
6.L.175.172; 6.L.175.175; 6.L.175.240; 6.L.175.244; 6.L.240.228;
6.L.240.229; 6.L.240.230; 6.L.240.231; 6.L.240.236; 6.L.240.237;
6.L.240.238; 6.L.240.239; 6.L.240.154; 6.L.240.157; 6.L.240.166;
6.L.240.169; 6.L.240.172; 6.L.240.175; 6.L.240.240; 6.L.240.244;
6.L.244.228; 6.L.244.229; 6.L.244.230; 6.L.244.231; 6.L.244.236;
6.L.244.237; 6.L.244.238; 6.L.244.239; 6.L.244.154; 6.L.244.157;
6.L.244.166; 6.L.244.169; 6.L.244.172; 6.L.244.175; 6.L.244.240;
6.L.244.244; Prodrugs of 6.O 6.O.228.228; 6.O.228.229; 6.O.228.230;
6.O.228.231; 6.O.228.236; 6.O.228.237; 6.O.228.238; 6.O.228.239;
6.O.228.154; 6.O.228.157; 6.O.228.166; 6.O.228.169; 6.O.228.172;
6.O.228.175; 6.O.228.240; 6.O.228.244; 6.O.229.228; 6.O.229.229;
6.O.229.230; 6.O.229.231; 6.O.229.236; 6.O.229.237; 6.O.229.238;
6.O.229.239; 6.O.229.154; 6.O.229.157; 6.O.229.166; 6.O.229.169;
6.O.229.172; 6.O.229.175; 6.O.229.240; 6.O.229.244; 6.O.230.228;
6.O.230.229; 6.O.230.230; 6.O.230.231; 6.O.230.236; 6.O.230.237;
6.O.230.238; 6.O.230.239; 6.O.230.154; 6.O.230.157; 6.O.230.166;
6.O.230.169; 6.O.230.172; 6.O.230.175; 6.O.230.240; 6.O.230.244;
6.O.231.228; 6.O.231.229; 6.O.231.230; 6.O.231.231; 6.O.231.236;
6.O.231.237; 6.O.231.238; 6.O.231.239; 6.O.231.154; 6.O.231.157;
6.O.231.166; 6.O.231.169; 6.O.231.172; 6.O.231.175; 6.O.231.240;
6.O.231.244; 6.O.236.228; 6.O.236.229; 6.O.236.230; 6.O.236.231;
6.O.236.236; 6.O.236.237; 6.O.236.238; 6.O.236.239; 6.O.236.154;
6.O.236.157; 6.O.236.166; 6.O.236.169; 6.O.236.172; 6.O.236.175;
6.O.236.240; 6.O.236.244; 6.O.237.228; 6.O.237.229; 6.O.237.230;
6.O.237.231; 6.O.237.236; 6.O.237.237; 6.O.237.238; 6.O.237.239;
6.O.237.154; 6.O.237.157; 6.O.237.166; 6.O.237.169; 6.O.237.172;
6.O.237.175; 6.O.237.240; 6.O.237.244; 6.O.238.228; 6.O.238.229;
6.O.238.230; 6.O.238.231; 6.O.238.236; 6.O.238.237; 6.O.238.238;
6.O.238.239; 6.O.238.154; 6.O.238.157; 6.O.238.166; 6.O.238.169;
6.O.238.172; 6.O.238.175; 6.O.238.240; 6.O.238.244; 6.O.239.228;
6.O.239.229; 6.O.239.230; 6.O.239.231; 6.O.239.236; 6.O.239.237;
6.O.239.238; 6.O.239.239; 6.O.239.154; 6.O.239.157; 6.O.239.166;
6.O.239.169; 6.O.239.172; 6.O.239.175; 6.O.239.240; 6.O.239.244;
6.O.154.228; 6.O.154.229; 6.O.154.230; 6.O.154.231; 6.O.154.236;
6.O.154.237; 6.O.154.238; 6.O.154.239; 6.O.154.154; 6.O.154.157;
6.O.154.166; 6.O.154.169; 6.O.154.172; 6.O.154.175; 6.O.154.240;
6.O.154.244; 6.O.157.228; 6.O.157.229; 6.O.157.230; 6.O.157.231;
6.O.157.236; 6.O.157.237; 6.O.157.238; 6.O.157.239; 6.O.157.154;
6.O.157.157; 6.O.157.166; 6.O.157.169; 6.O.157.172; 6.O.157.175;
6.O.157.240; 6.O.157.244; 6.O.166.228; 6.O.166.229; 6.O.166.230;
6.O.166.231; 6.O.166.236; 6.O.166.237; 6.O.166.238; 6.O.166.239;
6.O.166.154; 6.O.166.157; 6.O.166.166; 6.O.166.169; 6.O.166.172;
6.O.166.175; 6.O.166.240; 6.O.166.244; 6.O.169.228; 6.O.169.229;
6.O.169.230; 6.O.169.231; 6.O.169.236; 6.O.169.237; 6.O.169.238;
6.O.169.239; 6.O.169.154; 6.O.169.157; 6.O.169.166; 6.O.169.169;
6.O.169.172; 6.O.169.175; 6.O.169.240; 6.O.169.244; 6.O.172.228;
6.O.172.229; 6.O.172.230; 6.O.172.231; 6.O.172.236; 6.O.172.237;
6.O.172.238; 6.O.172.239; 6.O.172.154; 6.O.172.157; 6.O.172.166;
6.O.172.169; 6.O.172.172; 6.O.172.175; 6.O.172.240; 6.O.172.244;
6.O.175.228; 6.O.175.229; 6.O.175.230; 6.O.175.231; 6.O.175.236;
6.O.175.237; 6.O.175.238; 6.O.175.239; 6.O.175.154; 6.O.175.157;
6.O.175.166; 6.O.175.169; 6.O.175.172; 6.O.175.175; 6.O.175.240;
6.O.175.244; 6.O.240.228; 6.O.240.229; 6.O.240.230; 6.O.240.231;
6.O.240.236; 6.O.240.237; 6.O.240.238; 6.O.240.239; 6.O.240.154;
6.O.240.157; 6.O.240.166; 6.O.240.169; 6.O.240.172; 6.O.240.175;
6.O.240.240; 6.O.240.244; 6.O.244.228; 6.O.244.229; 6.O.244.230;
6.O.244.231; 6.O.244.236; 6.O.244.237; 6.O.244.238; 6.O.244.239;
6.O.244.154; 6.O.244.157; 6.O.244.166; 6.O.244.169; 6.O.244.172;
6.O.244.175; 6.O.244.240; 6.O.244.244; Prodrugs of 6.P 6.P.228.228;
6.P.228.229; 6.P.228.230; 6.P.228.231; 6.P.228.236; 6.P.228.237;
6.P.228.238; 6.P.228.239; 6.P.228.154; 6.P.228.157; 6.P.228.166;
6.P.228.169; 6.P.228.172; 6.P.228.175; 6.P.228.240; 6.P.228.244;
6.P.229.228; 6.P.229.229; 6.P.229.230; 6.P.229.231; 6.P.229.236;
6.P.229.237; 6.P.229.238; 6.P.229.239; 6.P.229.154; 6.P.229.157;
6.P.229.166; 6.P.229.169; 6.P.229.172; 6.P.229.175; 6.P.229.240;
6.P.229.244; 6.P.230.228; 6.P.230.229; 6.P.230.230; 6.P.230.231;
6.P.230.236; 6.P.230.237; 6.P.230.238; 6.P.230.239; 6.P.230.154;
6.P.230.157; 6.P.230.166; 6.P.230.169; 6.P.230.172; 6.P.230.175;
6.P.230.240; 6.P.230.244; 6.P.231.228; 6.P.231.229; 6.P.231.230;
6.P.231.231; 6.P.231.236; 6.P.231.237; 6.P.231.238; 6.P.231.239;
6.P.231.154; 6.P.231.157; 6.P.231.166; 6.P.231.169; 6.P.231.172;
6.P.231.175; 6.P.231.240; 6.P.231.244; 6.P.236.228; 6.P.236.229;
6.P.236.230; 6.P.236.231; 6.P.236.236; 6.P.236.237; 6.P.236.238;
6.P.236.239; 6.P.236.154; 6.P.236.157; 6.P.236.166; 6.P.236.169;
6.P.236.172; 6.P.236.175; 6.P.236.240; 6.P.236.244; 6.P.237.228;
6.P.237.229; 6.P.237.230; 6.P.237.231; 6.P.237.236; 6.P.237.237;
6.P.237.238; 6.P.237.239; 6.P.237.154; 6.P.237.157; 6.P.237.166;
6.P.237.169; 6.P.237.172; 6.P.237.175; 6.P.237.240; 6.P.237.244;
6.P.238.228; 6.P.238.229; 6.P.238.230; 6.P.238.231; 6.P.238.236;
6.P.238.237; 6.P.238.238; 6.P.238.239; 6.P.238.154; 6.P.238.157;
6.P.238.166; 6.P.238.169; 6.P.238.172; 6.P.238.175; 6.P.238.240;
6.P.238.244; 6.P.239.228; 6.P.239.229; 6.P.239.230; 6.P.239.231;
6.P.239.236; 6.P.239.237; 6.P.239.238; 6.P.239.239; 6.P.239.154;
6.P.239.157; 6.P.239.166; 6.P.239.169; 6.P.239.172; 6.P.239.175;
6.P.239.240; 6.P.239.244; 6.P.154.228; 6.P.154.229; 6.P.154.230;
6.P.154.231; 6.P.154.236; 6.P.154.237; 6.P.154.238; 6.P.154.239;
6.P.154.154; 6.P.154.157; 6.P.154.166; 6.P.154.169; 6.P.154.172;
6.P.154.175; 6.P.154.240; 6.P.154.244; 6.P.157.228; 6.P.157.229;
6.P.157.230; 6.P.157.231; 6.P.157.236; 6.P.157.237; 6.P.157.238;
6.P.157.239; 6.P.157.154; 6.P.157.157; 6.P.157.166; 6.P.157.169;
6.P.157.172; 6.P.157.175; 6.P.157.240; 6.P.157.244; 6.P.166.228;
6.P.166.229; 6.P.166.230; 6.P.166.231; 6.P.166.236; 6.P.166.237;
6.P.166.238; 6.P.166.239; 6.P.166.154; 6.P.166.157; 6.P.166.166;
6.P.166.169; 6.P.166.172; 6.P.166.175; 6.P.166.240; 6.P.166.244;
6.P.169.228; 6.P.169.229; 6.P.169.230; 6.P.169.231; 6.P.169.236;
6.P.169.237; 6.P.169.238; 6.P.169.239; 6.P.169.154; 6.P.169.157;
6.P.169.166; 6.P.169.169; 6.P.169.172; 6.P.169.175; 6.P.169.240;
6.P.169.244; 6.P.172.228; 6.P.172.229; 6.P.172.230; 6.P.172.231;
6.P.172.236; 6.P.172.237; 6.P.172.238; 6.P.172.239; 6.P.172.154;
6.P.172.157; 6.P.172.166; 6.P.172.169; 6.P.172.172; 6.P.172.175;
6.P.172.240; 6.P.172.244; 6.P.175.228; 6.P.175.229; 6.P.175.230;
6.P.175.231; 6.P.175.236; 6.P.175.237; 6.P.175.238; 6.P.175.239;
6.P.175.154; 6.P.175.157; 6.P.175.166; 6.P.175.169; 6.P.175.172;
6.P.175.175; 6.P.175.240; 6.P.175.244; 6.P.240.228; 6.P.240.229;
6.P.240.230; 6.P.240.231; 6.P.240.236; 6.P.240.237; 6.P.240.238;
6.P.240.239; 6.P.240.154; 6.P.240.157; 6.P.240.166; 6.P.240.169;
6.P.240.172; 6.P.240.175; 6.P.240.240; 6.P.240.244; 6.P.244.228;
6.P.244.229; 6.P.244.230; 6.P.244.231; 6.P.244.236; 6.P.244.237;
6.P.244.238; 6.P.244.239; 6.P.244.154; 6.P.244.157; 6.P.244.166;
6.P.244.169; 6.P.244.172; 6.P.244.175; 6.P.244.240; 6.P.244.244;
Prodrugs of 6.U 6.U.228.228; 6.U.228.229; 6.U.228.230; 6.U.228.231;
6.U.228.236; 6.U.228.237; 6.U.228.238; 6.U.228.239; 6.U.228.154;
6.U.228.157; 6.U.228.166; 6.U.228.169; 6.U.228.172; 6.U.228.175;
6.U.228.240; 6.U.228.244; 6.U.229.228; 6.U.229.229; 6.U.229.230;
6.U.229.231; 6.U.229.236; 6.U.229.237; 6.U.229.238; 6.U.229.239;
6.U.229.154; 6.U.229.157; 6.U.229.166; 6.U.229.169; 6.U.229.172;
6.U.229.175; 6.U.229.240; 6.U.229.244; 6.U.230.228; 6.U.230.229;
6.U.230.230; 6.U.230.231; 6.U.230.236; 6.U.230.237; 6.U.230.238;
6.U.230.239; 6.U.230.154; 6.U.230.157; 6.U.230.166; 6.U.230.169;
6.U.230.172; 6.U.230.175; 6.U.230.240; 6.U.230.244; 6.U.231.228;
6.U.231.229; 6.U.231.230; 6.U.231.231; 6.U.231.236; 6.U.231.237;
6.U.231.238; 6.U.231.239; 6.U.231.154; 6.U.231.157; 6.U.231.166;
6.U.231.169; 6.U.231.172; 6.U.231.175; 6.U.231.240; 6.U.231.244;
6.U.236.228; 6.U.236.229; 6.U.236.230; 6.U.236.231; 6.U.236.236;
6.U.236.237; 6.U.236.238; 6.U.236.239; 6.U.236.154; 6.U.236.157;
6.U.236.166; 6.U.236.169; 6.U.236.172; 6.U.236.175; 6.U.236.240;
6.U.236.244; 6.U.237.228; 6.U.237.229; 6.U.237.230; 6.U.237.231;
6.U.237.236; 6.U.237.237; 6.U.237.238; 6.U.237.239; 6.U.237.154;
6.U.237.157; 6.U.237.166; 6.U.237.169; 6.U.237.172; 6.U.237.175;
6.U.237.240; 6.U.237.244; 6.U.238.228; 6.U.238.229; 6.U.238.230;
6.U.238.231; 6.U.238.236; 6.U.238.237; 6.U.238.238; 6.U.238.239;
6.U.238.154; 6.U.238.157; 6.U.238.166; 6.U.238.169; 6.U.238.172;
6.U.238.175; 6.U.238.240; 6.U.238.244; 6.U.239.228; 6.U.239.229;
6.U.239.230; 6.U.239.231; 6.U.239.236; 6.U.239.237; 6.U.239.238;
6.U.239.239; 6.U.239.154; 6.U.239.157; 6.U.239.166; 6.U.239.169;
6.U.239.172; 6.U.239.175; 6.U.239.240; 6.U.239.244; 6.U.154.228;
6.U.154.229; 6.U.154.230; 6.U.154.231; 6.U.154.236; 6.U.154.237;
6.U.154.238; 6.U.154.239; 6.U.154.154; 6.U.154.157; 6.U.154.166;
6.U.154.169; 6.U.154.172; 6.U.154.175; 6.U.154.240; 6.U.154.244;
6.U.157.228; 6.U.157.229; 6.U.157.230; 6.U.157.231; 6.U.157.236;
6.U.157.237; 6.U.157.238; 6.U.157.239; 6.U.157.154; 6.U.157.157;
6.U.157.166; 6.U.157.169; 6.U.157.172; 6.U.157.175; 6.U.157.240;
6.U.157.244; 6.U.166.228; 6.U.166.229; 6.U.166.230; 6.U.166.231;
6.U.166.236; 6.U.166.237; 6.U.166.238; 6.U.166.239; 6.U.166.154;
6.U.166.157; 6.U.166.166; 6.U.166.169; 6.U.166.172; 6.U.166.175;
6.U.166.240; 6.U.166.244; 6.U.169.228; 6.U.169.229; 6.U.169.230;
6.U.169.231; 6.U.169.236; 6.U.169.237; 6.U.169.238; 6.U.169.239;
6.U.169.154; 6.U.169.157; 6.U.169.166; 6.U.169.169; 6.U.169.172;
6.U.169.175; 6.U.169.240; 6.U.169.244; 6.U.172.228; 6.U.172.229;
6.U.172.230; 6.U.172.231; 6.U.172.236; 6.U.172.237; 6.U.172.238;
6.U.172.239; 6.U.172.154; 6.U.172.157; 6.U.172.166; 6.U.172.169;
6.U.172.172; 6.U.172.175; 6.U.172.240; 6.U.172.244; 6.U.175.228;
6.U.175.229; 6.U.175.230; 6.U.175.231; 6.U.175.236; 6.U.175.237;
6.U.175.238; 6.U.175.239; 6.U.175.154; 6.U.175.157; 6.U.175.166;
6.U.175.169; 6.U.175.172; 6.U.175.175; 6.U.175.240; 6.U.175.244;
6.U.240.228; 6.U.240.229; 6.U.240.230; 6.U.240.231; 6.U.240.236;
6.U.240.237; 6.U.240.238; 6.U.240.239; 6.U.240.154; 6.U.240.157;
6.U.240.166; 6.U.240.169; 6.U.240.172; 6.U.240.175; 6.U.240.240;
6.U.240.244; 6.U.244.228; 6.U.244.229; 6.U.244.230; 6.U.244.231;
6.U.244.236; 6.U.244.237; 6.U.244.238; 6.U.244.239; 6.U.244.154;
6.U.244.157; 6.U.244.166; 6.U.244.169; 6.U.244.172; 6.U.244.175;
6.U.244.240; 6.U.244.244; Prodrugs of 6.W 6.W.228.228; 6.W.228.229;
6.W.228.230; 6.W.228.231; 6.W.228.236; 6.W.228.237; 6.W.228.238;
6.W.228.239; 6.W.228.154; 6.W.228.157; 6.W.228.166; 6.W.228.169;
6.W.228.172; 6.W.228.175; 6.W.228.240; 6.W.228.244; 6.W.229.228;
6.W.229.229; 6.W.229.230; 6.W.229.231; 6.W.229.236; 6.W.229.237;
6.W.229.238; 6.W.229.239; 6.W.229.154; 6.W.229.157; 6.W.229.166;
6.W.229.169; 6.W.229.172; 6.W.229.175; 6.W.229.240; 6.W.229.244;
6.W.230.228; 6.W.230.229; 6.W.230.230; 6.W.230.231; 6.W.230.236;
6.W.230.237; 6.W.230.238; 6.W.230.239; 6.W.230.154; 6.W.230.157;
6.W.230.166; 6.W.230.169; 6.W.230.172; 6.W.230.175; 6.W.230.240;
6.W.230.244; 6.W.231.228; 6.W.231.229; 6.W.231.230; 6.W.231.231;
6.W.231.236; 6.W.231.237; 6.W.231.238; 6.W.231.239; 6.W.231.154;
6.W.231.157; 6.W.231.166; 6.W.231.169; 6.W.231.172; 6.W.231.175;
6.W.231.240; 6.W.231.244; 6.W.236.228; 6.W.236.229; 6.W.236.230;
6.W.236.231; 6.W.236.236; 6.W.236.237; 6.W.236.238; 6.W.236.239;
6.W.236.154; 6.W.236.157; 6.W.236.166; 6.W.236.169; 6.W.236.172;
6.W.236.175; 6.W.236.240; 6.W.236.244; 6.W.237.228; 6.W.237.229;
6.W.237.230; 6.W.237.231; 6.W.237.236; 6.W.237.237; 6.W.237.238;
6.W.237.239; 6.W.237.154; 6.W.237.157; 6.W.237.166; 6.W.237.169;
6.W.237.172; 6.W.237.175; 6.W.237.240; 6.W.237.244; 6.W.238.228;
6.W.238.229; 6.W.238.230; 6.W.238.231; 6.W.238.236; 6.W.238.237;
6.W.238.238; 6.W.238.239; 6.W.238.154; 6.W.238.157; 6.W.238.166;
6.W.238.169; 6.W.238.172; 6.W.238.175; 6.W.238.240; 6.W.238.244;
6.W.239.228; 6.W.239.229; 6.W.239.230; 6.W.239.231; 6.W.239.236;
6.W.239.237; 6.W.239.238; 6.W.239.239; 6.W.239.154; 6.W.239.157;
6.W.239.166; 6.W.239.169; 6.W.239.172; 6.W.239.175; 6.W.239.240;
6.W.239.244; 6.W.154.228; 6.W.154.229; 6.W.154.230; 6.W.154.231;
6.W.154.236; 6.W.154.237; 6.W.154.238; 6.W.154.239; 6.W.154.154;
6.W.154.157; 6.W.154.166; 6.W.154.169; 6.W.154.172; 6.W.154.175;
6.W.154.240; 6.W.154.244; 6.W.157.228; 6.W.157.229; 6.W.157.230;
6.W.157.231; 6.W.157.236; 6.W.157.237; 6.W.157.238; 6.W.157.239;
6.W.157.154; 6.W.157.157; 6.W.157.166; 6.W.157.169; 6.W.157.172;
6.W.157.175; 6.W.157.240; 6.W.157.244; 6.W.166.228; 6.W.166.229;
6.W.166.230; 6.W.166.231; 6.W.166.236; 6.W.166.237; 6.W.166.238;
6.W.166.239; 6.W.166.154; 6.W.166.157; 6.W.166.166; 6.W.166.169;
6.W.166.172; 6.W.166.175; 6.W.166.240; 6.W.166.244; 6.W.169.228;
6.W.169.229; 6.W.169.230; 6.W.169.231; 6.W.169.236; 6.W.169.237;
6.W.169.238; 6.W.169.239; 6.W.169.154; 6.W.169.157; 6.W.169.166;
6.W.169.169; 6.W.169.172; 6.W.169.175; 6.W.169.240; 6.W.169.244;
6.W.172.228; 6.W.172.229; 6.W.172.230; 6.W.172.231; 6.W.172.236;
6.W.172.237; 6.W.172.238; 6.W.172.239; 6.W.172.154; 6.W.172.157;
6.W.172.166; 6.W.172.169; 6.W.172.172; 6.W.172.175; 6.W.172.240;
6.W.172.244; 6.W.175.228; 6.W.175.229; 6.W.175.230; 6.W.175.231;
6.W.175.236; 6.W.175.237; 6.W.175.238; 6.W.175.239; 6.W.175.154;
6.W.175.157; 6.W.175.166; 6.W.175.169; 6.W.175.172; 6.W.175.175;
6.W.175.240; 6.W.175.244; 6.W.240.228; 6.W.240.229; 6.W.240.230;
6.W.240.231; 6.W.240.236; 6.W.240.237; 6.W.240.238; 6.W.240.239;
6.W.240.154; 6.W.240.157; 6.W.240.166; 6.W.240.169; 6.W.240.172;
6.W.240.175; 6.W.240.240; 6.W.240.244; 6.W.244.228; 6.W.244.229;
6.W.244.230; 6.W.244.231; 6.W.244.236; 6.W.244.237; 6.W.244.238;
6.W.244.239; 6.W.244.154; 6.W.244.157; 6.W.244.166; 6.W.244.169;
6.W.244.172; 6.W.244.175; 6.W.244.240;
6.W.244.244; Prodrugs of 6.Y 6.Y.228.228; 6.Y.228.229; 6.Y.228.230;
6.Y.228.231; 6.Y.228.236; 6.Y.228.237; 6.Y.228.238; 6.Y.228.239;
6.Y.228.154; 6.Y.228.157; 6.Y.228.166; 6.Y.228.169; 6.Y.228.172;
6.Y.228.175; 6.Y.228.240; 6.Y.228.244; 6.Y.229.228; 6.Y.229.229;
6.Y.229.230; 6.Y.229.231; 6.Y.229.236; 6.Y.229.237; 6.Y.229.238;
6.Y.229.239; 6.Y.229.154; 6.Y.229.157; 6.Y.229.166; 6.Y.229.169;
6.Y.229.172; 6.Y.229.175; 6.Y.229.240; 6.Y.229.244; 6.Y.230.228;
6.Y.230.229; 6.Y.230.230; 6.Y.230.231; 6.Y.230.236; 6.Y.230.237;
6.Y.230.238; 6.Y.230.239; 6.Y.230.154; 6.Y.230.157; 6.Y.230.166;
6.Y.230.169; 6.Y.230.172; 6.Y.230.175; 6.Y.230.240; 6.Y.230.244;
6.Y.231.228; 6.Y.231.229; 6.Y.231.230; 6.Y.231.231; 6.Y.231.236;
6.Y.231.237; 6.Y.231.238; 6.Y.231.239; 6.Y.231.154; 6.Y.231.157;
6.Y.231.166; 6.Y.231.169; 6.Y.231.172; 6.Y.231.175; 6.Y.231.240;
6.Y.231.244; 6.Y.236.228; 6.Y.236.229; 6.Y.236.230; 6.Y.236.231;
6.Y.236.236; 6.Y.236.237; 6.Y.236.238; 6.Y.236.239; 6.Y.236.154;
6.Y.236.157; 6.Y.236.166; 6.Y.236.169; 6.Y.236.172; 6.Y.236.175;
6.Y.236.240; 6.Y.236.244; 6.Y.237.228; 6.Y.237.229; 6.Y.237.230;
6.Y.237.231; 6.Y.237.236; 6.Y.237.237; 6.Y.237.238; 6.Y.237.239;
6.Y.237.154; 6.Y.237.157; 6.Y.237.166; 6.Y.237.169; 6.Y.237.172;
6.Y.237.175; 6.Y.237.240; 6.Y.237.244; 6.Y.238.228; 6.Y.238.229;
6.Y.238.230; 6.Y.238.231; 6.Y.238.236; 6.Y.238.237; 6.Y.238.238;
6.Y.238.239; 6.Y.238.154; 6.Y.238.157; 6.Y.238.166; 6.Y.238.169;
6.Y.238.172; 6.Y.238.175; 6.Y.238.240; 6.Y.238.244; 6.Y.239.228;
6.Y.239.229; 6.Y.239.230; 6.Y.239.231; 6.Y.239.236; 6.Y.239.237;
6.Y.239.238; 6.Y.239.239; 6.Y.239.154; 6.Y.239.157; 6.Y.239.166;
6.Y.239.169; 6.Y.239.172; 6.Y.239.175; 6.Y.239.240; 6.Y.239.244;
6.Y.154.228; 6.Y.154.229; 6.Y.154.230; 6.Y.154.231; 6.Y.154.236;
6.Y.154.237; 6.Y.154.238; 6.Y.154.239; 6.Y.154.154; 6.Y.154.157;
6.Y.154.166; 6.Y.154.169; 6.Y.154.172; 6.Y.154.175; 6.Y.154.240;
6.Y.154.244; 6.Y.157.228; 6.Y.157.229; 6.Y.157.230; 6.Y.157.231;
6.Y.157.236; 6.Y.157.237; 6.Y.157.238; 6.Y.157.239; 6.Y.157.154;
6.Y.157.157; 6.Y.157.166; 6.Y.157.169; 6.Y.157.172; 6.Y.157.175;
6.Y.157.240; 6.Y.157.244; 6.Y.166.228; 6.Y.166.229; 6.Y.166.230;
6.Y.166.231; 6.Y.166.236; 6.Y.166.237; 6.Y.166.238; 6.Y.166.239;
6.Y.166.154; 6.Y.166.157; 6.Y.166.166; 6.Y.166.169; 6.Y.166.172;
6.Y.166.175; 6.Y.166.240; 6.Y.166.244; 6.Y.169.228; 6.Y.169.229;
6.Y.169.230; 6.Y.169.231; 6.Y.169.236; 6.Y.169.237; 6.Y.169.238;
6.Y.169.239; 6.Y.169.154; 6.Y.169.157; 6.Y.169.166; 6.Y.169.169;
6.Y.169.172; 6.Y.169.175; 6.Y.169.240; 6.Y.169.244; 6.Y.172.228;
6.Y.172.229; 6.Y.172.230; 6.Y.172.231; 6.Y.172.236; 6.Y.172.237;
6.Y.172.238; 6.Y.172.239; 6.Y.172.154; 6.Y.172.157; 6.Y.172.166;
6.Y.172.169; 6.Y.172.172; 6.Y.172.175; 6.Y.172.240; 6.Y.172.244;
6.Y.175.228; 6.Y.175.229; 6.Y.175.230; 6.Y.175.231; 6.Y.175.236;
6.Y.175.237; 6.Y.175.238; 6.Y.175.239; 6.Y.175.154; 6.Y.175.157;
6.Y.175.166; 6.Y.175.169; 6.Y.175.172; 6.Y.175.175; 6.Y.175.240;
6.Y.175.244; 6.Y.240.228; 6.Y.240.229; 6.Y.240.230; 6.Y.240.231;
6.Y.240.236; 6.Y.240.237; 6.Y.240.238; 6.Y.240.239; 6.Y.240.154;
6.Y.240.157; 6.Y.240.166; 6.Y.240.169; 6.Y.240.172; 6.Y.240.175;
6.Y.240.240; 6.Y.240.244; 6.Y.244.228; 6.Y.244.229; 6.Y.244.230;
6.Y.244.231; 6.Y.244.236; 6.Y.244.237; 6.Y.244.238; 6.Y.244.239;
6.Y.244.154; 6.Y.244.157; 6.Y.244.166; 6.Y.244.169; 6.Y.244.172;
6.Y.244.175; 6.Y.244.240; 6.Y.244.244; Prodrugs of 7.AH 7.AH.4.157;
7.AH.4.158; 7.AH.4.196; 7.AH.4.223; 7.AH.4.240; 7.AH.4.244;
7.AH.4.243; 7.AH.4.247; 7.AH.5.157; 7.AH.5.158; 7.AH.5.196;
7.AH.5.223; 7.AH.5.240; 7.AH.5.244; 7.AH.5.243; 7.AH.5.247;
7.AH.7.157; 7.AH.7.158; 7.AH.7.196; 7.AH.7.223; 7.AH.7.240;
7.AH.7.244; 7.AH.7.243; 7.AH.7.247; 7.AH.15.157; 7.AH.15.158;
7.AH.15.196; 7.AH.15.223; 7.AH.15.240; 7.AH.15.244; 7.AH.15.243;
7.AH.15.247; 7.AH.16.157; 7.AH.16.158; 7.AH.16.196; 7.AH.16.223;
7.AH.16.240; 7.AH.16.244; 7.AH.16.243; 7.AH.16.247; 7.AH.18.157;
7.AH.18.158; 7.AH.18.196; 7.AH.18.223; 7.AH.18.240; 7.AH.18.244;
7.AH.18.243; 7.AH.18.247; 7.AH.26.157; 7.AH.26.158; 7.AH.26.196;
7.AH.26.223; 7.AH.26.240; 7.AH.26.244; 7.AH.26.243; 7.AH.26.247;
7.AH.27.157; 7.AH.27.158; 7.AH.27.196; 7.AH.27.223; 7.AH.27.240;
7.AH.27.244; 7.AH.27.243; 7.AH.27.247; 7.AH.29.157; 7.AH.29.158;
7.AH.29.196; 7.AH.29.223; 7.AH.29.240; 7.AH.29.244; 7.AH.29.243;
7.AH.29.247; 7.AH.54.157; 7.AH.54.158; 7.AH.54.196; 7.AH.54.223;
7.AH.54.240; 7.AH.54.244; 7.AH.54.243; 7.AH.54.247; 7.AH.55.157;
7.AH.55.158; 7.AH.55.196; 7.AH.55.223; 7.AH.55.240; 7.AH.55.244;
7.AH.55.243; 7.AH.55.247; 7.AH.56.157; 7.AH.56.158; 7.AH.56.196;
7.AH.56.223; 7.AH.56.240; 7.AH.56.244; 7.AH.56.243; 7.AH.56.247;
7.AH.157.157; 7.AH.157.158; 7.AH.157.196; 7.AH.157.223;
7.AH.157.240; 7.AH.157.244; 7.AH.157.243; 7.AH.157.247;
7.AH.196.157; 7.AH.196.158; 7.AH.196.196; 7.AH.196.223;
7.AH.196.240; 7.AH.196.244; 7.AH.196.243; 7.AH.196.247;
7.AH.223.157; 7.AH.223.158; 7.AH.223.196; 7.AH.223.223;
7.AH.223.240; 7.AH.223.244; 7.AH.223.243; 7.AH.223.247;
7.AH.240.157; 7.AH.240.158; 7.AH.240.196; 7.AH.240.223;
7.AH.240.240; 7.AH.240.244; 7.AH.240.243; 7.AH.240.247;
7.AH.244.157; 7.AH.244.158; 7.AH.244.196; 7.AH.244.223;
7.AH.244.240; 7.AH.244.244; 7.AH.244.243; 7.AH.244.247;
7.AH.247.157; 7.AH.247.158; 7.AH.247.196; 7.AH.247.223;
7.AH.247.240; 7.AH.247.244; 7.AH.247.243; 7.AH.247.247; Prodrugs of
7.AJ 7.AJ.4.157; 7.AJ.4.158; 7.AJ.4.196; 7.AJ.4.223; 7.AJ.4.240;
7.AJ.4.244; 7.AJ.4.243; 7.AJ.4.247; 7.AJ.5.157; 7.AJ.5.158;
7.AJ.5.196; 7.AJ.5.223; 7.AJ.5.240; 7.AJ.5.244; 7.AJ.5.243;
7.AJ.5.247; 7.AJ.7.157; 7.AJ.7.158; 7.AJ.7.196; 7.AJ.7.223;
7.AJ.7.240; 7.AJ.7.244; 7.AJ.7.243; 7.AJ.7.247; 7.AJ.15.157;
7.AJ.15.158; 7.AJ.15.196; 7.AJ.15.223; 7.AJ.15.240; 7.AJ.15.244;
7.AJ.15.243; 7.AJ.15.247; 7.AJ.16.157; 7.AJ.16.158; 7.AJ.16.196;
7.AJ.16.223; 7.AJ.16.240; 7.AJ.16.244; 7.AJ.16.243; 7.AJ.16.247;
7.AJ.18.157; 7.AJ.18.158; 7.AJ.18.196; 7.AJ.18.223; 7.AJ.18.240;
7.AJ.18.244; 7.AJ.18.243; 7.AJ.18.247; 7.AJ.26.157; 7.AJ.26.158;
7.AJ.26.196; 7.AJ.26.223; 7.AJ.26.240; 7.AJ.26.244; 7.AJ.26.243;
7.AJ.26.247; 7.AJ.27.157; 7.AJ.27.158; 7.AJ.27.196; 7.AJ.27.223;
7.AJ.27.240; 7.AJ.27.244; 7.AJ.27.243; 7.AJ.27.247; 7.AJ.29.157;
7.AJ.29.158; 7.AJ.29.196; 7.AJ.29.223; 7.AJ.29.240; 7.AJ.29.244;
7.AJ.29.243; 7.AJ.29.247; 7.AJ.54.157; 7.AJ.54.158; 7.AJ.54.196;
7.AJ.54.223; 7.AJ.54.240; 7.AJ.54.244; 7.AJ.54.243; 7.AJ.54.247;
7.AJ.55.157; 7.AJ.55.158; 7.AJ.55.196; 7.AJ.55.223; 7.AJ.55.240;
7.AJ.55.244; 7.AJ.55.243; 7.AJ.55.247; 7.AJ.56.157; 7.AJ.56.158;
7.AJ.56.196; 7.AJ.56.223; 7.AJ.56.240; 7.AJ.56.244; 7.AJ.56.243;
7.AJ.56.247; 7.AJ.157.157; 7.AJ.157.158; 7.AJ.157.196;
7.AJ.157.223; 7.AJ.157.240; 7.AJ.157.244; 7.AJ.157.243;
7.AJ.157.247; 7.AJ.196.157; 7.AJ.196.158; 7.AJ.196.196;
7.AJ.196.223; 7.AJ.196.240; 7.AJ.196.244; 7.AJ.196.243;
7.AJ.196.247; 7.AJ.223.157; 7.AJ.223.158; 7.AJ.223.196;
7.AJ.223.223; 7.AJ.223.240; 7.AJ.223.244; 7.AJ.223.243;
7.AJ.223.247; 7.AJ.240.157; 7.AJ.240.158; 7.AJ.240.196;
7.AJ.240.223; 7.AJ.240.240; 7.AJ.240.244; 7.AJ.240.243;
7.AJ.240.247; 7.AJ.244.157; 7.AJ.244.158; 7.AJ.244.196;
7.AJ.244.223; 7.AJ.244.240; 7.AJ.244.244; 7.AJ.244.243;
7.AJ.244.247; 7.AJ.247.157; 7.AJ.247.158; 7.AJ.247.196;
7.AJ.247.223; 7.AJ.247.240; 7.AJ.247.244; 7.AJ.247.243;
7.AJ.247.247; Prodrugs of 7.AN 7.AN.4.157; 7.AN.4.158; 7.AN.4.196;
7.AN.4.223; 7.AN.4.240; 7.AN.4.244; 7.AN.4.243; 7.AN.4.247;
7.AN.5.157; 7.AN.5.158; 7.AN.5.196; 7.AN.5.223; 7.AN.5.240;
7.AN.5.244; 7.AN.5.243; 7.AN.5.247; 7.AN.7.157; 7.AN.7.158;
7.AN.7.196; 7.AN.7.223; 7.AN.7.240; 7.AN.7.244; 7.AN.7.243;
7.AN.7.247; 7.AN.15.157; 7.AN.15.158; 7.AN.15.196; 7.AN.15.223;
7.AN.15.240; 7.AN.15.244; 7.AN.15.243; 7.AN.15.247; 7.AN.16.157;
7.AN.16.158; 7.AN.16.196; 7.AN.16.223; 7.AN.16.240; 7.AN.16.244;
7.AN.16.243; 7.AN.16.247; 7.AN.18.157; 7.AN.18.158; 7.AN.18.196;
7.AN.18.223; 7.AN.18.240; 7.AN.18.244; 7.AN.18.243; 7.AN.18.247;
7.AN.26.157; 7.AN.26.158; 7.AN.26.196; 7.AN.26.223; 7.AN.26.240;
7.AN.26.244; 7.AN.26.243; 7.AN.26.247; 7.AN.27.157; 7.AN.27.158;
7.AN.27.196; 7.AN.27.223; 7.AN.27.240; 7.AN.27.244; 7.AN.27.243;
7.AN.27.247; 7.AN.29.157; 7.AN.29.158; 7.AN.29.196; 7.AN.29.223;
7.AN.29.240; 7.AN.29.244; 7.AN.29.243; 7.AN.29.247; 7.AN.54.157;
7.AN.54.158; 7.AN.54.196; 7.AN.54.223; 7.AN.54.240; 7.AN.54.244;
7.AN.54.243; 7.AN.54.247; 7.AN.55.157; 7.AN.55.158; 7.AN.55.196;
7.AN.55.223; 7.AN.55.240; 7.AN.55.244; 7.AN.55.243; 7.AN.55.247;
7.AN.56.157; 7.AN.56.158; 7.AN.56.196; 7.AN.56.223; 7.AN.56.240;
7.AN.56.244; 7.AN.56.243; 7.AN.56.247; 7.AN.157.157; 7.AN.157.158;
7.AN.157.196; 7.AN.157.223; 7.AN.157.240; 7.AN.157.244;
7.AN.157.243; 7.AN.157.247; 7.AN.196.157; 7.AN.196.158;
7.AN.196.196; 7.AN.196.223; 7.AN.196.240; 7.AN.196.244;
7.AN.196.243; 7.AN.196.247; 7.AN.223.157; 7.AN.223.158;
7.AN.223.196; 7.AN.223.223; 7.AN.223.240; 7.AN.223.244;
7.AN.223.243; 7.AN.223.247; 7.AN.240.157; 7.AN.240.158;
7.AN.240.196; 7.AN.240.223; 7.AN.240.240; 7.AN.240.244;
7.AN.240.243; 7.AN.240.247; 7.AN.244.157; 7.AN.244.158;
7.AN.244.196; 7.AN.244.223; 7.AN.244.240; 7.AN.244.244;
7.AN.244.243; 7.AN.244.247; 7.AN.247.157; 7.AN.247.158;
7.AN.247.196; 7.AN.247.223; 7.AN.247.240; 7.AN.247.244;
7.AN.247.243; 7.AN.247.247; Prodrugs of 7.AP 7.AP.4.157;
7.AP.4.158; 7.AP.4.196; 7.AP.4.223; 7.AP.4.240; 7.AP.4.244;
7.AP.4.243; 7.AP.4.247; 7.AP.5.157; 7.AP.5.158; 7.AP.5.196;
7.AP.5.223; 7.AP.5.240; 7.AP.5.244; 7.AP.5.243; 7.AP.5.247;
7.AP.7.157; 7.AP.7.158; 7.AP.7.196; 7.AP.7.223; 7.AP.7.240;
7.AP.7.244; 7.AP.7.243; 7.AP.7.247; 7.AP.15.157; 7.AP.15.158;
7.AP.15.196; 7.AP.15.223; 7.AP.15.240; 7.AP.15.244; 7.AP.15.243;
7.AP.15.247; 7.AP.16.157; 7.AP.16.158; 7.AP.16.196; 7.AP.16.223;
7.AP.16.240; 7.AP.16.244; 7.AP.16.243; 7.AP.16.247; 7.AP.18.157;
7.AP.18.158; 7.AP.18.196; 7.AP.18.223; 7.AP.18.240; 7.AP.18.244;
7.AP.18.243; 7.AP.18.247; 7.AP.26.157; 7.AP.26.158; 7.AP.26.196;
7.AP.26.223; 7.AP.26.240; 7.AP.26.244; 7.AP.26.243; 7.AP.26.247;
7.AP.27.157; 7.AP.27.158; 7.AP.27.196; 7.AP.27.223; 7.AP.27.240;
7.AP.27.244; 7.AP.27.243; 7.AP.27.247; 7.AP.29.157; 7.AP.29.158;
7.AP.29.196; 7.AP.29.223; 7.AP.29.240; 7.AP.29.244; 7.AP.29.243;
7.AP.29.247; 7.AP.54.157; 7.AP.54.158; 7.AP.54.196; 7.AP.54.223;
7.AP.54.240; 7.AP.54.244; 7.AP.54.243; 7.AP.54.247; 7.AP.55.157;
7.AP.55.158; 7.AP.55.196; 7.AP.55.223; 7.AP.55.240; 7.AP.55.244;
7.AP.55.243; 7.AP.55.247; 7.AP.56.157; 7.AP.56.158; 7.AP.56.196;
7.AP.56.223; 7.AP.56.240; 7.AP.56.244; 7.AP.56.243; 7.AP.56.247;
7.AP.157.157; 7.AP.157.158; 7.AP.157.196; 7.AP.157.223;
7.AP.157.240; 7.AP.157.244; 7.AP.157.243; 7.AP.157.247;
7.AP.196.157; 7.AP.196.158; 7.AP.196.196; 7.AP.196.223;
7.AP.196.240; 7.AP.196.244; 7.AP.196.243; 7.AP.196.247;
7.AP.223.157; 7.AP.223.158; 7.AP.223.196; 7.AP.223.223;
7.AP.223.240; 7.AP.223.244; 7.AP.223.243; 7.AP.223.247;
7.AP.240.157; 7.AP.240.158; 7.AP.240.196; 7.AP.240.223;
7.AP.240.240; 7.AP.240.244; 7.AP.240.243; 7.AP.240.247;
7.AP.244.157; 7.AP.244.158; 7.AP.244.196; 7.AP.244.223;
7.AP.244.240; 7.AP.244.244; 7.AP.244.243; 7.AP.244.247;
7.AP.247.157; 7.AP.247.158; 7.AP.247.196; 7.AP.247.223;
7.AP.247.240; 7.AP.247.244; 7.AP.247.243; 7.AP.247.247; Prodrugs of
7.AZ 7.AZ.4.157; 7.AZ.4.158; 7.AZ.4.196; 7.AZ.4.223; 7.AZ.4.240;
7.AZ.4.244; 7.AZ.4.243; 7.AZ.4.247; 7.AZ.5.157; 7.AZ.5.158;
7.AZ.5.196; 7.AZ.5.223; 7.AZ.5.240; 7.AZ.5.244; 7.AZ.5.243;
7.AZ.5.247; 7.AZ.7.157; 7.AZ.7.158; 7.AZ.7.196; 7.AZ.7.223;
7.AZ.7.240; 7.AZ.7.244; 7.AZ.7.243; 7.AZ.7.247; 7.AZ.15.157;
7.AZ.15.158; 7.AZ.15.196; 7.AZ.15.223; 7.AZ.15.240; 7.AZ.15.244;
7.AZ.15.243; 7.AZ.15.247; 7.AZ.16.157; 7.AZ.16.158; 7.AZ.16.196;
7.AZ.16.223; 7.AZ.16.240; 7.AZ.16.244; 7.AZ.16.243; 7.AZ.16.247;
7.AZ.18.157; 7.AZ.18.158; 7.AZ.18.196; 7.AZ.18.223; 7.AZ.18.240;
7.AZ.18.244; 7.AZ.18.243; 7.AZ.18.247; 7.AZ.26.157; 7.AZ.26.158;
7.AZ.26.196; 7.AZ.26.223; 7.AZ.26.240; 7.AZ.26.244; 7.AZ.26.243;
7.AZ.26.247; 7.AZ.27.157; 7.AZ.27.158; 7.AZ.27.196; 7.AZ.27.223;
7.AZ.27.240; 7.AZ.27.244; 7.AZ.27.243; 7.AZ.27.247; 7.AZ.29.157;
7.AZ.29.158; 7.AZ.29.196; 7.AZ.29.223; 7.AZ.29.240; 7.AZ.29.244;
7.AZ.29.243; 7.AZ.29.247; 7.AZ.54.157; 7.AZ.54.158; 7.AZ.54.196;
7.AZ.54.223; 7.AZ.54.240; 7.AZ.54.244; 7.AZ.54.243; 7.AZ.54.247;
7.AZ.55.157; 7.AZ.55.158; 7.AZ.55.196; 7.AZ.55.223; 7.AZ.55.240;
7.AZ.55.244; 7.AZ.55.243; 7.AZ.55.247; 7.AZ.56.157; 7.AZ.56.158;
7.AZ.56.196; 7.AZ.56.223; 7.AZ.56.240; 7.AZ.56.244; 7.AZ.56.243;
7.AZ.56.247; 7.AZ.157.157; 7.AZ.157.158; 7.AZ.157.196;
7.AZ.157.223; 7.AZ.157.240; 7.AZ.157.244; 7.AZ.157.243;
7.AZ.157.247; 7.AZ.196.157; 7.AZ.196.158; 7.AZ.196.196;
7.AZ.196.223; 7.AZ.196.240; 7.AZ.196.244; 7.AZ.196.243;
7.AZ.196.247; 7.AZ.223.157; 7.AZ.223.158; 7.AZ.223.196;
7.AZ.223.223; 7.AZ.223.240; 7.AZ.223.244; 7.AZ.223.243;
7.AZ.223.247; 7.AZ.240.157; 7.AZ.240.158; 7.AZ.240.196;
7.AZ.240.223; 7.AZ.240.240; 7.AZ.240.244; 7.AZ.240.243;
7.AZ.240.247; 7.AZ.244.157; 7.AZ.244.158; 7.AZ.244.196;
7.AZ.244.223; 7.AZ.244.240; 7.AZ.244.244; 7.AZ.244.243;
7.AZ.244.247; 7.AZ.247.157; 7.AZ.247.158; 7.AZ.247.196;
7.AZ.247.223; 7.AZ.247.240; 7.AZ.247.244; 7.AZ.247.243;
7.AZ.247.247; Prodrugs of 7.BF 7.BF.4.157; 7.BF.4.158; 7.BF.4.196;
7.BF.4.223; 7.BF.4.240; 7.BF.4.244; 7.BF.4.243; 7.BF.4.247;
7.BF.5.157; 7.BF.5.158; 7.BF.5.196; 7.BF.5.223; 7.BF.5.240;
7.BF.5.244; 7.BF.5.243; 7.BF.5.247; 7.BF.7.157; 7.BF.7.158;
7.BF.7.196; 7.BF.7.223; 7.BF.7.240; 7.BF.7.244; 7.BF.7.243;
7.BF.7.247; 7.BF.15.157; 7.BF.15.158; 7.BF.15.196; 7.BF.15.223;
7.BF.15.240; 7.BF.15.244; 7.BF.15.243; 7.BF.15.247; 7.BF.16.157;
7.BF.16.158; 7.BF.16.196; 7.BF.16.223; 7.BF.16.240; 7.BF.16.244;
7.BF.16.243; 7.BF.16.247; 7.BF.18.157; 7.BF.18.158; 7.BF.18.196;
7.BF.18.223; 7.BF.18.240; 7.BF.18.244; 7.BF.18.243; 7.BF.18.247;
7.BF.26.157; 7.BF.26.158; 7.BF.26.196; 7.BF.26.223; 7.BF.26.240;
7.BF.26.244; 7.BF.26.243; 7.BF.26.247; 7.BF.27.157; 7.BF.27.158;
7.BF.27.196; 7.BF.27.223;
7.BF.27.240; 7.BF.27.244; 7.BF.27.243; 7.BF.27.247; 7.BF.29.157;
7.BF.29.158; 7.BF.29.196; 7.BF.29.223; 7.BF.29.240; 7.BF.29.244;
7.BF.29.243; 7.BF.29.247; 7.BF.54.157; 7.BF.54.158; 7.BF.54.196;
7.BF.54.223; 7.BF.54.240; 7.BF.54.244; 7.BF.54.243; 7.BF.54.247;
7.BF.55.157; 7.BF.55.158; 7.BF.55.196; 7.BF.55.223; 7.BF.55.240;
7.BF.55.244; 7.BF.55.243; 7.BF.55.247; 7.BF.56.157; 7.BF.56.158;
7.BF.56.196; 7.BF.56.223; 7.BF.56.240; 7.BF.56.244; 7.BF.56.243;
7.BF.56.247; 7.BF.157.157; 7.BF.157.158; 7.BF.157.196;
7.BF.157.223; 7.BF.157.240; 7.BF.157.244; 7.BF.157.243;
7.BF.157.247; 7.BF.196.157; 7.BF.196.158; 7.BF.196.196;
7.BF.196.223; 7.BF.196.240; 7.BF.196.244; 7.BF.196.243;
7.BF.196.247; 7.BF.223.157; 7.BF.223.158; 7.BF.223.196;
7.BF.223.223; 7.BF.223.240; 7.BF.223.244; 7.BF.223.243;
7.BF.223.247; 7.BF.240.157; 7.BF.240.158; 7.BF.240.196;
7.BF.240.223; 7.BF.240.240; 7.BF.240.244; 7.BF.240.243;
7.BF.240.247; 7.BF.244.157; 7.BF.244.158; 7.BF.244.196;
7.BF.244.223; 7.BF.244.240; 7.BF.244.244; 7.BF.244.243;
7.BF.244.247; 7.BF.247.157; 7.BF.247.158; 7.BF.247.196;
7.BF.247.223; 7.BF.247.240; 7.BF.247.244; 7.BF.247.243;
7.BF.247.247; Prodrugs of 7.CI 7.CI.4.157; 7.CI.4.158; 7.CI.4.196;
7.CI.4.223; 7.CI.4.240; 7.CI.4.244; 7.CI.4.243; 7.CI.4.247;
7.CI.5.157; 7.CI.5.158; 7.CI.5.196; 7.CI.5.223; 7.CI.5.240;
7.CI.5.244; 7.CI.5.243; 7.CI.5.247; 7.CI.7.157; 7.CI.7.158;
7.CI.7.196; 7.CI.7.223; 7.CI.7.240; 7.CI.7.244; 7.CI.7.243;
7.CI.7.247; 7.CI.15.157; 7.CI.15.158; 7.CI.15.196; 7.CI.15.223;
7.CI.15.240; 7.CI.15.244; 7.CI.15.243; 7.CI.15.247; 7.CI.16.157;
7.CI.16.158; 7.CI.16.196; 7.CI.16.223; 7.CI.16.240; 7.CI.16.244;
7.CI.16.243; 7.CI.16.247; 7.CI.18.157; 7.CI.18.158; 7.CI.18.196;
7.CI.18.223; 7.CI.18.240; 7.CI.18.244; 7.CI.18.243; 7.CI.18.247;
7.CI.26.157; 7.CI.26.158; 7.CI.26.196; 7.CI.26.223; 7.CI.26.240;
7.CI.26.244; 7.CI.26.243; 7.CI.26.247; 7.CI.27.157; 7.CI.27.158;
7.CI.27.196; 7.CI.27.223; 7.CI.27.240; 7.CI.27.244; 7.CI.27.243;
7.CI.27.247; 7.CI.29.157; 7.CI.29.158; 7.CI.29.196; 7.CI.29.223;
7.CI.29.240; 7.CI.29.244; 7.CI.29.243; 7.CI.29.247; 7.CI.54.157;
7.CI.54.158; 7.CI.54.196; 7.CI.54.223; 7.CI.54.240; 7.CI.54.244;
7.CI.54.243; 7.CI.54.247; 7.CI.55.157; 7.CI.55.158; 7.CI.55.196;
7.CI.55.223; 7.CI.55.240; 7.CI.55.244; 7.CI.55.243; 7.CI.55.247;
7.CI.56.157; 7.CI.56.158; 7.CI.56.196; 7.CI.56.223; 7.CI.56.240;
7.CI.56.244; 7.CI.56.243; 7.CI.56.247; 7.CI.157.157; 7.CI.157.158;
7.CI.157.196; 7.CI.157.223; 7.CI.157.240; 7.CI.157.244;
7.CI.157.243; 7.CI.157.247; 7.CI.196.157; 7.CI.196.158;
7.CI.196.196; 7.CI.196.223; 7.CI.196.240; 7.CI.196.244;
7.CI.196.243; 7.CI.196.247; 7.CI.223.157; 7.CI.223.158;
7.CI.223.196; 7.CI.223.223; 7.CI.223.240; 7.CI.223.244;
7.CI.223.243; 7.CI.223.247; 7.CI.240.157; 7.CI.240.158;
7.CI.240.196; 7.CI.240.223; 7.CI.240.240; 7.CI.240.244;
7.CI.240.243; 7.CI.240.247; 7.CI.244.157; 7.CI.244.158;
7.CI.244.196; 7.CI.244.223; 7.CI.244.240; 7.CI.244.244;
7.CI.244.243; 7.CI.244.247; 7.CI.247.157; 7.CI.247.158;
7.CI.247.196; 7.CI.247.223; 7.CI.247.240; 7.CI.247.244;
7.CI.247.243; 7.CI.247.247; Prodrugs of 7.CO 7.CO.4.157;
7.CO.4.158; 7.CO.4.196; 7.CO.4.223; 7.CO.4.240; 7.CO.4.244;
7.CO.4.243; 7.CO.4.247; 7.CO.5.157; 7.CO.5.158; 7.CO.5.196;
7.CO.5.223; 7.CO.5.240; 7.CO.5.244; 7.CO.5.243; 7.CO.5.247;
7.CO.7.157; 7.CO.7.158; 7.CO.7.196; 7.CO.7.223; 7.CO.7.240;
7.CO.7.244; 7.CO.7.243; 7.CO.7.247; 7.CO.15.157; 7.CO.15.158;
7.CO.15.196; 7.CO.15.223; 7.CO.15.240; 7.CO.15.244; 7.CO.15.243;
7.CO.15.247; 7.CO.16.157; 7.CO.16.158; 7.CO.16.196; 7.CO.16.223;
7.CO.16.240; 7.CO.16.244; 7.CO.16.243; 7.CO.16.247; 7.CO.18.157;
7.CO.18.158; 7.CO.18.196; 7.CO.18.223; 7.CO.18.240; 7.CO.18.244;
7.CO.18.243; 7.CO.18.247; 7.CO.26.157; 7.CO.26.158; 7.CO.26.196;
7.CO.26.223; 7.CO.26.240; 7.CO.26.244; 7.CO.26.243; 7.CO.26.247;
7.CO.27.157; 7.CO.27.158; 7.CO.27.196; 7.CO.27.223; 7.CO.27.240;
7.CO.27.244; 7.CO.27.243; 7.CO.27.247; 7.CO.29.157; 7.CO.29.158;
7.CO.29.196; 7.CO.29.223; 7.CO.29.240; 7.CO.29.244; 7.CO.29.243;
7.CO.29.247; 7.CO.54.157; 7.CO.54.158; 7.CO.54.196; 7.CO.54.223;
7.CO.54.240; 7.CO.54.244; 7.CO.54.243; 7.CO.54.247; 7.CO.55.157;
7.CO.55.158; 7.CO.55.196; 7.CO.55.223; 7.CO.55.240; 7.CO.55.244;
7.CO.55.243; 7.CO.55.247; 7.CO.56.157; 7.CO.56.158; 7.CO.56.196;
7.CO.56.223; 7.CO.56.240; 7.CO.56.244; 7.CO.56.243; 7.CO.56.247;
7.CO.157.157; 7.CO.157.158; 7.CO.157.196; 7.CO.157.223;
7.CO.157.240; 7.CO.157.244; 7.CO.157.243; 7.CO.157.247;
7.CO.196.157; 7.CO.196.158; 7.CO.196.196; 7.CO.196.223;
7.CO.196.240; 7.CO.196.244; 7.CO.196.243; 7.CO.196.247;
7.CO.223.157; 7.CO.223.158; 7.CO.223.196; 7.CO.223.223;
7.CO.223.240; 7.CO.223.244; 7.CO.223.243; 7.CO.223.247;
7.CO.240.157; 7.CO.240.158; 7.CO.240.196; 7.CO.240.223;
7.CO.240.240; 7.CO.240.244; 7.CO.240.243; 7.CO.240.247;
7.CO.244.157; 7.CO.244.158; 7.CO.244.196; 7.CO.244.223;
7.CO.244.240; 7.CO.244.244; 7.CO.244.243; 7.CO.244.247; 7.CO.4.157;
7.CO.4.158; 7.CO.4.196; 7.CO.4.223; 7.CO.4.240; 7.CO.4.244;
7.CO.4.243; 7.CO.4.247; Prodrugs of 8.AH 8.AH.4.157; 8.AH.4.158;
8.AH.4.196; 8.AH.4.223; 8.AH.4.240; 8.AH.4.244; 8.AH.4.243;
8.AH.4.247; 8.AH.5.157; 8.AH.5.158; 8.AH.5.196; 8.AH.5.223;
8.AH.5.240; 8.AH.5.244; 8.AH.5.243; 8.AH.5.247; 8.AH.7.157;
8.AH.7.158; 8.AH.7.196; 8.AH.7.223; 8.AH.7.240; 8.AH.7.244;
8.AH.7.243; 8.AH.7.247; 8.AH.15.157; 8.AH.15.158; 8.AH.15.196;
8.AH.15.223; 8.AH.15.240; 8.AH.15.244; 8.AH.15.243; 8.AH.15.247;
8.AH.16.157; 8.AH.16.158; 8.AH.16.196; 8.AH.16.223; 8.AH.16.240;
8.AH.16.244; 8.AH.16.243; 8.AH.16.247; 8.AH.18.157; 8.AH.18.158;
8.AH.18.196; 8.AH.18.223; 8.AH.18.240; 8.AH.18.244; 8.AH.18.243;
8.AH.18.247; 8.AH.26.157; 8.AH.26.158; 8.AH.26.196; 8.AH.26.223;
8.AH.26.240; 8.AH.26.244; 8.AH.26.243; 8.AH.26.247; 8.AH.27.157;
8.AH.27.158; 8.AH.27.196; 8.AH.27.223; 8.AH.27.240; 8.AH.27.244;
8.AH.27.243; 8.AH.27.247; 8.AH.29.157; 8.AH.29.158; 8.AH.29.196;
8.AH.29.223; 8.AH.29.240; 8.AH.29.244; 8.AH.29.243; 8.AH.29.247;
8.AH.54.157; 8.AH.54.158; 8.AH.54.196; 8.AH.54.223; 8.AH.54.240;
8.AH.54.244; 8.AH.54.243; 8.AH.54.247; 8.AH.55.157; 8.AH.55.158;
8.AH.55.196; 8.AH.55.223; 8.AH.55.240; 8.AH.55.244; 8.AH.55.243;
8.AH.55.247; 8.AH.56.157; 8.AH.56.158; 8.AH.56.196; 8.AH.56.223;
8.AH.56.240; 8.AH.56.244; 8.AH.56.243; 8.AH.56.247; 8.AH.157.157;
8.AH.157.158; 8.AH.157.196; 8.AH.157.223; 8.AH.157.240;
8.AH.157.244; 8.AH.157.243; 8.AH.157.247; 8.AH.196.157;
8.AH.196.158; 8.AH.196.196; 8.AH.196.223; 8.AH.196.240;
8.AH.196.244; 8.AH.196.243; 8.AH.196.247; 8.AH.223.157;
8.AH.223.158; 8.AH.223.196; 8.AH.223.223; 8.AH.223.240;
8.AH.223.244; 8.AH.223.243; 8.AH.223.247; 8.AH.240.157;
8.AH.240.158; 8.AH.240.196; 8.AH.240.223; 8.AH.240.240;
8.AH.240.244; 8.AH.240.243; 8.AH.240.247; 8.AH.244.157;
8.AH.244.158; 8.AH.244.196; 8.AH.244.223; 8.AH.244.240;
8.AH.244.244; 8.AH.244.243; 8.AH.244.247; 8.AH.247.157;
8.AH.247.158; 8.AH.247.196; 8.AH.247.223; 8.AH.247.240;
8.AH.247.244; 8.AH.247.243; 8.AH.247.247; Prodrugs of 8.AJ
8.AJ.4.157; 8.AJ.4.158; 8.AJ.4.196; 8.AJ.4.223; 8.AJ.4.240;
8.AJ.4.244; 8.AJ.4.243; 8.AJ.4.247; 8.AJ.5.157; 8.AJ.5.158;
8.AJ.5.196; 8.AJ.5.223; 8.AJ.5.240; 8.AJ.5.244; 8.AJ.5.243;
8.AJ.5.247; 8.AJ.7.157; 8.AJ.7.158; 8.AJ.7.196; 8.AJ.7.223;
8.AJ.7.240; 8.AJ.7.244; 8.AJ.7.243; 8.AJ.7.247; 8.AJ.15.157;
8.AJ.15.158; 8.AJ.15.196; 8.AJ.15.223; 8.AJ.15.240; 8.AJ.15.244;
8.AJ.15.243; 8.AJ.15.247; 8.AJ.16.157; 8.AJ.16.158; 8.AJ.16.196;
8.AJ.16.223; 8.AJ.16.240; 8.AJ.16.244; 8.AJ.16.243; 8.AJ.16.247;
8.AJ.18.157; 8.AJ.18.158; 8.AJ.18.196; 8.AJ.18.223; 8.AJ.18.240;
8.AJ.18.244; 8.AJ.18.243; 8.AJ.18.247; 8.AJ.26.157; 8.AJ.26.158;
8.AJ.26.196; 8.AJ.26.223; 8.AJ.26.240; 8.AJ.26.244; 8.AJ.26.243;
8.AJ.26.247; 8.AJ.27.157; 8.AJ.27.158; 8.AJ.27.196; 8.AJ.27.223;
8.AJ.27.240; 8.AJ.27.244; 8.AJ.27.243; 8.AJ.27.247; 8.AJ.29.157;
8.AJ.29.158; 8.AJ.29.196; 8.AJ.29.223; 8.AJ.29.240; 8.AJ.29.244;
8.AJ.29.243; 8.AJ.29.247; 8.AJ.54.157; 8.AJ.54.158; 8.AJ.54.196;
8.AJ.54.223; 8.AJ.54.240; 8.AJ.54.244; 8.AJ.54.243; 8.AJ.54.247;
8.AJ.55.157; 8.AJ.55.158; 8.AJ.55.196; 8.AJ.55.223; 8.AJ.55.240;
8.AJ.55.244; 8.AJ.55.243; 8.AJ.55.247; 8.AJ.56.157; 8.AJ.56.158;
8.AJ.56.196; 8.AJ.56.223; 8.AJ.56.240; 8.AJ.56.244; 8.AJ.56.243;
8.AJ.56.247; 8.AJ.157.157; 8.AJ.157.158; 8.AJ.157.196;
8.AJ.157.223; 8.AJ.157.240; 8.AJ.157.244; 8.AJ.157.243;
8.AJ.157.247; 8.AJ.196.157; 8.AJ.196.158; 8.AJ.196.196;
8.AJ.196.223; 8.AJ.196.240; 8.AJ.196.244; 8.AJ.196.243;
8.AJ.196.247; 8.AJ.223.157; 8.AJ.223.158; 8.AJ.223.196;
8.AJ.223.223; 8.AJ.223.240; 8.AJ.223.244; 8.AJ.223.243;
8.AJ.223.247; 8.AJ.240.157; 8.AJ.240.158; 8.AJ.240.196;
8.AJ.240.223; 8.AJ.240.240; 8.AJ.240.244; 8.AJ.240.243;
8.AJ.240.247; 8.AJ.244.157; 8.AJ.244.158; 8.AJ.244.196;
8.AJ.244.223; 8.AJ.244.240; 8.AJ.244.244; 8.AJ.244.243;
8.AJ.244.247; 8.AJ.247.157; 8.AJ.247.158; 8.AJ.247.196;
8.AJ.247.223; 8.AJ.247.240; 8.AJ.247.244; 8.AJ.247.243;
8.AJ.247.247; Prodrugs of 8.AN 8.AN.4.157; 8.AN.4.158; 8.AN.4.196;
8.AN.4.223; 8.AN.4.240; 8.AN.4.244; 8.AN.4.243; 8.AN.4.247;
8.AN.5.157; 8.AN.5.158; 8.AN.5.196; 8.AN.5.223; 8.AN.5.240;
8.AN.5.244; 8.AN.5.243; 8.AN.5.247; 8.AN.7.157; 8.AN.7.158;
8.AN.7.196; 8.AN.7.223; 8.AN.7.240; 8.AN.7.244; 8.AN.7.243;
8.AN.7.247; 8.AN.15.157; 8.AN.15.158; 8.AN.15.196; 8.AN.15.223;
8.AN.15.240; 8.AN.15.244; 8.AN.15.243; 8.AN.15.247; 8.AN.16.157;
8.AN.16.158; 8.AN.16.196; 8.AN.16.223; 8.AN.16.240; 8.AN.16.244;
8.AN.16.243; 8.AN.16.247; 8.AN.18.157; 8.AN.18.158; 8.AN.18.196;
8.AN.18.223; 8.AN.18.240; 8.AN.18.244; 8.AN.18.243; 8.AN.18.247;
8.AN.26.157; 8.AN.26.158; 8.AN.26.196; 8.AN.26.223; 8.AN.26.240;
8.AN.26.244; 8.AN.26.243; 8.AN.26.247; 8.AN.27.157; 8.AN.27.158;
8.AN.27.196; 8.AN.27.223; 8.AN.27.240; 8.AN.27.244; 8.AN.27.243;
8.AN.27.247; 8.AN.29.157; 8.AN.29.158; 8.AN.29.196; 8.AN.29.223;
8.AN.29.240; 8.AN.29.244; 8.AN.29.243; 8.AN.29.247; 8.AN.54.157;
8.AN.54.158; 8.AN.54.196; 8.AN.54.223; 8.AN.54.240; 8.AN.54.244;
8.AN.54.243; 8.AN.54.247; 8.AN.55.157; 8.AN.55.158; 8.AN.55.196;
8.AN.55.223; 8.AN.55.240; 8.AN.55.244; 8.AN.55.243; 8.AN.55.247;
8.AN.56.157; 8.AN.56.158; 8.AN.56.196; 8.AN.56.223; 8.AN.56.240;
8.AN.56.244; 8.AN.56.243; 8.AN.56.247; 8.AN.157.157; 8.AN.157.158;
8.AN.157.196; 8.AN.157.223; 8.AN.157.240; 8.AN.157.244;
8.AN.157.243; 8.AN.157.247; 8.AN.196.157; 8.AN.196.158;
8.AN.196.196; 8.AN.196.223; 8.AN.196.240; 8.AN.196.244;
8.AN.196.243; 8.AN.196.247; 8.AN.223.157; 8.AN.223.158;
8.AN.223.196; 8.AN.223.223; 8.AN.223.240; 8.AN.223.244;
8.AN.223.243; 8.AN.223.247; 8.AN.240.157; 8.AN.240.158;
8.AN.240.196; 8.AN.240.223; 8.AN.240.240; 8.AN.240.244;
8.AN.240.243; 8.AN.240.247; 8.AN.244.157; 8.AN.244.158;
8.AN.244.196; 8.AN.244.223; 8.AN.244.240; 8.AN.244.244;
8.AN.244.243; 8.AN.244.247; 8.AN.247.157; 8.AN.247.158;
8.AN.247.196; 8.AN.247.223; 8.AN.247.240; 8.AN.247.244;
8.AN.247.243; 8.AN.247.247; Prodrugs of 8.AP 8.AP.4.157;
8.AP.4.158; 8.AP.4.196; 8.AP.4.223; 8.AP.4.240; 8.AP.4.244;
8.AP.4.243; 8.AP.4.247; 8.AP.5.157; 8.AP.5.158; 8.AP.5.196;
8.AP.5.223; 8.AP.5.240; 8.AP.5.244; 8.AP.5.243; 8.AP.5.247;
8.AP.7.157; 8.AP.7.158; 8.AP.7.196; 8.AP.7.223; 8.AP.7.240;
8.AP.7.244; 8.AP.7.243; 8.AP.7.247; 8.AP.15.157; 8.AP.15.158;
8.AP.15.196; 8.AP.15.223; 8.AP.15.240; 8.AP.15.244; 8.AP.15.243;
8.AP.15.247; 8.AP.16.157; 8.AP.16.158; 8.AP.16.196; 8.AP.16.223;
8.AP.16.240; 8.AP.16.244; 8.AP.16.243; 8.AP.16.247; 8.AP.18.157;
8.AP.18.158; 8.AP.18.196; 8.AP.18.223; 8.AP.18.240; 8.AP.18.244;
8.AP.18.243; 8.AP.18.247; 8.AP.26.157; 8.AP.26.158; 8.AP.26.196;
8.AP.26.223; 8.AP.26.240; 8.AP.26.244; 8.AP.26.243; 8.AP.26.247;
8.AP.27.157; 8.AP.27.158; 8.AP.27.196; 8.AP.27.223; 8.AP.27.240;
8.AP.27.244; 8.AP.27.243; 8.AP.27.247; 8.AP.29.157; 8.AP.29.158;
8.AP.29.196; 8.AP.29.223; 8.AP.29.240; 8.AP.29.244; 8.AP.29.243;
8.AP.29.247; 8.AP.54.157; 8.AP.54.158; 8.AP.54.196; 8.AP.54.223;
8.AP.54.240; 8.AP.54.244; 8.AP.54.243; 8.AP.54.247; 8.AP.55.157;
8.AP.55.158; 8.AP.55.196; 8.AP.55.223; 8.AP.55.240; 8.AP.55.244;
8.AP.55.243; 8.AP.55.247; 8.AP.56.157; 8.AP.56.158; 8.AP.56.196;
8.AP.56.223; 8.AP.56.240; 8.AP.56.244; 8.AP.56.243; 8.AP.56.247;
8.AP.157.157; 8.AP.157.158; 8.AP.157.196; 8.AP.157.223;
8.AP.157.240; 8.AP.157.244; 8.AP.157.243; 8.AP.157.247;
8.AP.196.157; 8.AP.196.158; 8.AP.196.196; 8.AP.196.223;
8.AP.196.240; 8.AP.196.244; 8.AP.196.243; 8.AP.196.247;
8.AP.223.157; 8.AP.223.158; 8.AP.223.196; 8.AP.223.223;
8.AP.223.240; 8.AP.223.244; 8.AP.223.243; 8.AP.223.247;
8.AP.240.157; 8.AP.240.158; 8.AP.240.196; 8.AP.240.223;
8.AP.240.240; 8.AP.240.244; 8.AP.240.243; 8.AP.240.247;
8.AP.244.157; 8.AP.244.158; 8.AP.244.196; 8.AP.244.223;
8.AP.244.240; 8.AP.244.244; 8.AP.244.243; 8.AP.244.247;
8.AP.247.157; 8.AP.247.158; 8.AP.247.196;
8.AP.247.223; 8.AP.247.240; 8.AP.247.244; 8.AP.247.243;
8.AP.247.247; Prodrugs of 8.AZ 8.AZ.4.157; 8.AZ.4.158; 8.AZ.4.196;
8.AZ.4.223; 8.AZ.4.240; 8.AZ.4.244; 8.AZ.4.243; 8.AZ.4.247;
8.AZ.5.157; 8.AZ.5.158; 8.AZ.5.196; 8.AZ.5.223; 8.AZ.5.240;
8.AZ.5.244; 8.AZ.5.243; 8.AZ.5.247; 8.AZ.7.157; 8.AZ.7.158;
8.AZ.7.196; 8.AZ.7.223; 8.AZ.7.240; 8.AZ.7.244; 8.AZ.7.243;
8.AZ.7.247; 8.AZ.15.157; 8.AZ.15.158; 8.AZ.15.196; 8.AZ.15.223;
8.AZ.15.240; 8.AZ.15.244; 8.AZ.15.243; 8.AZ.15.247; 8.AZ.16.157;
8.AZ.16.158; 8.AZ.16.196; 8.AZ.16.223; 8.AZ.16.240; 8.AZ.16.244;
8.AZ.16.243; 8.AZ.16.247; 8.AZ.18.157; 8.AZ.18.158; 8.AZ.18.196;
8.AZ.18.223; 8.AZ.18.240; 8.AZ.18.244; 8.AZ.18.243; 8.AZ.18.247;
8.AZ.26.157; 8.AZ.26.158; 8.AZ.26.196; 8.AZ.26.223; 8.AZ.26.240;
8.AZ.26.244; 8.AZ.26.243; 8.AZ.26.247; 8.AZ.27.157; 8.AZ.27.158;
8.AZ.27.196; 8.AZ.27.223; 8.AZ.27.240; 8.AZ.27.244; 8.AZ.27.243;
8.AZ.27.247; 8.AZ.29.157; 8.AZ.29.158; 8.AZ.29.196; 8.AZ.29.223;
8.AZ.29.240; 8.AZ.29.244; 8.AZ.29.243; 8.AZ.29.247; 8.AZ.54.157;
8.AZ.54.158; 8.AZ.54.196; 8.AZ.54.223; 8.AZ.54.240; 8.AZ.54.244;
8.AZ.54.243; 8.AZ.54.247; 8.AZ.55.157; 8.AZ.55.158; 8.AZ.55.196;
8.AZ.55.223; 8.AZ.55.240; 8.AZ.55.244; 8.AZ.55.243; 8.AZ.55.247;
8.AZ.56.157; 8.AZ.56.158; 8.AZ.56.196; 8.AZ.56.223; 8.AZ.56.240;
8.AZ.56.244; 8.AZ.56.243; 8.AZ.56.247; 8.AZ.157.157; 8.AZ.157.158;
8.AZ.157.196; 8.AZ.157.223; 8.AZ.157.240; 8.AZ.157.244;
8.AZ.157.243; 8.AZ.157.247; 8.AZ.196.157; 8.AZ.196.158;
8.AZ.196.196; 8.AZ.196.223; 8.AZ.196.240; 8.AZ.196.244;
8.AZ.196.243; 8.AZ.196.247; 8.AZ.223.157; 8.AZ.223.158;
8.AZ.223.196; 8.AZ.223.223; 8.AZ.223.240; 8.AZ.223.244;
8.AZ.223.243; 8.AZ.223.247; 8.AZ.240.157; 8.AZ.240.158;
8.AZ.240.196; 8.AZ.240.223; 8.AZ.240.240; 8.AZ.240.244;
8.AZ.240.243; 8.AZ.240.247; 8.AZ.244.157; 8.AZ.244.158;
8.AZ.244.196; 8.AZ.244.223; 8.AZ.244.240; 8.AZ.244.244;
8.AZ.244.243; 8.AZ.244.247; 8.AZ.247.157; 8.AZ.247.158;
8.AZ.247.196; 8.AZ.247.223; 8.AZ.247.240; 8.AZ.247.244;
8.AZ.247.243; 8.AZ.247.247; Prodrugs of 8.BF 8.BF.4.157;
8.BF.4.158; 8.BF.4.196; 8.BF.4.223; 8.BF.4.240; 8.BF.4.244;
8.BF.4.243; 8.BF.4.247; 8.BF.5.157; 8.BF.5.158; 8.BF.5.196;
8.BF.5.223; 8.BF.5.240; 8.BF.5.244; 8.BF.5.243; 8.BF.5.247;
8.BF.7.157; 8.BF.7.158; 8.BF.7.196; 8.BF.7.223; 8.BF.7.240;
8.BF.7.244; 8.BF.7.243; 8.BF.7.247; 8.BF.15.157; 8.BF.15.158;
8.BF.15.196; 8.BF.15.223; 8.BF.15.240; 8.BF.15.244; 8.BF.15.243;
8.BF.15.247; 8.BF.16.157; 8.BF.16.158; 8.BF.16.196; 8.BF.16.223;
8.BF.16.240; 8.BF.16.244; 8.BF.16.243; 8.BF.16.247; 8.BF.18.157;
8.BF.18.158; 8.BF.18.196; 8.BF.18.223; 8.BF.18.240; 8.BF.18.244;
8.BF.18.243; 8.BF.18.247; 8.BF.26.157; 8.BF.26.158; 8.BF.26.196;
8.BF.26.223; 8.BF.26.240; 8.BF.26.244; 8.BF.26.243; 8.BF.26.247;
8.BF.27.157; 8.BF.27.158; 8.BF.27.196; 8.BF.27.223; 8.BF.27.240;
8.BF.27.244; 8.BF.27.243; 8.BF.27.247; 8.BF.29.157; 8.BF.29.158;
8.BF.29.196; 8.BF.29.223; 8.BF.29.240; 8.BF.29.244; 8.BF.29.243;
8.BF.29.247; 8.BF.54.157; 8.BF.54.158; 8.BF.54.196; 8.BF.54.223;
8.BF.54.240; 8.BF.54.244; 8.BF.54.243; 8.BF.54.247; 8.BF.55.157;
8.BF.55.158; 8.BF.55.196; 8.BF.55.223; 8.BF.55.240; 8.BF.55.244;
8.BF.55.243; 8.BF.55.247; 8.BF.56.157; 8.BF.56.158; 8.BF.56.196;
8.BF.56.223; 8.BF.56.240; 8.BF.56.244; 8.BF.56.243; 8.BF.56.247;
8.BF.157.157; 8.BF.157.158; 8.BF.157.196; 8.BF.157.223;
8.BF.157.240; 8.BF.157.244; 8.BF.157.243; 8.BF.157.247;
8.BF.196.157; 8.BF.196.158; 8.BF.196.196; 8.BF.196.223;
8.BF.196.240; 8.BF.196.244; 8.BF.196.243; 8.BF.196.247;
8.BF.223.157; 8.BF.223.158; 8.BF.223.196; 8.BF.223.223;
8.BF.223.240; 8.BF.223.244; 8.BF.223.243; 8.BF.223.247;
8.BF.240.157; 8.BF.240.158; 8.BF.240.196; 8.BF.240.223;
8.BF.240.240; 8.BF.240.244; 8.BF.240.243; 8.BF.240.247;
8.BF.244.157; 8.BF.244.158; 8.BF.244.196; 8.BF.244.223;
8.BF.244.240; 8.BF.244.244; 8.BF.244.243; 8.BF.244.247;
8.BF.247.157; 8.BF.247.158; 8.BF.247.196; 8.BF.247.223;
8.BF.247.240; 8.BF.247.244; 8.BF.247.243; 8.BF.247.247; Prodrugs of
8.CI 8.CI.4.157; 8.CI.4.158; 8.CI.4.196; 8.CI.4.223; 8.CI.4.240;
8.CI.4.244; 8.CI.4.243; 8.CI.4.247; 8.CI.5.157; 8.CI.5.158;
8.CI.5.196; 8.CI.5.223; 8.CI.5.240; 8.CI.5.244; 8.CI.5.243;
8.CI.5.247; 8.CI.7.157; 8.CI.7.158; 8.CI.7.196; 8.CI.7.223;
8.CI.7.240; 8.CI.7.244; 8.CI.7.243; 8.CI.7.247; 8.CI.15.157;
8.CI.15.158; 8.CI.15.196; 8.CI.15.223; 8.CI.15.240; 8.CI.15.244;
8.CI.15.243; 8.CI.15.247; 8.CI.16.157; 8.CI.16.158; 8.CI.16.196;
8.CI.16.223; 8.CI.16.240; 8.CI.16.244; 8.CI.16.243; 8.CI.16.247;
8.CI.18.157; 8.CI.18.158; 8.CI.18.196; 8.CI.18.223; 8.CI.18.240;
8.CI.18.244; 8.CI.18.243; 8.CI.18.247; 8.CI.26.157; 8.CI.26.158;
8.CI.26.196; 8.CI.26.223; 8.CI.26.240; 8.CI.26.244; 8.CI.26.243;
8.CI.26.247; 8.CI.27.157; 8.CI.27.158; 8.CI.27.196; 8.CI.27.223;
8.CI.27.240; 8.CI.27.244; 8.CI.27.243; 8.CI.27.247; 8.CI.29.157;
8.CI.29.158; 8.CI.29.196; 8.CI.29.223; 8.CI.29.240; 8.CI.29.244;
8.CI.29.243; 8.CI.29.247; 8.CI.54.157; 8.CI.54.158; 8.CI.54.196;
8.CI.54.223; 8.CI.54.240; 8.CI.54.244; 8.CI.54.243; 8.CI.54.247;
8.CI.55.157; 8.CI.55.158; 8.CI.55.196; 8.CI.55.223; 8.CI.55.240;
8.CI.55.244; 8.CI.55.243; 8.CI.55.247; 8.CI.56.157; 8.CI.56.158;
8.CI.56.196; 8.CI.56.223; 8.CI.56.240; 8.CI.56.244; 8.CI.56.243;
8.CI.56.247; 8.CI.157.157; 8.CI.157.158; 8.CI.157.196;
8.CI.157.223; 8.CI.157.240; 8.CI.157.244; 8.CI.157.243;
8.CI.157.247; 8.CI.196.157; 8.CI.196.158; 8.CI.196.196;
8.CI.196.223; 8.CI.196.240; 8.CI.196.244; 8.CI.196.243;
8.CI.196.247; 8.CI.223.157; 8.CI.223.158; 8.CI.223.196;
8.CI.223.223; 8.CI.223.240; 8.CI.223.244; 8.CI.223.243;
8.CI.223.247; 8.CI.240.157; 8.CI.240.158; 8.CI.240.196;
8.CI.240.223; 8.CI.240.240; 8.CI.240.244; 8.CI.240.243;
8.CI.240.247; 8.CI.244.157; 8.CI.244.158; 8.CI.244.196;
8.CI.244.223; 8.CI.244.240; 8.CI.244.244; 8.CI.244.243;
8.CI.244.247; 8.CI.247.157; 8.CI.247.158; 8.CI.247.196;
8.CI.247.223; 8.CI.247.240; 8.CI.247.244; 8.CI.247.243;
8.CI.247.247; Prodrugs of 8.CO 8.CO.4.157; 8.CO.4.158; 8.CO.4.196;
8.CO.4.223; 8.CO.4.240; 8.CO.4.244; 8.CO.4.243; 8.CO.4.247;
8.CO.5.157; 8.CO.5.158; 8.CO.5.196; 8.CO.5.223; 8.CO.5.240;
8.CO.5.244; 8.CO.5.243; 8.CO.5.247; 8.CO.7.157; 8.CO.7.158;
8.CO.7.196; 8.CO.7.223; 8.CO.7.240; 8.CO.7.244; 8.CO.7.243;
8.CO.7.247; 8.CO.15.157; 8.CO.15.158; 8.CO.15.196; 8.CO.15.223;
8.CO.15.240; 8.CO.15.244; 8.CO.15.243; 8.CO.15.247; 8.CO.16.157;
8.CO.16.158; 8.CO.16.196; 8.CO.16.223; 8.CO.16.240; 8.CO.16.244;
8.CO.16.243; 8.CO.16.247; 8.CO.18.157; 8.CO.18.158; 8.CO.18.196;
8.CO.18.223; 8.CO.18.240; 8.CO.18.244; 8.CO.18.243; 8.CO.18.247;
8.CO.26.157; 8.CO.26.158; 8.CO.26.196; 8.CO.26.223; 8.CO.26.240;
8.CO.26.244; 8.CO.26.243; 8.CO.26.247; 8.CO.27.157; 8.CO.27.158;
8.CO.27.196; 8.CO.27.223; 8.CO.27.240; 8.CO.27.244; 8.CO.27.243;
8.CO.27.247; 8.CO.29.157; 8.CO.29.158; 8.CO.29.196; 8.CO.29.223;
8.CO.29.240; 8.CO.29.244; 8.CO.29.243; 8.CO.29.247; 8.CO.54.157;
8.CO.54.158; 8.CO.54.196; 8.CO.54.223; 8.CO.54.240; 8.CO.54.244;
8.CO.54.243; 8.CO.54.247; 8.CO.55.157; 8.CO.55.158; 8.CO.55.196;
8.CO.55.223; 8.CO.55.240; 8.CO.55.244; 8.CO.55.243; 8.CO.55.247;
8.CO.56.157; 8.CO.56.158; 8.CO.56.196; 8.CO.56.223; 8.CO.56.240;
8.CO.56.244; 8.CO.56.243; 8.CO.56.247; 8.CO.157.157; 8.CO.157.158;
8.CO.157.196; 8.CO.157.223; 8.CO.157.240; 8.CO.157.244;
8.CO.157.243; 8.CO.157.247; 8.CO.196.157; 8.CO.196.158;
8.CO.196.196; 8.CO.196.223; 8.CO.196.240; 8.CO.196.244;
8.CO.196.243; 8.CO.196.247; 8.CO.223.157; 8.CO.223.158;
8.CO.223.196; 8.CO.223.223; 8.CO.223.240; 8.CO.223.244;
8.CO.223.243; 8.CO.223.247; 8.CO.240.157; 8.CO.240.158;
8.CO.240.196; 8.CO.240.223; 8.CO.240.240; 8.CO.240.244;
8.CO.240.243; 8.CO.240.247; 8.CO.244.157; 8.CO.244.158;
8.CO.244.196; 8.CO.244.223; 8.CO.244.240; 8.CO.244.244;
8.CO.244.243; 8.CO.244.247; 8.CO.247.157; 8.CO.247.158;
8.CO.247.196; 8.CO.247.223; 8.CO.247.240; 8.CO.247.244;
8.CO.247.243; 8.CO.247.247; Prodrugs of 9.AH 9.AH.4.157;
9.AH.4.158; 9.AH.4.196; 9.AH.4.223; 9.AH.4.240; 9.AH.4.244;
9.AH.4.243; 9.AH.4.247; 9.AH.5.157; 9.AH.5.158; 9.AH.5.196;
9.AH.5.223; 9.AH.5.240; 9.AH.5.244; 9.AH.5.243; 9.AH.5.247;
9.AH.7.157; 9.AH.7.158; 9.AH.7.196; 9.AH.7.223; 9.AH.7.240;
9.AH.7.244; 9.AH.7.243; 9.AH.7.247; 9.AH.15.157; 9.AH.15.158;
9.AH.15.196; 9.AH.15.223; 9.AH.15.240; 9.AH.15.244; 9.AH.15.243;
9.AH.15.247; 9.AH.16.157; 9.AH.16.158; 9.AH.16.196; 9.AH.16.223;
9.AH.16.240; 9.AH.16.244; 9.AH.16.243; 9.AH.16.247; 9.AH.18.157;
9.AH.18.158; 9.AH.18.196; 9.AH.18.223; 9.AH.18.240; 9.AH.18.244;
9.AH.18.243; 9.AH.18.247; 9.AH.26.157; 9.AH.26.158; 9.AH.26.196;
9.AH.26.223; 9.AH.26.240; 9.AH.26.244; 9.AH.26.243; 9.AH.26.247;
9.AH.27.157; 9.AH.27.158; 9.AH.27.196; 9.AH.27.223; 9.AH.27.240;
9.AH.27.244; 9.AH.27.243; 9.AH.27.247; 9.AH.29.157; 9.AH.29.158;
9.AH.29.196; 9.AH.29.223; 9.AH.29.240; 9.AH.29.244; 9.AH.29.243;
9.AH.29.247; 9.AH.54.157; 9.AH.54.158; 9.AH.54.196; 9.AH.54.223;
9.AH.54.240; 9.AH.54.244; 9.AH.54.243; 9.AH.54.247; 9.AH.55.157;
9.AH.55.158; 9.AH.55.196; 9.AH.55.223; 9.AH.55.240; 9.AH.55.244;
9.AH.55.243; 9.AH.55.247; 9.AH.56.157; 9.AH.56.158; 9.AH.56.196;
9.AH.56.223; 9.AH.56.240; 9.AH.56.244; 9.AH.56.243; 9.AH.56.247;
9.AH.157.157; 9.AH.157.158; 9.AH.157.196; 9.AH.157.223;
9.AH.157.240; 9.AH.157.244; 9.AH.157.243; 9.AH.157.247;
9.AH.196.157; 9.AH.196.158; 9.AH.196.196; 9.AH.196.223;
9.AH.196.240; 9.AH.196.244; 9.AH.196.243; 9.AH.196.247;
9.AH.223.157; 9.AH.223.158; 9.AH.223.196; 9.AH.223.223;
9.AH.223.240; 9.AH.223.244; 9.AH.223.243; 9.AH.223.247;
9.AH.240.157; 9.AH.240.158; 9.AH.240.196; 9.AH.240.223;
9.AH.240.240; 9.AH.240.244; 9.AH.240.243; 9.AH.240.247;
9.AH.244.157; 9.AH.244.158; 9.AH.244.196; 9.AH.244.223;
9.AH.244.240; 9.AH.244.244; 9.AH.244.243; 9.AH.244.247;
9.AH.247.157; 9.AH.247.158; 9.AH.247.196; 9.AH.247.223;
9.AH.247.240; 9.AH.247.244; 9.AH.247.243; 9.AH.247.247; Prodrugs of
9.AJ 9.AJ.4.157; 9.AJ.4.158; 9.AJ.4.196; 9.AJ.4.223; 9.AJ.4.240;
9.AJ.4.244; 9.AJ.4.243; 9.AJ.4.247; 9.AJ.5.157; 9.AJ.5.158;
9.AJ.5.196; 9.AJ.5.223; 9.AJ.5.240; 9.AJ.5.244; 9.AJ.5.243;
9.AJ.5.247; 9.AJ.7.157; 9.AJ.7.158; 9.AJ.7.196; 9.AJ.7.223;
9.AJ.7.240; 9.AJ.7.244; 9.AJ.7.243; 9.AJ.7.247; 9.AJ.15.157;
9.AJ.15.158; 9.AJ.15.196; 9.AJ.15.223; 9.AJ.15.240; 9.AJ.15.244;
9.AJ.15.243; 9.AJ.15.247; 9.AJ.16.157; 9.AJ.16.158; 9.AJ.16.196;
9.AJ.16.223; 9.AJ.16.240; 9.AJ.16.244; 9.AJ.16.243; 9.AJ.16.247;
9.AJ.18.157; 9.AJ.18.158; 9.AJ.18.196; 9.AJ.18.223; 9.AJ.18.240;
9.AJ.18.244; 9.AJ.18.243; 9.AJ.18.247; 9.AJ.26.157; 9.AJ.26.158;
9.AJ.26.196; 9.AJ.26.223; 9.AJ.26.240; 9.AJ.26.244; 9.AJ.26.243;
9.AJ.26.247; 9.AJ.27.157; 9.AJ.27.158; 9.AJ.27.196; 9.AJ.27.223;
9.AJ.27.240; 9.AJ.27.244; 9.AJ.27.243; 9.AJ.27.247; 9.AJ.29.157;
9.AJ.29.158; 9.AJ.29.196; 9.AJ.29.223; 9.AJ.29.240; 9.AJ.29.244;
9.AJ.29.243; 9.AJ.29.247; 9.AJ.54.157; 9.AJ.54.158; 9.AJ.54.196;
9.AJ.54.223; 9.AJ.54.240; 9.AJ.54.244; 9.AJ.54.243; 9.AJ.54.247;
9.AJ.55.157; 9.AJ.55.158; 9.AJ.55.196; 9.AJ.55.223; 9.AJ.55.240;
9.AJ.55.244; 9.AJ.55.243; 9.AJ.55.247; 9.AJ.56.157; 9.AJ.56.158;
9.AJ.56.196; 9.AJ.56.223; 9.AJ.56.240; 9.AJ.56.244; 9.AJ.56.243;
9.AJ.56.247; 9.AJ.157.157; 9.AJ.157.158; 9.AJ.157.196;
9.AJ.157.223; 9.AJ.157.240; 9.AJ.157.244; 9.AJ.157.243;
9.AJ.157.247; 9.AJ.196.157; 9.AJ.196.158; 9.AJ.196.196;
9.AJ.196.223; 9.AJ.196.240; 9.AJ.196.244; 9.AJ.196.243;
9.AJ.196.247; 9.AJ.223.157; 9.AJ.223.158; 9.AJ.223.196;
9.AJ.223.223; 9.AJ.223.240; 9.AJ.223.244; 9.AJ.223.243;
9.AJ.223.247; 9.AJ.240.157; 9.AJ.240.158; 9.AJ.240.196;
9.AJ.240.223; 9.AJ.240.240; 9.AJ.240.244; 9.AJ.240.243;
9.AJ.240.247; 9.AJ.244.157; 9.AJ.244.158; 9.AJ.244.196;
9.AJ.244.223; 9.AJ.244.240; 9.AJ.244.244; 9.AJ.244.243;
9.AJ.244.247; 9.AJ.247.157; 9.AJ.247.158; 9.AJ.247.196;
9.AJ.247.223; 9.AJ.247.240; 9.AJ.247.244; 9.AJ.247.243;
9.AJ.247.247; Prodrugs of 9.AN 9.AN.4.157; 9.AN.4.158; 9.AN.4.196;
9.AN.4.223; 9.AN.4.240; 9.AN.4.244; 9.AN.4.243; 9.AN.4.247;
9.AN.5.157; 9.AN.5.158; 9.AN.5.196; 9.AN.5.223; 9.AN.5.240;
9.AN.5.244; 9.AN.5.243; 9.AN.5.247; 9.AN.7.157; 9.AN.7.158;
9.AN.7.196; 9.AN.7.223; 9.AN.7.240; 9.AN.7.244; 9.AN.7.243;
9.AN.7.247; 9.AN.15.157; 9.AN.15.158; 9.AN.15.196; 9.AN.15.223;
9.AN.15.240; 9.AN.15.244; 9.AN.15.243; 9.AN.15.247; 9.AN.16.157;
9.AN.16.158; 9.AN.16.196; 9.AN.16.223; 9.AN.16.240; 9.AN.16.244;
9.AN.16.243; 9.AN.16.247; 9.AN.18.157; 9.AN.18.158; 9.AN.18.196;
9.AN.18.223; 9.AN.18.240; 9.AN.18.244; 9.AN.18.243; 9.AN.18.247;
9.AN.26.157; 9.AN.26.158; 9.AN.26.196; 9.AN.26.223; 9.AN.26.240;
9.AN.26.244; 9.AN.26.243; 9.AN.26.247; 9.AN.27.157; 9.AN.27.158;
9.AN.27.196; 9.AN.27.223; 9.AN.27.240; 9.AN.27.244; 9.AN.27.243;
9.AN.27.247; 9.AN.29.157; 9.AN.29.158; 9.AN.29.196; 9.AN.29.223;
9.AN.29.240; 9.AN.29.244; 9.AN.29.243; 9.AN.29.247; 9.AN.54.157;
9.AN.54.158; 9.AN.54.196; 9.AN.54.223; 9.AN.54.240; 9.AN.54.244;
9.AN.54.243; 9.AN.54.247; 9.AN.55.157; 9.AN.55.158; 9.AN.55.196;
9.AN.55.223; 9.AN.55.240; 9.AN.55.244; 9.AN.55.243; 9.AN.55.247;
9.AN.56.157; 9.AN.56.158; 9.AN.56.196; 9.AN.56.223; 9.AN.56.240;
9.AN.56.244; 9.AN.56.243;
9.AN.56.247; 9.AN.157.157; 9.AN.157.158; 9.AN.157.196;
9.AN.157.223; 9.AN.157.240; 9.AN.157.244; 9.AN.157.243;
9.AN.157.247; 9.AN.196.157; 9.AN.196.158; 9.AN.196.196;
9.AN.196.223; 9.AN.196.240; 9.AN.196.244; 9.AN.196.243;
9.AN.196.247; 9.AN.223.157; 9.AN.223.158; 9.AN.223.196;
9.AN.223.223; 9.AN.223.240; 9.AN.223.244; 9.AN.223.243;
9.AN.223.247; 9.AN.240.157; 9.AN.240.158; 9.AN.240.196;
9.AN.240.223; 9.AN.240.240; 9.AN.240.244; 9.AN.240.243;
9.AN.240.247; 9.AN.244.157; 9.AN.244.158; 9.AN.244.196;
9.AN.244.223; 9.AN.244.240; 9.AN.244.244; 9.AN.244.243;
9.AN.244.247; 9.AN.247.157; 9.AN.247.158; 9.AN.247.196;
9.AN.247.223; 9.AN.247.240; 9.AN.247.244; 9.AN.247.243;
9.AN.247.247; Prodrugs of 9.AP 9.AP.4.157; 9.AP.4.158; 9.AP.4.196;
9.AP.4.223; 9.AP.4.240; 9.AP.4.244; 9.AP.4.243; 9.AP.4.247;
9.AP.5.157; 9.AP.5.158; 9.AP.5.196; 9.AP.5.223; 9.AP.5.240;
9.AP.5.244; 9.AP.5.243; 9.AP.5.247; 9.AP.7.157; 9.AP.7.158;
9.AP.7.196; 9.AP.7.223; 9.AP.7.240; 9.AP.7.244; 9.AP.7.243;
9.AP.7.247; 9.AP.15.157; 9.AP.15.158; 9.AP.15.196; 9.AP.15.223;
9.AP.15.240; 9.AP.15.244; 9.AP.15.243; 9.AP.15.247; 9.AP.16.157;
9.AP.16.158; 9.AP.16.196; 9.AP.16.223; 9.AP.16.240; 9.AP.16.244;
9.AP.16.243; 9.AP.16.247; 9.AP.18.157; 9.AP.18.158; 9.AP.18.196;
9.AP.18.223; 9.AP.18.240; 9.AP.18.244; 9.AP.18.243; 9.AP.18.247;
9.AP.26.157; 9.AP.26.158; 9.AP.26.196; 9.AP.26.223; 9.AP.26.240;
9.AP.26.244; 9.AP.26.243; 9.AP.26.247; 9.AP.27.157; 9.AP.27.158;
9.AP.27.196; 9.AP.27.223; 9.AP.27.240; 9.AP.27.244; 9.AP.27.243;
9.AP.27.247; 9.AP.29.157; 9.AP.29.158; 9.AP.29.196; 9.AP.29.223;
9.AP.29.240; 9.AP.29.244; 9.AP.29.243; 9.AP.29.247; 9.AP.54.157;
9.AP.54.158; 9.AP.54.196; 9.AP.54.223; 9.AP.54.240; 9.AP.54.244;
9.AP.54.243; 9.AP.54.247; 9.AP.55.157; 9.AP.55.158; 9.AP.55.196;
9.AP.55.223; 9.AP.55.240; 9.AP.55.244; 9.AP.55.243; 9.AP.55.247;
9.AP.56.157; 9.AP.56.158; 9.AP.56.196; 9.AP.56.223; 9.AP.56.240;
9.AP.56.244; 9.AP.56.243; 9.AP.56.247; 9.AP.157.157; 9.AP.157.158;
9.AP.157.196; 9.AP.157.223; 9.AP.157.240; 9.AP.157.244;
9.AP.157.243; 9.AP.157.247; 9.AP.196.157; 9.AP.196.158;
9.AP.196.196; 9.AP.196.223; 9.AP.196.240; 9.AP.196.244;
9.AP.196.243; 9.AP.196.247; 9.AP.223.157; 9.AP.223.158;
9.AP.223.196; 9.AP.223.223; 9.AP.223.240; 9.AP.223.244;
9.AP.223.243; 9.AP.223.247; 9.AP.240.157; 9.AP.240.158;
9.AP.240.196; 9.AP.240.223; 9.AP.240.240; 9.AP.240.244;
9.AP.240.243; 9.AP.240.247; 9.AP.244.157; 9.AP.244.158;
9.AP.244.196; 9.AP.244.223; 9.AP.244.240; 9.AP.244.244;
9.AP.244.243; 9.AP.244.247; 9.AP.247.157; 9.AP.247.158;
9.AP.247.196; 9.AP.247.223; 9.AP.247.240; 9.AP.247.244;
9.AP.247.243; 9.AP.247.247; Prodrugs of 9.AZ 9.AZ.4.157;
9.AZ.4.158; 9.AZ.4.196; 9.AZ.4.223; 9.AZ.4.240; 9.AZ.4.244;
9.AZ.4.243; 9.AZ.4.247; 9.AZ.5.157; 9.AZ.5.158; 9.AZ.5.196;
9.AZ.5.223; 9.AZ.5.240; 9.AZ.5.244; 9.AZ.5.243; 9.AZ.5.247;
9.AZ.7.157; 9.AZ.7.158; 9.AZ.7.196; 9.AZ.7.223; 9.AZ.7.240;
9.AZ.7.244; 9.AZ.7.243; 9.AZ.7.247; 9.AZ.15.157; 9.AZ.15.158;
9.AZ.15.196; 9.AZ.15.223; 9.AZ.15.240; 9.AZ.15.244; 9.AZ.15.243;
9.AZ.15.247; 9.AZ.16.157; 9.AZ.16.158; 9.AZ.16.196; 9.AZ.16.223;
9.AZ.16.240; 9.AZ.16.244; 9.AZ.16.243; 9.AZ.16.247; 9.AZ.18.157;
9.AZ.18.158; 9.AZ.18.196; 9.AZ.18.223; 9.AZ.18.240; 9.AZ.18.244;
9.AZ.18.243; 9.AZ.18.247; 9.AZ.26.157; 9.AZ.26.158; 9.AZ.26.196;
9.AZ.26.223; 9.AZ.26.240; 9.AZ.26.244; 9.AZ.26.243; 9.AZ.26.247;
9.AZ.27.157; 9.AZ.27.158; 9.AZ.27.196; 9.AZ.27.223; 9.AZ.27.240;
9.AZ.27.244; 9.AZ.27.243; 9.AZ.27.247; 9.AZ.29.157; 9.AZ.29.158;
9.AZ.29.196; 9.AZ.29.223; 9.AZ.29.240; 9.AZ.29.244; 9.AZ.29.243;
9.AZ.29.247; 9.AZ.54.157; 9.AZ.54.158; 9.AZ.54.196; 9.AZ.54.223;
9.AZ.54.240; 9.AZ.54.244; 9.AZ.54.243; 9.AZ.54.247; 9.AZ.55.157;
9.AZ.55.158; 9.AZ.55.196; 9.AZ.55.223; 9.AZ.55.240; 9.AZ.55.244;
9.AZ.55.243; 9.AZ.55.247; 9.AZ.56.157; 9.AZ.56.158; 9.AZ.56.196;
9.AZ.56.223; 9.AZ.56.240; 9.AZ.56.244; 9.AZ.56.243; 9.AZ.56.247;
9.AZ.157.157; 9.AZ.157.158; 9.AZ.157.196; 9.AZ.157.223;
9.AZ.157.240; 9.AZ.157.244; 9.AZ.157.243; 9.AZ.157.247;
9.AZ.196.157; 9.AZ.196.158; 9.AZ.196.196; 9.AZ.196.223;
9.AZ.196.240; 9.AZ.196.244; 9.AZ.196.243; 9.AZ.196.247;
9.AZ.223.157; 9.AZ.223.158; 9.AZ.223.196; 9.AZ.223.223;
9.AZ.223.240; 9.AZ.223.244; 9.AZ.223.243; 9.AZ.223.247;
9.AZ.240.157; 9.AZ.240.158; 9.AZ.240.196; 9.AZ.240.223;
9.AZ.240.240; 9.AZ.240.244; 9.AZ.240.243; 9.AZ.240.247;
9.AZ.244.157; 9.AZ.244.158; 9.AZ.244.196; 9.AZ.244.223;
9.AZ.244.240; 9.AZ.244.244; 9.AZ.244.243; 9.AZ.244.247;
9.AZ.247.157; 9.AZ.247.158; 9.AZ.247.196; 9.AZ.247.223;
9.AZ.247.240; 9.AZ.247.244; 9.AZ.247.243; 9.AZ.247.247; Prodrugs of
9.BF 9.BF.4.157; 9.BF.4.158; 9.BF.4.196; 9.BF.4.223; 9.BF.4.240;
9.BF.4.244; 9.BF.4.243; 9.BF.4.247; 9.BF.5.157; 9.BF.5.158;
9.BF.5.196; 9.BF.5.223; 9.BF.5.240; 9.BF.5.244; 9.BF.5.243;
9.BF.5.247; 9.BF.7.157; 9.BF.7.158; 9.BF.7.196; 9.BF.7.223;
9.BF.7.240; 9.BF.7.244; 9.BF.7.243; 9.BF.7.247; 9.BF.15.157;
9.BF.15.158; 9.BF.15.196; 9.BF.15.223; 9.BF.15.240; 9.BF.15.244;
9.BF.15.243; 9.BF.15.247; 9.BF.16.157; 9.BF.16.158; 9.BF.16.196;
9.BF.16.223; 9.BF.16.240; 9.BF.16.244; 9.BF.16.243; 9.BF.16.247;
9.BF.18.157; 9.BF.18.158; 9.BF.18.196; 9.BF.18.223; 9.BF.18.240;
9.BF.18.244; 9.BF.18.243; 9.BF.18.247; 9.BF.26.157; 9.BF.26.158;
9.BF.26.196; 9.BF.26.223; 9.BF.26.240; 9.BF.26.244; 9.BF.26.243;
9.BF.26.247; 9.BF.27.157; 9.BF.27.158; 9.BF.27.196; 9.BF.27.223;
9.BF.27.240; 9.BF.27.244; 9.BF.27.243; 9.BF.27.247; 9.BF.29.157;
9.BF.29.158; 9.BF.29.196; 9.BF.29.223; 9.BF.29.240; 9.BF.29.244;
9.BF.29.243; 9.BF.29.247; 9.BF.54.157; 9.BF.54.158; 9.BF.54.196;
9.BF.54.223; 9.BF.54.240; 9.BF.54.244; 9.BF.54.243; 9.BF.54.247;
9.BF.55.157; 9.BF.55.158; 9.BF.55.196; 9.BF.55.223; 9.BF.55.240;
9.BF.55.244; 9.BF.55.243; 9.BF.55.247; 9.BF.56.157; 9.BF.56.158;
9.BF.56.196; 9.BF.56.223; 9.BF.56.240; 9.BF.56.244; 9.BF.56.243;
9.BF.56.247; 9.BF.157.157; 9.BF.157.158; 9.BF.157.196;
9.BF.157.223; 9.BF.157.240; 9.BF.157.244; 9.BF.157.243;
9.BF.157.247; 9.BF.196.157; 9.BF.196.158; 9.BF.196.196;
9.BF.196.223; 9.BF.196.240; 9.BF.196.244; 9.BF.196.243;
9.BF.196.247; 9.BF.223.157; 9.BF.223.158; 9.BF.223.196;
9.BF.223.223; 9.BF.223.240; 9.BF.223.244; 9.BF.223.243;
9.BF.223.247; 9.BF.240.157; 9.BF.240.158; 9.BF.240.196;
9.BF.240.223; 9.BF.240.240; 9.BF.240.244; 9.BF.240.243;
9.BF.240.247; 9.BF.244.157; 9.BF.244.158; 9.BF.244.196;
9.BF.244.223; 9.BF.244.240; 9.BF.244.244; 9.BF.244.243;
9.BF.244.247; 9.BF.247.157; 9.BF.247.158; 9.BF.247.196;
9.BF.247.223; 9.BF.247.240; 9.BF.247.244; 9.BF.247.243;
9.BF.247.247; Prodrugs of 9.CI 9.CI.4.157; 9.CI.4.158; 9.CI.4.196;
9.CI.4.223; 9.CI.4.240; 9.CI.4.244; 9.CI.4.243; 9.CI.4.247;
9.CI.5.157; 9.CI.5.158; 9.CI.5.196; 9.CI.5.223; 9.CI.5.240;
9.CI.5.244; 9.CI.5.243; 9.CI.5.247; 9.CI.7.157; 9.CI.7.158;
9.CI.7.196; 9.CI.7.223; 9.CI.7.240; 9.CI.7.244; 9.CI.7.243;
9.CI.7.247; 9.CI.15.157; 9.CI.15.158; 9.CI.15.196; 9.CI.15.223;
9.CI.15.240; 9.CI.15.244; 9.CI.15.243; 9.CI.15.247; 9.CI.16.157;
9.CI.16.158; 9.CI.16.196; 9.CI.16.223; 9.CI.16.240; 9.CI.16.244;
9.CI.16.243; 9.CI.16.247; 9.CI.18.157; 9.CI.18.158; 9.CI.18.196;
9.CI.18.223; 9.CI.18.240; 9.CI.18.244; 9.CI.18.243; 9.CI.18.247;
9.CI.26.157; 9.CI.26.158; 9.CI.26.196; 9.CI.26.223; 9.CI.26.240;
9.CI.26.244; 9.CI.26.243; 9.CI.26.247; 9.CI.27.157; 9.CI.27.158;
9.CI.27.196; 9.CI.27.223; 9.CI.27.240; 9.CI.27.244; 9.CI.27.243;
9.CI.27.247; 9.CI.29.157; 9.CI.29.158; 9.CI.29.196; 9.CI.29.223;
9.CI.29.240; 9.CI.29.244; 9.CI.29.243; 9.CI.29.247; 9.CI.54.157;
9.CI.54.158; 9.CI.54.196; 9.CI.54.223; 9.CI.54.240; 9.CI.54.244;
9.CI.54.243; 9.CI.54.247; 9.CI.55.157; 9.CI.55.158; 9.CI.55.196;
9.CI.55.223; 9.CI.55.240; 9.CI.55.244; 9.CI.55.243; 9.CI.55.247;
9.CI.56.157; 9.CI.56.158; 9.CI.56.196; 9.CI.56.223; 9.CI.56.240;
9.CI.56.244; 9.CI.56.243; 9.CI.56.247; 9.CI.157.157; 9.CI.157.158;
9.CI.157.196; 9.CI.157.223; 9.CI.157.240; 9.CI.157.244;
9.CI.157.243; 9.CI.157.247; 9.CI.196.157; 9.CI.196.158;
9.CI.196.196; 9.CI.196.223; 9.CI.196.240; 9.CI.196.244;
9.CI.196.243; 9.CI.196.247; 9.CI.223.157; 9.CI.223.158;
9.CI.223.196; 9.CI.223.223; 9.CI.223.240; 9.CI.223.244;
9.CI.223.243; 9.CI.223.247; 9.CI.240.157; 9.CI.240.158;
9.CI.240.196; 9.CI.240.223; 9.CI.240.240; 9.CI.240.244;
9.CI.240.243; 9.CI.240.247; 9.CI.244.157; 9.CI.244.158;
9.CI.244.196; 9.CI.244.223; 9.CI.244.240; 9.CI.244.244;
9.CI.244.243; 9.CI.244.247; 9.CI.247.157; 9.CI.247.158;
9.CI.247.196; 9.CI.247.223; 9.CI.247.240; 9.CI.247.244;
9.CI.247.243; 9.CI.247.247; Prodrugs of 9.CO 9.CO.4.157;
9.CO.4.158; 9.CO.4.196; 9.CO.4.223; 9.CO.4.240; 9.CO.4.244;
9.CO.4.243; 9.CO.4.247; 9.CO.5.157; 9.CO.5.158; 9.CO.5.196;
9.CO.5.223; 9.CO.5.240; 9.CO.5.244; 9.CO.5.243; 9.CO.5.247;
9.CO.7.157; 9.CO.7.158; 9.CO.7.196; 9.CO.7.223; 9.CO.7.240;
9.CO.7.244; 9.CO.7.243; 9.CO.7.247; 9.CO.15.157; 9.CO.15.158;
9.CO.15.196; 9.CO.15.223; 9.CO.15.240; 9.CO.15.244; 9.CO.15.243;
9.CO.15.247; 9.CO.16.157; 9.CO.16.158; 9.CO.16.196; 9.CO.16.223;
9.CO.16.240; 9.CO.16.244; 9.CO.16.243; 9.CO.16.247; 9.CO.18.157;
9.CO.18.158; 9.CO.18.196; 9.CO.18.223; 9.CO.18.240; 9.CO.18.244;
9.CO.18.243; 9.CO.18.247; 9.CO.26.157; 9.CO.26.158; 9.CO.26.196;
9.CO.26.223; 9.CO.26.240; 9.CO.26.244; 9.CO.26.243; 9.CO.26.247;
9.CO.27.157; 9.CO.27.158; 9.CO.27.196; 9.CO.27.223; 9.CO.27.240;
9.CO.27.244; 9.CO.27.243; 9.CO.27.247; 9.CO.29.157; 9.CO.29.158;
9.CO.29.196; 9.CO.29.223; 9.CO.29.240; 9.CO.29.244; 9.CO.29.243;
9.CO.29.247; 9.CO.54.157; 9.CO.54.158; 9.CO.54.196; 9.CO.54.223;
9.CO.54.240; 9.CO.54.244; 9.CO.54.243; 9.CO.54.247; 9.CO.55.157;
9.CO.55.158; 9.CO.55.196; 9.CO.55.223; 9.CO.55.240; 9.CO.55.244;
9.CO.55.243; 9.CO.55.247; 9.CO.56.157; 9.CO.56.158; 9.CO.56.196;
9.CO.56.223; 9.CO.56.240; 9.CO.56.244; 9.CO.56.243; 9.CO.56.247;
9.CO.157.157; 9.CO.157.158; 9.CO.157.196; 9.CO.157.223;
9.CO.157.240; 9.CO.157.244; 9.CO.157.243; 9.CO.157.247;
9.CO.196.157; 9.CO.196.158; 9.CO.196.196; 9.CO.196.223;
9.CO.196.240; 9.CO.196.244; 9.CO.196.243; 9.CO.196.247;
9.CO.223.157; 9.CO.223.158; 9.CO.223.196; 9.CO.223.223;
9.CO.223.240; 9.CO.223.244; 9.CO.223.243; 9.CO.223.247;
9.CO.240.157; 9.CO.240.158; 9.CO.240.196; 9.CO.240.223;
9.CO.240.240; 9.CO.240.244; 9.CO.240.243; 9.CO.240.247;
9.CO.244.157; 9.CO.244.158; 9.CO.244.196; 9.CO.244.223;
9.CO.244.240; 9.CO.244.244; 9.CO.244.243; 9.CO.244.247;
9.CO.247.157; 9.CO.247.158; 9.CO.247.196; 9.CO.247.223;
9.CO.247.240; 9.CO.247.244; 9.CO.247.243; 9.CO.247.247; Prodrugs of
10.AH 10.AH.4.157; 10.AH.4.158; 10.AH.4.196; 10.AH.4.223;
10.AH.4.240; 10.AH.4.244; 10.AH.4.243; 10.AH.4.247; 10.AH.5.157;
10.AH.5.158; 10.AH.5.196; 10.AH.5.223; 10.AH.5.240; 10.AH.5.244;
10.AH.5.243; 10.AH.5.247; 10.AH.7.157; 10.AH.7.158; 10.AH.7.196;
10.AH.7.223; 10.AH.7.240; 10.AH.7.244; 10.AH.7.243; 10.AH.7.247;
10.AH.15.157; 10.AH.15.158; 10.AH.15.196; 10.AH.15.223;
10.AH.15.240; 10.AH.15.244; 10.AH.15.243; 10.AH.15.247;
10.AH.16.157; 10.AH.16.158; 10.AH.16.196; 10.AH.16.223;
10.AH.16.240; 10.AH.16.244; 10.AH.16.243; 10.AH.16.247;
10.AH.18.157; 10.AH.18.158; 10.AH.18.196; 10.AH.18.223;
10.AH.18.240; 10.AH.18.244; 10.AH.18.243; 10.AH.18.247;
10.AH.26.157; 10.AH.26.158; 10.AH.26.196; 10.AH.26.223;
10.AH.26.240; 10.AH.26.244; 10.AH.26.243; 10.AH.26.247;
10.AH.27.157; 10.AH.27.158; 10.AH.27.196; 10.AH.27.223;
10.AH.27.240; 10.AH.27.244; 10.AH.27.243; 10.AH.27.247;
10.AH.29.157; 10.AH.29.158; 10.AH.29.196; 10.AH.29.223;
10.AH.29.240; 10.AH.29.244; 10.AH.29.243; 10.AH.29.247;
10.AH.54.157; 10.AH.54.158; 10.AH.54.196; 10.AH.54.223;
10.AH.54.240; 10.AH.54.244; 10.AH.54.243; 10.AH.54.247;
10.AH.55.157; 10.AH.55.158; 10.AH.55.196; 10.AH.55.223;
10.AH.55.240; 10.AH.55.244; 10.AH.55.243; 10.AH.55.247;
10.AH.56.157; 10.AH.56.158; 10.AH.56.196; 10.AH.56.223;
10.AH.56.240; 10.AH.56.244; 10.AH.56.243; 10.AH.56.247;
10.AH.157.157; 10.AH.157.158; 10.AH.157.196; 10.AH.157.223;
10.AH.157.240; 10.AH.157.244; 10.AH.157.243; 10.AH.157.247;
10.AH.196.157; 10.AH.196.158; 10.AH.196.196; 10.AH.196.223;
10.AH.196.240; 10.AH.196.244; 10.AH.196.243; 10.AH.196.247;
10.AH.223.157; 10.AH.223.158; 10.AH.223.196; 10.AH.223.223;
10.AH.223.240; 10.AH.223.244; 10.AH.223.243;
10.AH.223.247; 10.AH.240.157; 10.AH.240.158; 10.AH.240.196;
10.AH.240.223; 10.AH.240.240; 10.AH.240.244; 10.AH.240.243;
10.AH.240.247; 10.AH.244.157; 10.AH.244.158; 10.AH.244.196;
10.AH.244.223; 10.AH.244.240; 10.AH.244.244; 10.AH.244.243;
10.AH.244.247; 10.AH.247.157; 10.AH.247.158; 10.AH.247.196;
10.AH.247.223; 10.AH.247.240; 10.AH.247.244; 10.AH.247.243;
10.AH.247.247; Prodrugs of 10.AJ 10.AJ.4.157; 10.AJ.4.158;
10.AJ.4.196; 10.AJ.4.223; 10.AJ.4.240; 10.AJ.4.244; 10.AJ.4.243;
10.AJ.4.247; 10.AJ.5.157; 10.AJ.5.158; 10.AJ.5.196; 10.AJ.5.223;
10.AJ.5.240; 10.AJ.5.244; 10.AJ.5.243; 10.AJ.5.247; 10.AJ.7.157;
10.AJ.7.158; 10.AJ.7.196; 10.AJ.7.223; 10.AJ.7.240; 10.AJ.7.244;
10.AJ.7.243; 10.AJ.7.247; 10.AJ.15.157; 10.AJ.15.158; 10.AJ.15.196;
10.AJ.15.223; 10.AJ.15.240; 10.AJ.15.244; 10.AJ.15.243;
10.AJ.15.247; 10.AJ.16.157; 10.AJ.16.158; 10.AJ.16.196;
10.AJ.16.223; 10.AJ.16.240; 10.AJ.16.244; 10.AJ.16.243;
10.AJ.16.247; 10.AJ.18.157; 10.AJ.18.158; 10.AJ.18.196;
10.AJ.18.223; 10.AJ.18.240; 10.AJ.18.244; 10.AJ.18.243;
10.AJ.18.247; 10.AJ.26.157; 10.AJ.26.158; 10.AJ.26.196;
10.AJ.26.223; 10.AJ.26.240; 10.AJ.26.244; 10.AJ.26.243;
10.AJ.26.247; 10.AJ.27.157; 10.AJ.27.158; 10.AJ.27.196;
10.AJ.27.223; 10.AJ.27.240; 10.AJ.27.244; 10.AJ.27.243;
10.AJ.27.247; 10.AJ.29.157; 10.AJ.29.158; 10.AJ.29.196;
10.AJ.29.223; 10.AJ.29.240; 10.AJ.29.244; 10.AJ.29.243;
10.AJ.29.247; 10.AJ.54.157; 10.AJ.54.158; 10.AJ.54.196;
10.AJ.54.223; 10.AJ.54.240; 10.AJ.54.244; 10.AJ.54.243;
10.AJ.54.247; 10.AJ.55.157; 10.AJ.55.158; 10.AJ.55.196;
10.AJ.55.223; 10.AJ.55.240; 10.AJ.55.244; 10.AJ.55.243;
10.AJ.55.247; 10.AJ.56.157; 10.AJ.56.158; 10.AJ.56.196;
10.AJ.56.223; 10.AJ.56.240; 10.AJ.56.244; 10.AJ.56.243;
10.AJ.56.247; 10.AJ.157.157; 10.AJ.157.158; 10.AJ.157.196;
10.AJ.157.223; 10.AJ.157.240; 10.AJ.157.244; 10.AJ.157.243;
10.AJ.157.247; 10.AJ.196.157; 10.AJ.196.158; 10.AJ.196.196;
10.AJ.196.223; 10.AJ.196.240; 10.AJ.196.244; 10.AJ.196.243;
10.AJ.196.247; 10.AJ.223.157; 10.AJ.223.158; 10.AJ.223.196;
10.AJ.223.223; 10.AJ.223.240; 10.AJ.223.244; 10.AJ.223.243;
10.AJ.223.247; 10.AJ.240.157; 10.AJ.240.158; 10.AJ.240.196;
10.AJ.240.223; 10.AJ.240.240; 10.AJ.240.244; 10.AJ.240.243;
10.AJ.240.247; 10.AJ.244.157; 10.AJ.244.158; 10.AJ.244.196;
10.AJ.244.223; 10.AJ.244.240; 10.AJ.244.244; 10.AJ.244.243;
10.AJ.244.247; 10.AJ.247.157; 10.AJ.247.158; 10.AJ.247.196;
10.AJ.247.223; 10.AJ.247.240; 10.AJ.247.244; 10.AJ.247.243;
10.AJ.247.247; Prodrugs of 10.AN 10.AN.4.157; 10.AN.4.158;
10.AN.4.196; 10.AN.4.223; 10.AN.4.240; 10.AN.4.244; 10.AN.4.243;
10.AN.4.247; 10.AN.5.157; 10.AN.5.158; 10.AN.5.196; 10.AN.5.223;
10.AN.5.240; 10.AN.5.244; 10.AN.5.243; 10.AN.5.247; 10.AN.7.157;
10.AN.7.158; 10.AN.7.196; 10.AN.7.223; 10.AN.7.240; 10.AN.7.244;
10.AN.7.243; 10.AN.7.247; 10.AN.15.157; 10.AN.15.158; 10.AN.15.196;
10.AN.15.223; 10.AN.15.240; 10.AN.15.244; 10.AN.15.243;
10.AN.15.247; 10.AN.16.157; 10.AN.16.158; 10.AN.16.196;
10.AN.16.223; 10.AN.16.240; 10.AN.16.244; 10.AN.16.243;
10.AN.16.247; 10.AN.18.157; 10.AN.18.158; 10.AN.18.196;
10.AN.18.223; 10.AN.18.240; 10.AN.18.244; 10.AN.18.243;
10.AN.18.247; 10.AN.26.157; 10.AN.26.158; 10.AN.26.196;
10.AN.26.223; 10.AN.26.240; 10.AN.26.244; 10.AN.26.243;
10.AN.26.247; 10.AN.27.157; 10.AN.27.158; 10.AN.27.196;
10.AN.27.223; 10.AN.27.240; 10.AN.27.244; 10.AN.27.243;
10.AN.27.247; 10.AN.29.157; 10.AN.29.158; 10.AN.29.196;
10.AN.29.223; 10.AN.29.240; 10.AN.29.244; 10.AN.29.243;
10.AN.29.247; 10.AN.54.157; 10.AN.54.158; 10.AN.54.196;
10.AN.54.223; 10.AN.54.240; 10.AN.54.244; 10.AN.54.243;
10.AN.54.247; 10.AN.55.157; 10.AN.55.158; 10.AN.55.196;
10.AN.55.223; 10.AN.55.240; 10.AN.55.244; 10.AN.55.243;
10.AN.55.247; 10.AN.56.157; 10.AN.56.158; 10.AN.56.196;
10.AN.56.223; 10.AN.56.240; 10.AN.56.244; 10.AN.56.243;
10.AN.56.247; 10.AN.157.157; 10.AN.157.158; 10.AN.157.196;
10.AN.157.223; 10.AN.157.240; 10.AN.157.244; 10.AN.157.243;
10.AN.157.247; 10.AN.196.157; 10.AN.196.158; 10.AN.196.196;
10.AN.196.223; 10.AN.196.240; 10.AN.196.244; 10.AN.196.243;
10.AN.196.247; 10.AN.223.157; 10.AN.223.158; 10.AN.223.196;
10.AN.223.223; 10.AN.223.240; 10.AN.223.244; 10.AN.223.243;
10.AN.223.247; 10.AN.240.157; 10.AN.240.158; 10.AN.240.196;
10.AN.240.223; 10.AN.240.240; 10.AN.240.244; 10.AN.240.243;
10.AN.240.247; 10.AN.244.157; 10.AN.244.158; 10.AN.244.196;
10.AN.244.223; 10.AN.244.240; 10.AN.244.244; 10.AN.244.243;
10.AN.244.247; 10.AN.247.157; 10.AN.247.158; 10.AN.247.196;
10.AN.247.223; 10.AN.247.240; 10.AN.247.244; 10.AN.247.243;
10.AN.247.247; Prodrugs of 10.AP 10.AP.4.157; 10.AP.4.158;
10.AP.4.196; 10.AP.4.223; 10.AP.4.240; 10.AP.4.244; 10.AP.4.243;
10.AP.4.247; 10.AP.5.157; 10.AP.5.158; 10.AP.5.196; 10.AP.5.223;
10.AP.5.240; 10.AP.5.244; 10.AP.5.243; 10.AP.5.247; 10.AP.7.157;
10.AP.7.158; 10.AP.7.196; 10.AP.7.223; 10.AP.7.240; 10.AP.7.244;
10.AP.7.243; 10.AP.7.247; 10.AP.15.157; 10.AP.15.158; 10.AP.15.196;
10.AP.15.223; 10.AP.15.240; 10.AP.15.244; 10.AP.15.243;
10.AP.15.247; 10.AP.16.157; 10.AP.16.158; 10.AP.16.196;
10.AP.16.223; 10.AP.16.240; 10.AP.16.244; 10.AP.16.243;
10.AP.16.247; 10.AP.18.157; 10.AP.18.158; 10.AP.18.196;
10.AP.18.223; 10.AP.18.240; 10.AP.18.244; 10.AP.18.243;
10.AP.18.247; 10.AP.26.157; 10.AP.26.158; 10.AP.26.196;
10.AP.26.223; 10.AP.26.240; 10.AP.26.244; 10.AP.26.243;
10.AP.26.247; 10.AP.27.157; 10.AP.27.158; 10.AP.27.196;
10.AP.27.223; 10.AP.27.240; 10.AP.27.244; 10.AP.27.243;
10.AP.27.247; 10.AP.29.157; 10.AP.29.158; 10.AP.29.196;
10.AP.29.223; 10.AP.29.240; 10.AP.29.244; 10.AP.29.243;
10.AP.29.247; 10.AP.54.157; 10.AP.54.158; 10.AP.54.196;
10.AP.54.223; 10.AP.54.240; 10.AP.54.244; 10.AP.54.243;
10.AP.54.247; 10.AP.55.157; 10.AP.55.158; 10.AP.55.196;
10.AP.55.223; 10.AP.55.240; 10.AP.55.244; 10.AP.55.243;
10.AP.55.247; 10.AP.56.157; 10.AP.56.158; 10.AP.56.196;
10.AP.56.223; 10.AP.56.240; 10.AP.56.244; 10.AP.56.243;
10.AP.56.247; 10.AP.157.157; 10.AP.157.158; 10.AP.157.196;
10.AP.157.223; 10.AP.157.240; 10.AP.157.244; 10.AP.157.243;
10.AP.157.247; 10.AP.196.157; 10.AP.196.158; 10.AP.196.196;
10.AP.196.223; 10.AP.196.240; 10.AP.196.244; 10.AP.196.243;
10.AP.196.247; 10.AP.223.157; 10.AP.223.158; 10.AP.223.196;
10.AP.223.223; 10.AP.223.240; 10.AP.223.244; 10.AP.223.243;
10.AP.223.247; 10.AP.240.157; 10.AP.240.158; 10.AP.240.196;
10.AP.240.223; 10.AP.240.240; 10.AP.240.244; 10.AP.240.243;
10.AP.240.247; 10.AP.244.157; 10.AP.244.158; 10.AP.244.196;
10.AP.244.223; 10.AP.244.240; 10.AP.244.244; 10.AP.244.243;
10.AP.244.247; 10.AP.247.157; 10.AP.247.158; 10.AP.247.196;
10.AP.247.223; 10.AP.247.240; 10.AP.247.244; 10.AP.247.243;
10.AP.247.247; Prodrugs of 10.AZ 10.AZ.4.157; 10.AZ.4.158;
10.AZ.4.196; 10.AZ.4.223; 10.AZ.4.240; 10.AZ.4.244; 10.AZ.4.243;
10.AZ.4.247; 10.AZ.5.157; 10.AZ.5.158; 10.AZ.5.196; 10.AZ.5.223;
10.AZ.5.240; 10.AZ.5.244; 10.AZ.5.243; 10.AZ.5.247; 10.AZ.7.157;
10.AZ.7.158; 10.AZ.7.196; 10.AZ.7.223; 10.AZ.7.240; 10.AZ.7.244;
10.AZ.7.243; 10.AZ.7.247; 10.AZ.15.157; 10.AZ.15.158; 10.AZ.15.196;
10.AZ.15.223; 10.AZ.15.240; 10.AZ.15.244; 10.AZ.15.243;
10.AZ.15.247; 10.AZ.16.157; 10.AZ.16.158; 10.AZ.16.196;
10.AZ.16.223; 10.AZ.16.240; 10.AZ.16.244; 10.AZ.16.243;
10.AZ.16.247; 10.AZ.18.157; 10.AZ.18.158; 10.AZ.18.196;
10.AZ.18.223; 10.AZ.18.240; 10.AZ.18.244; 10.AZ.18.243;
10.AZ.18.247; 10.AZ.26.157; 10.AZ.26.158; 10.AZ.26.196;
10.AZ.26.223; 10.AZ.26.240; 10.AZ.26.244; 10.AZ.26.243;
10.AZ.26.247; 10.AZ.27.157; 10.AZ.27.158; 10.AZ.27.196;
10.AZ.27.223; 10.AZ.27.240; 10.AZ.27.244; 10.AZ.27.243;
10.AZ.27.247; 10.AZ.29.157; 10.AZ.29.158; 10.AZ.29.196;
10.AZ.29.223; 10.AZ.29.240; 10.AZ.29.244; 10.AZ.29.243;
10.AZ.29.247; 10.AZ.54.157; 10.AZ.54.158; 10.AZ.54.196;
10.AZ.54.223; 10.AZ.54.240; 10.AZ.54.244; 10.AZ.54.243;
10.AZ.54.247; 10.AZ.55.157; 10.AZ.55.158; 10.AZ.55.196;
10.AZ.55.223; 10.AZ.55.240; 10.AZ.55.244; 10.AZ.55.243;
10.AZ.55.247; 10.AZ.56.157; 10.AZ.56.158; 10.AZ.56.196;
10.AZ.56.223; 10.AZ.56.240; 10.AZ.56.244; 10.AZ.56.243;
10.AZ.56.247; 10.AZ.157.157; 10.AZ.157.158; 10.AZ.157.196;
10.AZ.157.223; 10.AZ.157.240; 10.AZ.157.244; 10.AZ.157.243;
10.AZ.157.247; 10.AZ.196.157; 10.AZ.196.158; 10.AZ.196.196;
10.AZ.196.223; 10.AZ.196.240; 10.AZ.196.244; 10.AZ.196.243;
10.AZ.196.247; 10.AZ.223.157; 10.AZ.223.158; 10.AZ.223.196;
10.AZ.223.223; 10.AZ.223.240; 10.AZ.223.244; 10.AZ.223.243;
10.AZ.223.247; 10.AZ.240.157; 10.AZ.240.158; 10.AZ.240.196;
10.AZ.240.223; 10.AZ.240.240; 10.AZ.240.244; 10.AZ.240.243;
10.AZ.240.247; 10.AZ.244.157; 10.AZ.244.158; 10.AZ.244.196;
10.AZ.244.223; 10.AZ.244.240; 10.AZ.244.244; 10.AZ.244.243;
10.AZ.244.247; 10.AZ.247.157; 10.AZ.247.158; 10.AZ.247.196;
10.AZ.247.223; 10.AZ.247.240; 10.AZ.247.244; 10.AZ.247.243;
10.AZ.247.247; Prodrugs of 10.BF 10.BF.4.157; 10.BF.4.158;
10.BF.4.196; 10.BF.4.223; 10.BF.4.240; 10.BF.4.244; 10.BF.4.243;
10.BF.4.247; 10.BF.5.157; 10.BF.5.158; 10.BF.5.196; 10.BF.5.223;
10.BF.5.240; 10.BF.5.244; 10.BF.5.243; 10.BF.5.247; 10.BF.7.157;
10.BF.7.158; 10.BF.7.196; 10.BF.7.223; 10.BF.7.240; 10.BF.7.244;
10.BF.7.243; 10.BF.7.247; 10.BF.15.157; 10.BF.15.158; 10.BF.15.196;
10.BF.15.223; 10.BF.15.240; 10.BF.15.244; 10.BF.15.243;
10.BF.15.247; 10.BF.16.157; 10.BF.16.158; 10.BF.16.196;
10.BF.16.223; 10.BF.16.240; 10.BF.16.244; 10.BF.16.243;
10.BF.16.247; 10.BF.18.157; 10.BF.18.158; 10.BF.18.196;
10.BF.18.223; 10.BF.18.240; 10.BF.18.244; 10.BF.18.243;
10.BF.18.247; 10.BF.26.157; 10.BF.26.158; 10.BF.26.196;
10.BF.26.223; 10.BF.26.240; 10.BF.26.244; 10.BF.26.243;
10.BF.26.247; 10.BF.27.157; 10.BF.27.158; 10.BF.27.196;
10.BF.27.223; 10.BF.27.240; 10.BF.27.244; 10.BF.27.243;
10.BF.27.247; 10.BF.29.157; 10.BF.29.158; 10.BF.29.196;
10.BF.29.223; 10.BF.29.240; 10.BF.29.244; 10.BF.29.243;
10.BF.29.247; 10.BF.54.157; 10.BF.54.158; 10.BF.54.196;
10.BF.54.223; 10.BF.54.240; 10.BF.54.244; 10.BF.54.243;
10.BF.54.247; 10.BF.55.157; 10.BF.55.158; 10.BF.55.196;
10.BF.55.223; 10.BF.55.240; 10.BF.55.244; 10.BF.55.243;
10.BF.55.247; 10.BF.56.157; 10.BF.56.158; 10.BF.56.196;
10.BF.56.223; 10.BF.56.240; 10.BF.56.244; 10.BF.56.243;
10.BF.56.247; 10.BF.157.157; 10.BF.157.158; 10.BF.157.196;
10.BF.157.223; 10.BF.157.240; 10.BF.157.244; 10.BF.157.243;
10.BF.157.247; 10.BF.196.157; 10.BF.196.158; 10.BF.196.196;
10.BF.196.223; 10.BF.196.240; 10.BF.196.244; 10.BF.196.243;
10.BF.196.247; 10.BF.223.157; 10.BF.223.158; 10.BF.223.196;
10.BF.223.223; 10.BF.223.240; 10.BF.223.244; 10.BF.223.243;
10.BF.223.247; 10.BF.240.157; 10.BF.240.158; 10.BF.240.196;
10.BF.240.223; 10.BF.240.240; 10.BF.240.244; 10.BF.240.243;
10.BF.240.247; 10.BF.244.157; 10.BF.244.158; 10.BF.244.196;
10.BF.244.223; 10.BF.244.240; 10.BF.244.244; 10.BF.244.243;
10.BF.244.247; 10.BF.247.157; 10.BF.247.158; 10.BF.247.196;
10.BF.247.223; 10.BF.247.240; 10.BF.247.244; 10.BF.247.243;
10.BF.247.247; Prodrugs of 10.CI 10.CI.4.157; 10.CI.4.158;
10.CI.4.196; 10.CI.4.223; 10.CI.4.240; 10.CI.4.244; 10.CI.4.243;
10.CI.4.247; 10.CI.5.157; 10.CI.5.158; 10.CI.5.196; 10.CI.5.223;
10.CI.5.240; 10.CI.5.244; 10.CI.5.243;
10.CI.5.247; 10.CI.7.157; 10.CI.7.158; 10.CI.7.196; 10.CI.7.223;
10.CI.7.240; 10.CI.7.244; 10.CI.7.243; 10.CI.7.247; 10.CI.15.157;
10.CI.15.158; 10.CI.15.196; 10.CI.15.223; 10.CI.15.240;
10.CI.15.244; 10.CI.15.243; 10.CI.15.247; 10.CI.16.157;
10.CI.16.158; 10.CI.16.196; 10.CI.16.223; 10.CI.16.240;
10.CI.16.244; 10.CI.16.243; 10.CI.16.247; 10.CI.18.157;
10.CI.18.158; 10.CI.18.196; 10.CI.18.223; 10.CI.18.240;
10.CI.18.244; 10.CI.18.243; 10.CI.18.247; 10.CI.26.157;
10.CI.26.158; 10.CI.26.196; 10.CI.26.223; 10.CI.26.240;
10.CI.26.244; 10.CI.26.243; 10.CI.26.247; 10.CI.27.157;
10.CI.27.158; 10.CI.27.196; 10.CI.27.223; 10.CI.27.240;
10.CI.27.244; 10.CI.27.243; 10.CI.27.247; 10.CI.29.157;
10.CI.29.158; 10.CI.29.196; 10.CI.29.223; 10.CI.29.240;
10.CI.29.244; 10.CI.29.243; 10.CI.29.247; 10.CI.54.157;
10.CI.54.158; 10.CI.54.196; 10.CI.54.223; 10.CI.54.240;
10.CI.54.244; 10.CI.54.243; 10.CI.54.247; 10.CI.55.157;
10.CI.55.158; 10.CI.55.196; 10.CI.55.223; 10.CI.55.240;
10.CI.55.244; 10.CI.55.243; 10.CI.55.247; 10.CI.56.157;
10.CI.56.158; 10.CI.56.196; 10.CI.56.223; 10.CI.56.240;
10.CI.56.244; 10.CI.56.243; 10.CI.56.247; 10.CI.157.157;
10.CI.157.158; 10.CI.157.196; 10.CI.157.223; 10.CI.157.240;
10.CI.157.244; 10.CI.157.243; 10.CI.157.247; 10.CI.196.157;
10.CI.196.158; 10.CI.196.196; 10.CI.196.223; 10.CI.196.240;
10.CI.196.244; 10.CI.196.243; 10.CI.196.247; 10.CI.223.157;
10.CI.223.158; 10.CI.223.196; 10.CI.223.223; 10.CI.223.240;
10.CI.223.244; 10.CI.223.243; 10.CI.223.247; 10.CI.240.157;
10.CI.240.158; 10.CI.240.196; 10.CI.240.223; 10.CI.240.240;
10.CI.240.244; 10.CI.240.243; 10.CI.240.247; 10.CI.244.157;
10.CI.244.158; 10.CI.244.196; 10.CI.244.223; 10.CI.244.240;
10.CI.244.244; 10.CI.244.243; 10.CI.244.247; 10.CI.247.157;
10.CI.247.158; 10.CI.247.196; 10.CI.247.223; 10.CI.247.240;
10.CI.247.244; 10.CI.247.243; 10.CI.247.247; Prodrugs of 10.CO
10.CO.4.157; 10.CO.4.158; 10.CO.4.196; 10.CO.4.223; 10.CO.4.240;
10.CO.4.244; 10.CO.4.243; 10.CO.4.247; 10.CO.5.157; 10.CO.5.158;
10.CO.5.196; 10.CO.5.223; 10.CO.5.240; 10.CO.5.244; 10.CO.5.243;
10.CO.5.247; 10.CO.7.157; 10.CO.7.158; 10.CO.7.196; 10.CO.7.223;
10.CO.7.240; 10.CO.7.244; 10.CO.7.243; 10.CO.7.247; 10.CO.15.157;
10.CO.15.158; 10.CO.15.196; 10.CO.15.223; 10.CO.15.240;
10.CO.15.244; 10.CO.15.243; 10.CO.15.247; 10.CO.16.157;
10.CO.16.158; 10.CO.16.196; 10.CO.16.223; 10.CO.16.240;
10.CO.16.244; 10.CO.16.243; 10.CO.16.247; 10.CO.18.157;
10.CO.18.158; 10.CO.18.196; 10.CO.18.223; 10.CO.18.240;
10.CO.18.244; 10.CO.18.243; 10.CO.18.247; 10.CO.26.157;
10.CO.26.158; 10.CO.26.196; 10.CO.26.223; 10.CO.26.240;
10.CO.26.244; 10.CO.26.243; 10.CO.26.247; 10.CO.27.157;
10.CO.27.158; 10.CO.27.196; 10.CO.27.223; 10.CO.27.240;
10.CO.27.244; 10.CO.27.243; 10.CO.27.247; 10.CO.29.157;
10.CO.29.158; 10.CO.29.196; 10.CO.29.223; 10.CO.29.240;
10.CO.29.244; 10.CO.29.243; 10.CO.29.247; 10.CO.54.157;
10.CO.54.158; 10.CO.54.196; 10.CO.54.223; 10.CO.54.240;
10.CO.54.244; 10.CO.54.243; 10.CO.54.247; 10.CO.55.157;
10.CO.55.158; 10.CO.55.196; 10.CO.55.223; 10.CO.55.240;
10.CO.55.244; 10.CO.55.243; 10.CO.55.247; 10.CO.56.157;
10.CO.56.158; 10.CO.56.196; 10.CO.56.223; 10.CO.56.240;
10.CO.56.244; 10.CO.56.243; 10.CO.56.247; 10.CO.157.157;
10.CO.157.158; 10.CO.157.196; 10.CO.157.223; 10.CO.157.240;
10.CO.157.244; 10.CO.157.243; 10.CO.157.247; 10.CO.196.157;
10.CO.196.158; 10.CO.196.196; 10.CO.196.223; 10.CO.196.240;
10.CO.196.244; 10.CO.196.243; 10.CO.196.247; 10.CO.223.157;
10.CO.223.158; 10.CO.223.196; 10.CO.223.223; 10.CO.223.240;
10.CO.223.244; 10.CO.223.243; 10.CO.223.247; 10.CO.240.157;
10.CO.240.158; 10.CO.240.196; 10.CO.240.223; 10.CO.240.240;
10.CO.240.244; 10.CO.240.243; 10.CO.240.247; 10.CO.244.157;
10.CO.244.158; 10.CO.244.196; 10.CO.244.223; 10.CO.244.240;
10.CO.244.244; 10.CO.244.243; 10.CO.244.247; 10.CO.247.157;
10.CO.247.158; 10.CO.247.196; 10.CO.247.223; 10.CO.247.240;
10.CO.247.244; 10.CO.247.243; 10.CO.247.247; Prodrugs of 11.AH
11.AH.4.157; 11.AH.4.158; 11.AH.4.196; 11.AH.4.223; 11.AH.4.240;
11.AH.4.244; 11.AH.4.243; 11.AH.4.247; 11.AH.5.157; 11.AH.5.158;
11.AH.5.196; 11.AH.5.223; 11.AH.5.240; 11.AH.5.244; 11.AH.5.243;
11.AH.5.247; 11.AH.7.157; 11.AH.7.158; 11.AH.7.196; 11.AH.7.223;
11.AH.7.240; 11.AH.7.244; 11.AH.7.243; 11.AH.7.247; 11.AH.15.157;
11.AH.15.158; 11.AH.15.196; 11.AH.15.223; 11.AH.15.240;
11.AH.15.244; 11.AH.15.243; 11.AH.15.247; 11.AH.16.157;
11.AH.16.158; 11.AH.16.196; 11.AH.16.223; 11.AH.16.240;
11.AH.16.244; 11.AH.16.243; 11.AH.16.247; 11.AH.18.157;
11.AH.18.158; 11.AH.18.196; 11.AH.18.223; 11.AH.18.240;
11.AH.18.244; 11.AH.18.243; 11.AH.18.247; 11.AH.26.157;
11.AH.26.158; 11.AH.26.196; 11.AH.26.223; 11.AH.26.240;
11.AH.26.244; 11.AH.26.243; 11.AH.26.247; 11.AH.27.157;
11.AH.27.158; 11.AH.27.196; 11.AH.27.223; 11.AH.27.240;
11.AH.27.244; 11.AH.27.243; 11.AH.27.247; 11.AH.29.157;
11.AH.29.158; 11.AH.29.196; 11.AH.29.223; 11.AH.29.240;
11.AH.29.244; 11.AH.29.243; 11.AH.29.247; 11.AH.54.157;
11.AH.54.158; 11.AH.54.196; 11.AH.54.223; 11.AH.54.240;
11.AH.54.244; 11.AH.54.243; 11.AH.54.247; 11.AH.55.157;
11.AH.55.158; 11.AH.55.196; 11.AH.55.223; 11.AH.55.240;
11.AH.55.244; 11.AH.55.243; 11.AH.55.247; 11.AH.56.157;
11.AH.56.158; 11.AH.56.196; 11.AH.56.223; 11.AH.56.240;
11.AH.56.244; 11.AH.56.243; 11.AH.56.247; 11.AH.157.157;
11.AH.157.158; 11.AH.157.196; 11.AH.157.223; 11.AH.157.240;
11.AH.157.244; 11.AH.157.243; 11.AH.157.247; 11.AH.196.157;
11.AH.196.158; 11.AH.196.196; 11.AH.196.223; 11.AH.196.240;
11.AH.196.244; 11.AH.196.243; 11.AH.196.247; 11.AH.223.157;
11.AH.223.158; 11.AH.223.196; 11.AH.223.223; 11.AH.223.240;
11.AH.223.244; 11.AH.223.243; 11.AH.223.247; 11.AH.240.157;
11.AH.240.158; 11.AH.240.196; 11.AH.240.223; 11.AH.240.240;
11.AH.240.244; 11.AH.240.243; 11.AH.240.247; 11.AH.244.157;
11.AH.244.158; 11.AH.244.196; 11.AH.244.223; 11.AH.244.240;
11.AH.244.244; 11.AH.244.243; 11.AH.244.247; 11.AH.247.157;
11.AH.247.158; 11.AH.247.196; 11.AH.247.223; 11.AH.247.240;
11.AH.247.244; 11.AH.247.243; 11.AH.247.247; Prodrugs of 11.AJ
11.AJ.4.157; 11.AJ.4.158; 11.AJ.4.196; 11.AJ.4.223; 11.AJ.4.240;
11.AJ.4.244; 11.AJ.4.243; 11.AJ.4.247; 11.AJ.5.157; 11.AJ.5.158;
11.AJ.5.196; 11.AJ.5.223; 11.AJ.5.240; 11.AJ.5.244; 11.AJ.5.243;
11.AJ.5.247; 11.AJ.7.157; 11.AJ.7.158; 11.AJ.7.196; 11.AJ.7.223;
11.AJ.7.240; 11.AJ.7.244; 11.AJ.7.243; 11.AJ.7.247; 11.AJ.15.157;
11.AJ.15.158; 11.AJ.15.196; 11.AJ.15.223; 11.AJ.15.240;
11.AJ.15.244; 11.AJ.15.243; 11.AJ.15.247; 11.AJ.16.157;
11.AJ.16.158; 11.AJ.16.196; 11.AJ.16.223; 11.AJ.16.240;
11.AJ.16.244; 11.AJ.16.243; 11.AJ.16.247; 11.AJ.18.157;
11.AJ.18.158; 11.AJ.18.196; 11.AJ.18.223; 11.AJ.18.240;
11.AJ.18.244; 11.AJ.18.243; 11.AJ.18.247; 11.AJ.26.157;
11.AJ.26.158; 11.AJ.26.196; 11.AJ.26.223; 11.AJ.26.240;
11.AJ.26.244; 11.AJ.26.243; 11.AJ.26.247; 11.AJ.27.157;
11.AJ.27.158; 11.AJ.27.196; 11.AJ.27.223; 11.AJ.27.240;
11.AJ.27.244; 11.AJ.27.243; 11.AJ.27.247; 11.AJ.29.157;
11.AJ.29.158; 11.AJ.29.196; 11.AJ.29.223; 11.AJ.29.240;
11.AJ.29.244; 11.AJ.29.243; 11.AJ.29.247; 11.AJ.54.157;
11.AJ.54.158; 11.AJ.54.196; 11.AJ.54.223; 11.AJ.54.240;
11.AJ.54.244; 11.AJ.54.243; 11.AJ.54.247; 11.AJ.55.157;
11.AJ.55.158; 11.AJ.55.196; 11.AJ.55.223; 11.AJ.55.240;
11.AJ.55.244; 11.AJ.55.243; 11.AJ.55.247; 11.AJ.56.157;
11.AJ.56.158; 11.AJ.56.196; 11.AJ.56.223; 11.AJ.56.240;
11.AJ.56.244; 11.AJ.56.243; 11.AJ.56.247; 11.AJ.157.157;
11.AJ.157.158; 11.AJ.157.196; 11.AJ.157.223; 11.AJ.157.240;
11.AJ.157.244; 11.AJ.157.243; 11.AJ.157.247; 11.AJ.196.157;
11.AJ.196.158; 11.AJ.196.196; 11.AJ.196.223; 11.AJ.196.240;
11.AJ.196.244; 11.AJ.196.243; 11.AJ.196.247; 11.AJ.223.157;
11.AJ.223.158; 11.AJ.223.196; 11.AJ.223.223; 11.AJ.223.240;
11.AJ.223.244; 11.AJ.223.243; 11.AJ.223.247; 11.AJ.240.157;
11.AJ.240.158; 11.AJ.240.196; 11.AJ.240.223; 11.AJ.240.240;
11.AJ.240.244; 11.AJ.240.243; 11.AJ.240.247; 11.AJ.244.157;
11.AJ.244.158; 11.AJ.244.196; 11.AJ.244.223; 11.AJ.244.240;
11.AJ.244.244; 11.AJ.244.243; 11.AJ.244.247; 11.AJ.247.157;
11.AJ.247.158; 11.AJ.247.196; 11.AJ.247.223; 11.AJ.247.240;
11.AJ.247.244; 11.AJ.247.243; 11.AJ.247.247; Prodrugs of 11.AN
11.AN.4.157; 11.AN.4.158; 11.AN.4.196; 11.AN.4.223; 11.AN.4.240;
11.AN.4.244; 11.AN.4.243; 11.AN.4.247; 11.AN.5.157; 11.AN.5.158;
11.AN.5.196; 11.AN.5.223; 11.AN.5.240; 11.AN.5.244; 11.AN.5.243;
11.AN.5.247; 11.AN.7.157; 11.AN.7.158; 11.AN.7.196; 11.AN.7.223;
11.AN.7.240; 11.AN.7.244; 11.AN.7.243; 11.AN.7.247; 11.AN.15.157;
11.AN.15.158; 11.AN.15.196; 11.AN.15.223; 11.AN.15.240;
11.AN.15.244; 11.AN.15.243; 11.AN.15.247; 11.AN.16.157;
11.AN.16.158; 11.AN.16.196; 11.AN.16.223; 11.AN.16.240;
11.AN.16.244; 11.AN.16.243; 11.AN.16.247; 11.AN.18.157;
11.AN.18.158; 11.AN.18.196; 11.AN.18.223; 11.AN.18.240;
11.AN.18.244; 11.AN.18.243; 11.AN.18.247; 11.AN.26.157;
11.AN.26.158; 11.AN.26.196; 11.AN.26.223; 11.AN.26.240;
11.AN.26.244; 11.AN.26.243; 11.AN.26.247; 11.AN.27.157;
11.AN.27.158; 11.AN.27.196; 11.AN.27.223; 11.AN.27.240;
11.AN.27.244; 11.AN.27.243; 11.AN.27.247; 11.AN.29.157;
11.AN.29.158; 11.AN.29.196; 11.AN.29.223; 11.AN.29.240;
11.AN.29.244; 11.AN.29.243; 11.AN.29.247; 11.AN.54.157;
11.AN.54.158; 11.AN.54.196; 11.AN.54.223; 11.AN.54.240;
11.AN.54.244; 11.AN.54.243; 11.AN.54.247; 11.AN.55.157;
11.AN.55.158; 11.AN.55.196; 11.AN.55.223; 11.AN.55.240;
11.AN.55.244; 11.AN.55.243; 11.AN.55.247; 11.AN.56.157;
11.AN.56.158; 11.AN.56.196; 11.AN.56.223; 11.AN.56.240;
11.AN.56.244; 11.AN.56.243; 11.AN.56.247; 11.AN.157.157;
11.AN.157.158; 11.AN.157.196; 11.AN.157.223; 11.AN.157.240;
11.AN.157.244; 11.AN.157.243; 11.AN.157.247; 11.AN.196.157;
11.AN.196.158; 11.AN.196.196; 11.AN.196.223; 11.AN.196.240;
11.AN.196.244; 11.AN.196.243; 11.AN.196.247; 11.AN.223.157;
11.AN.223.158; 11.AN.223.196; 11.AN.223.223; 11.AN.223.240;
11.AN.223.244; 11.AN.223.243; 11.AN.223.247; 11.AN.240.157;
11.AN.240.158; 11.AN.240.196; 11.AN.240.223; 11.AN.240.240;
11.AN.240.244; 11.AN.240.243; 11.AN.240.247; 11.AN.244.157;
11.AN.244.158; 11.AN.244.196; 11.AN.244.223; 11.AN.244.240;
11.AN.244.244; 11.AN.244.243; 11.AN.244.247; 11.AN.247.157;
11.AN.247.158; 11.AN.247.196; 11.AN.247.223; 11.AN.247.240;
11.AN.247.244; 11.AN.247.243; 11.AN.247.247; Prodrugs of 11.AP
11.AP.4.157; 11.AP.4.158; 11.AP.4.196; 11.AP.4.223; 11.AP.4.240;
11.AP.4.244; 11.AP.4.243; 11.AP.4.247; 11.AP.5.157; 11.AP.5.158;
11.AP.5.196; 11.AP.5.223; 11.AP.5.240; 11.AP.5.244; 11.AP.5.243;
11.AP.5.247; 11.AP.7.157; 11.AP.7.158; 11.AP.7.196; 11.AP.7.223;
11.AP.7.240; 11.AP.7.244; 11.AP.7.243; 11.AP.7.247; 11.AP.15.157;
11.AP.15.158; 11.AP.15.196; 11.AP.15.223; 11.AP.15.240;
11.AP.15.244; 11.AP.15.243; 11.AP.15.247; 11.AP.16.157;
11.AP.16.158; 11.AP.16.196; 11.AP.16.223; 11.AP.16.240;
11.AP.16.244; 11.AP.16.243; 11.AP.16.247; 11.AP.18.157;
11.AP.18.158; 11.AP.18.196; 11.AP.18.223; 11.AP.18.240;
11.AP.18.244; 11.AP.18.243; 11.AP.18.247; 11.AP.26.157;
11.AP.26.158; 11.AP.26.196; 11.AP.26.223; 11.AP.26.240;
11.AP.26.244; 11.AP.26.243; 11.AP.26.247; 11.AP.27.157;
11.AP.27.158; 11.AP.27.196; 11.AP.27.223; 11.AP.27.240;
11.AP.27.244; 11.AP.27.243; 11.AP.27.247; 11.AP.29.157;
11.AP.29.158; 11.AP.29.196; 11.AP.29.223; 11.AP.29.240;
11.AP.29.244; 11.AP.29.243; 11.AP.29.247; 11.AP.54.157;
11.AP.54.158; 11.AP.54.196; 11.AP.54.223; 11.AP.54.240;
11.AP.54.244; 11.AP.54.243; 11.AP.54.247; 11.AP.55.157;
11.AP.55.158; 11.AP.55.196; 11.AP.55.223; 11.AP.55.240;
11.AP.55.244; 11.AP.55.243; 11.AP.55.247; 11.AP.56.157;
11.AP.56.158; 11.AP.56.196; 11.AP.56.223; 11.AP.56.240;
11.AP.56.244; 11.AP.56.243; 11.AP.56.247; 11.AP.157.157;
11.AP.157.158; 11.AP.157.196; 11.AP.157.223; 11.AP.157.240;
11.AP.157.244; 11.AP.157.243; 11.AP.157.247; 11.AP.196.157;
11.AP.196.158; 11.AP.196.196; 11.AP.196.223; 11.AP.196.240;
11.AP.196.244; 11.AP.196.243; 11.AP.196.247; 11.AP.223.157;
11.AP.223.158; 11.AP.223.196; 11.AP.223.223; 11.AP.223.240;
11.AP.223.244; 11.AP.223.243; 11.AP.223.247; 11.AP.240.157;
11.AP.240.158; 11.AP.240.196; 11.AP.240.223; 11.AP.240.240;
11.AP.240.244; 11.AP.240.243; 11.AP.240.247; 11.AP.244.157;
11.AP.244.158; 11.AP.244.196; 11.AP.244.223; 11.AP.244.240;
11.AP.244.244; 11.AP.244.243; 11.AP.244.247; 11.AP.247.157;
11.AP.247.158; 11.AP.247.196; 11.AP.247.223; 11.AP.247.240;
11.AP.247.244; 11.AP.247.243; 11.AP.247.247; Prodrugs of 11.AZ
11.AZ.4.157; 11.AZ.4.158; 11.AZ.4.196; 11.AZ.4.223; 11.AZ.4.240;
11.AZ.4.244; 11.AZ.4.243; 11.AZ.4.247; 11.AZ.5.157; 11.AZ.5.158;
11.AZ.5.196; 11.AZ.5.223; 11.AZ.5.240; 11.AZ.5.244; 11.AZ.5.243;
11.AZ.5.247; 11.AZ.7.157; 11.AZ.7.158; 11.AZ.7.196; 11.AZ.7.223;
11.AZ.7.240; 11.AZ.7.244; 11.AZ.7.243; 11.AZ.7.247; 11.AZ.15.157;
11.AZ.15.158; 11.AZ.15.196; 11.AZ.15.223; 11.AZ.15.240;
11.AZ.15.244; 11.AZ.15.243; 11.AZ.15.247; 11.AZ.16.157;
11.AZ.16.158; 11.AZ.16.196; 11.AZ.16.223; 11.AZ.16.240;
11.AZ.16.244; 11.AZ.16.243; 11.AZ.16.247; 11.AZ.18.157;
11.AZ.18.158; 11.AZ.18.196; 11.AZ.18.223; 11.AZ.18.240;
11.AZ.18.244; 11.AZ.18.243; 11.AZ.18.247; 11.AZ.26.157;
11.AZ.26.158; 11.AZ.26.196; 11.AZ.26.223; 11.AZ.26.240;
11.AZ.26.244; 11.AZ.26.243; 11.AZ.26.247; 11.AZ.27.157;
11.AZ.27.158; 11.AZ.27.196; 11.AZ.27.223; 11.AZ.27.240;
11.AZ.27.244; 11.AZ.27.243; 11.AZ.27.247; 11.AZ.29.157;
11.AZ.29.158; 11.AZ.29.196; 11.AZ.29.223; 11.AZ.29.240;
11.AZ.29.244; 11.AZ.29.243; 11.AZ.29.247; 11.AZ.54.157;
11.AZ.54.158; 11.AZ.54.196; 11.AZ.54.223; 11.AZ.54.240;
11.AZ.54.244; 11.AZ.54.243; 11.AZ.54.247; 11.AZ.55.157;
11.AZ.55.158; 11.AZ.55.196; 11.AZ.55.223; 11.AZ.55.240;
11.AZ.55.244; 11.AZ.55.243; 11.AZ.55.247; 11.AZ.56.157;
11.AZ.56.158; 11.AZ.56.196; 11.AZ.56.223; 11.AZ.56.240;
11.AZ.56.244; 11.AZ.56.243; 11.AZ.56.247; 11.AZ.157.157;
11.AZ.157.158; 11.AZ.157.196; 11.AZ.157.223; 11.AZ.157.240;
11.AZ.157.244; 11.AZ.157.243; 11.AZ.157.247; 11.AZ.196.157;
11.AZ.196.158; 11.AZ.196.196; 11.AZ.196.223; 11.AZ.196.240;
11.AZ.196.244; 11.AZ.196.243; 11.AZ.196.247; 11.AZ.223.157;
11.AZ.223.158; 11.AZ.223.196; 11.AZ.223.223; 11.AZ.223.240;
11.AZ.223.244; 11.AZ.223.243; 11.AZ.223.247; 11.AZ.240.157;
11.AZ.240.158; 11.AZ.240.196; 11.AZ.240.223; 11.AZ.240.240;
11.AZ.240.244; 11.AZ.240.243; 11.AZ.240.247; 11.AZ.244.157;
11.AZ.244.158; 11.AZ.244.196; 11.AZ.244.223; 11.AZ.244.240;
11.AZ.244.244; 11.AZ.244.243; 11.AZ.244.247; 11.AZ.247.157;
11.AZ.247.158; 11.AZ.247.196; 11.AZ.247.223; 11.AZ.247.240;
11.AZ.247.244; 11.AZ.247.243; 11.AZ.247.247; Prodrugs of 11.BF
11.BF.4.157; 11.BF.4.158; 11.BF.4.196; 11.BF.4.223; 11.BF.4.240;
11.BF.4.244; 11.BF.4.243; 11.BF.4.247; 11.BF.5.157; 11.BF.5.158;
11.BF.5.196; 11.BF.5.223; 11.BF.5.240; 11.BF.5.244; 11.BF.5.243;
11.BF.5.247; 11.BF.7.157; 11.BF.7.158; 11.BF.7.196; 11.BF.7.223;
11.BF.7.240; 11.BF.7.244; 11.BF.7.243; 11.BF.7.247; 11.BF.15.157;
11.BF.15.158; 11.BF.15.196; 11.BF.15.223; 11.BF.15.240;
11.BF.15.244; 11.BF.15.243; 11.BF.15.247; 11.BF.16.157;
11.BF.16.158; 11.BF.16.196; 11.BF.16.223; 11.BF.16.240;
11.BF.16.244; 11.BF.16.243; 11.BF.16.247; 11.BF.18.157;
11.BF.18.158; 11.BF.18.196; 11.BF.18.223; 11.BF.18.240;
11.BF.18.244; 11.BF.18.243; 11.BF.18.247; 11.BF.26.157;
11.BF.26.158; 11.BF.26.196; 11.BF.26.223; 11.BF.26.240;
11.BF.26.244; 11.BF.26.243; 11.BF.26.247; 11.BF.27.157;
11.BF.27.158; 11.BF.27.196; 11.BF.27.223; 11.BF.27.240;
11.BF.27.244; 11.BF.27.243; 11.BF.27.247; 11.BF.29.157;
11.BF.29.158; 11.BF.29.196; 11.BF.29.223; 11.BF.29.240;
11.BF.29.244; 11.BF.29.243; 11.BF.29.247; 11.BF.54.157;
11.BF.54.158; 11.BF.54.196; 11.BF.54.223; 11.BF.54.240;
11.BF.54.244; 11.BF.54.243; 11.BF.54.247; 11.BF.55.157;
11.BF.55.158; 11.BF.55.196; 11.BF.55.223; 11.BF.55.240;
11.BF.55.244; 11.BF.55.243; 11.BF.55.247; 11.BF.56.157;
11.BF.56.158; 11.BF.56.196; 11.BF.56.223; 11.BF.56.240;
11.BF.56.244; 11.BF.56.243; 11.BF.56.247; 11.BF.157.157;
11.BF.157.158; 11.BF.157.196; 11.BF.157.223; 11.BF.157.240;
11.BF.157.244; 11.BF.157.243; 11.BF.157.247; 11.BF.196.157;
11.BF.196.158; 11.BF.196.196; 11.BF.196.223; 11.BF.196.240;
11.BF.196.244; 11.BF.196.243; 11.BF.196.247; 11.BF.223.157;
11.BF.223.158; 11.BF.223.196; 11.BF.223.223; 11.BF.223.240;
11.BF.223.244; 11.BF.223.243; 11.BF.223.247; 11.BF.240.157;
11.BF.240.158; 11.BF.240.196; 11.BF.240.223; 11.BF.240.240;
11.BF.240.244; 11.BF.240.243; 11.BF.240.247; 11.BF.244.157;
11.BF.244.158; 11.BF.244.196; 11.BF.244.223; 11.BF.244.240;
11.BF.244.244; 11.BF.244.243; 11.BF.244.247; 11.BF.247.157;
11.BF.247.158; 11.BF.247.196; 11.BF.247.223; 11.BF.247.240;
11.BF.247.244; 11.BF.247.243; 11.BF.247.247; Prodrugs of 11.CI
11.CI.4.157; 11.CI.4.158; 11.CI.4.196; 11.CI.4.223; 11.CI.4.240;
11.CI.4.244; 11.CI.4.243; 11.CI.4.247; 11.CI.5.157; 11.CI.5.158;
11.CI.5.196; 11.CI.5.223; 11.CI.5.240; 11.CI.5.244; 11.CI.5.243;
11.CI.5.247; 11.CI.7.157; 11.CI.7.158; 11.CI.7.196; 11.CI.7.223;
11.CI.7.240; 11.CI.7.244; 11.CI.7.243; 11.CI.7.247; 11.CI.15.157;
11.CI.15.158; 11.CI.15.196; 11.CI.15.223; 11.CI.15.240;
11.CI.15.244; 11.CI.15.243; 11.CI.15.247; 11.CI.16.157;
11.CI.16.158; 11.CI.16.196; 11.CI.16.223; 11.CI.16.240;
11.CI.16.244; 11.CI.16.243; 11.CI.16.247; 11.CI.18.157;
11.CI.18.158; 11.CI.18.196; 11.CI.18.223; 11.CI.18.240;
11.CI.18.244; 11.CI.18.243; 11.CI.18.247; 11.CI.26.157;
11.CI.26.158; 11.CI.26.196; 11.CI.26.223; 11.CI.26.240;
11.CI.26.244; 11.CI.26.243; 11.CI.26.247; 11.CI.27.157;
11.CI.27.158; 11.CI.27.196; 11.CI.27.223; 11.CI.27.240;
11.CI.27.244; 11.CI.27.243; 11.CI.27.247; 11.CI.29.157;
11.CI.29.158; 11.CI.29.196; 11.CI.29.223; 11.CI.29.240;
11.CI.29.244; 11.CI.29.243; 11.CI.29.247; 11.CI.54.157;
11.CI.54.158; 11.CI.54.196; 11.CI.54.223; 11.CI.54.240;
11.CI.54.244; 11.CI.54.243; 11.CI.54.247; 11.CI.55.157;
11.CI.55.158; 11.CI.55.196; 11.CI.55.223; 11.CI.55.240;
11.CI.55.244; 11.CI.55.243; 11.CI.55.247; 11.CI.56.157;
11.CI.56.158; 11.CI.56.196; 11.CI.56.223; 11.CI.56.240;
11.CI.56.244; 11.CI.56.243; 11.CI.56.247; 11.CI.157.157;
11.CI.157.158; 11.CI.157.196; 11.CI.157.223; 11.CI.157.240;
11.CI.157.244; 11.CI.157.243; 11.CI.157.247; 11.CI.196.157;
11.CI.196.158; 11.CI.196.196; 11.CI.196.223; 11.CI.196.240;
11.CI.196.244; 11.CI.196.243; 11.CI.196.247; 11.CI.223.157;
11.CI.223.158; 11.CI.223.196; 11.CI.223.223; 11.CI.223.240;
11.CI.223.244; 11.CI.223.243; 11.CI.223.247; 11.CI.240.157;
11.CI.240.158; 11.CI.240.196; 11.CI.240.223; 11.CI.240.240;
11.CI.240.244; 11.CI.240.243; 11.CI.240.247; 11.CI.244.157;
11.CI.244.158; 11.CI.244.196; 11.CI.244.223; 11.CI.244.240;
11.CI.244.244; 11.CI.244.243; 11.CI.244.247; 11.CI.247.157;
11.CI.247.158; 11.CI.247.196; 11.CI.247.223; 11.CI.247.240;
11.CI.247.244; 11.CI.247.243; 11.CI.247.247; Prodrugs of 11.CO
11.CO.4.157; 11.CO.4.158; 11.CO.4.196; 11.CO.4.223; 11.CO.4.240;
11.CO.4.244; 11.CO.4.243; 11.CO.4.247; 11.CO.5.157; 11.CO.5.158;
11.CO.5.196; 11.CO.5.223; 11.CO.5.240; 11.CO.5.244; 11.CO.5.243;
11.CO.5.247; 11.CO.7.157; 11.CO.7.158; 11.CO.7.196; 11.CO.7.223;
11.CO.7.240; 11.CO.7.244; 11.CO.7.243; 11.CO.7.247; 11.CO.15.157;
11.CO.15.158; 11.CO.15.196; 11.CO.15.223; 11.CO.15.240;
11.CO.15.244; 11.CO.15.243; 11.CO.15.247; 11.CO.16.157;
11.CO.16.158; 11.CO.16.196; 11.CO.16.223; 11.CO.16.240;
11.CO.16.244; 11.CO.16.243; 11.CO.16.247; 11.CO.18.157;
11.CO.18.158; 11.CO.18.196; 11.CO.18.223; 11.CO.18.240;
11.CO.18.244; 11.CO.18.243; 11.CO.18.247; 11.CO.26.157;
11.CO.26.158; 11.CO.26.196; 11.CO.26.223; 11.CO.26.240;
11.CO.26.244; 11.CO.26.243; 11.CO.26.247; 11.CO.27.157;
11.CO.27.158; 11.CO.27.196; 11.CO.27.223; 11.CO.27.240;
11.CO.27.244; 11.CO.27.243; 11.CO.27.247; 11.CO.29.157;
11.CO.29.158; 11.CO.29.196; 11.CO.29.223; 11.CO.29.240;
11.CO.29.244; 11.CO.29.243; 11.CO.29.247; 11.CO.54.157;
11.CO.54.158; 11.CO.54.196; 11.CO.54.223; 11.CO.54.240;
11.CO.54.244; 11.CO.54.243; 11.CO.54.247; 11.CO.55.157;
11.CO.55.158; 11.CO.55.196; 11.CO.55.223; 11.CO.55.240;
11.CO.55.244; 11.CO.55.243; 11.CO.55.247; 11.CO.56.157;
11.CO.56.158; 11.CO.56.196; 11.CO.56.223; 11.CO.56.240;
11.CO.56.244; 11.CO.56.243; 11.CO.56.247; 11.CO.157.157;
11.CO.157.158; 11.CO.157.196; 11.CO.157.223; 11.CO.157.240;
11.CO.157.244; 11.CO.157.243; 11.CO.157.247; 11.CO.196.157;
11.CO.196.158; 11.CO.196.196; 11.CO.196.223; 11.CO.196.240;
11.CO.196.244; 11.CO.196.243; 11.CO.196.247; 11.CO.223.157;
11.CO.223.158; 11.CO.223.196; 11.CO.223.223; 11.CO.223.240;
11.CO.223.244; 11.CO.223.243; 11.CO.223.247; 11.CO.240.157;
11.CO.240.158; 11.CO.240.196; 11.CO.240.223; 11.CO.240.240;
11.CO.240.244; 11.CO.240.243; 11.CO.240.247; 11.CO.244.157;
11.CO.244.158; 11.CO.244.196; 11.CO.244.223; 11.CO.244.240;
11.CO.244.244; 11.CO.244.243; 11.CO.244.247; 11.CO.247.157;
11.CO.247.158; 11.CO.247.196; 11.CO.247.223; 11.CO.247.240;
11.CO.247.244; 11.CO.247.243; 11.CO.247.247; Prodrugs of 12.AH
12.AH.4.157; 12.AH.4.158; 12.AH.4.196; 12.AH.4.223; 12.AH.4.240;
12.AH.4.244; 12.AH.4.243; 12.AH.4.247; 12.AH.5.157; 12.AH.5.158;
12.AH.5.196; 12.AH.5.223; 12.AH.5.240; 12.AH.5.244; 12.AH.5.243;
12.AH.5.247; 12.AH.7.157; 12.AH.7.158; 12.AH.7.196; 12.AH.7.223;
12.AH.7.240; 12.AH.7.244; 12.AH.7.243; 12.AH.7.247; 12.AH.15.157;
12.AH.15.158; 12.AH.15.196; 12.AH.15.223; 12.AH.15.240;
12.AH.15.244; 12.AH.15.243; 12.AH.15.247; 12.AH.16.157;
12.AH.16.158; 12.AH.16.196; 12.AH.16.223; 12.AH.16.240;
12.AH.16.244; 12.AH.16.243; 12.AH.16.247; 12.AH.18.157;
12.AH.18.158; 12.AH.18.196; 12.AH.18.223; 12.AH.18.240;
12.AH.18.244; 12.AH.18.243; 12.AH.18.247; 12.AH.26.157;
12.AH.26.158; 12.AH.26.196; 12.AH.26.223; 12.AH.26.240;
12.AH.26.244; 12.AH.26.243; 12.AH.26.247; 12.AH.27.157;
12.AH.27.158; 12.AH.27.196; 12.AH.27.223; 12.AH.27.240;
12.AH.27.244; 12.AH.27.243; 12.AH.27.247; 12.AH.29.157;
12.AH.29.158; 12.AH.29.196; 12.AH.29.223; 12.AH.29.240;
12.AH.29.244; 12.AH.29.243; 12.AH.29.247; 12.AH.54.157;
12.AH.54.158; 12.AH.54.196; 12.AH.54.223; 12.AH.54.240;
12.AH.54.244; 12.AH.54.243; 12.AH.54.247; 12.AH.55.157;
12.AH.55.158; 12.AH.55.196; 12.AH.55.223; 12.AH.55.240;
12.AH.55.244; 12.AH.55.243; 12.AH.55.247; 12.AH.56.157;
12.AH.56.158; 12.AH.56.196; 12.AH.56.223; 12.AH.56.240;
12.AH.56.244; 12.AH.56.243; 12.AH.56.247; 12.AH.157.157;
12.AH.157.158; 12.AH.157.196; 12.AH.157.223; 12.AH.157.240;
12.AH.157.244; 12.AH.157.243; 12.AH.157.247; 12.AH.196.157;
12.AH.196.158; 12.AH.196.196; 12.AH.196.223; 12.AH.196.240;
12.AH.196.244; 12.AH.196.243; 12.AH.196.247; 12.AH.223.157;
12.AH.223.158; 12.AH.223.196; 12.AH.223.223; 12.AH.223.240;
12.AH.223.244; 12.AH.223.243; 12.AH.223.247; 12.AH.240.157;
12.AH.240.158; 12.AH.240.196; 12.AH.240.223; 12.AH.240.240;
12.AH.240.244; 12.AH.240.243; 12.AH.240.247; 12.AH.244.157;
12.AH.244.158; 12.AH.244.196; 12.AH.244.223; 12.AH.244.240;
12.AH.244.244; 12.AH.244.243; 12.AH.244.247; 12.AH.247.157;
12.AH.247.158; 12.AH.247.196; 12.AH.247.223; 12.AH.247.240;
12.AH.247.244; 12.AH.247.243; 12.AH.247.247; Prodrugs of 12.AJ
12.AJ.4.157; 12.AJ.4.158; 12.AJ.4.196; 12.AJ.4.223; 12.AJ.4.240;
12.AJ.4.244; 12.AJ.4.243; 12.AJ.4.247; 12.AJ.5.157; 12.AJ.5.158;
12.AJ.5.196; 12.AJ.5.223; 12.AJ.5.240; 12.AJ.5.244; 12.AJ.5.243;
12.AJ.5.247; 12.AJ.7.157; 12.AJ.7.158; 12.AJ.7.196; 12.AJ.7.223;
12.AJ.7.240; 12.AJ.7.244; 12.AJ.7.243; 12.AJ.7.247; 12.AJ.15.157;
12.AJ.15.158; 12.AJ.15.196; 12.AJ.15.223; 12.AJ.15.240;
12.AJ.15.244;
12.AJ.15.243; 12.AJ.15.247; 12.AJ.16.157; 12.AJ.16.158;
12.AJ.16.196; 12.AJ.16.223; 12.AJ.16.240; 12.AJ.16.244;
12.AJ.16.243; 12.AJ.16.247; 12.AJ.18.157; 12.AJ.18.158;
12.AJ.18.196; 12.AJ.18.223; 12.AJ.18.240; 12.AJ.18.244;
12.AJ.18.243; 12.AJ.18.247; 12.AJ.26.157; 12.AJ.26.158;
12.AJ.26.196; 12.AJ.26.223; 12.AJ.26.240; 12.AJ.26.244;
12.AJ.26.243; 12.AJ.26.247; 12.AJ.27.157; 12.AJ.27.158;
12.AJ.27.196; 12.AJ.27.223; 12.AJ.27.240; 12.AJ.27.244;
12.AJ.27.243; 12.AJ.27.247; 12.AJ.29.157; 12.AJ.29.158;
12.AJ.29.196; 12.AJ.29.223; 12.AJ.29.240; 12.AJ.29.244;
12.AJ.29.243; 12.AJ.29.247; 12.AJ.54.157; 12.AJ.54.158;
12.AJ.54.196; 12.AJ.54.223; 12.AJ.54.240; 12.AJ.54.244;
12.AJ.54.243; 12.AJ.54.247; 12.AJ.55.157; 12.AJ.55.158;
12.AJ.55.196; 12.AJ.55.223; 12.AJ.55.240; 12.AJ.55.244;
12.AJ.55.243; 12.AJ.55.247; 12.AJ.56.157; 12.AJ.56.158;
12.AJ.56.196; 12.AJ.56.223; 12.AJ.56.240; 12.AJ.56.244;
12.AJ.56.243; 12.AJ.56.247; 12.AJ.157.157; 12.AJ.157.158;
12.AJ.157.196; 12.AJ.157.223; 12.AJ.157.240; 12.AJ.157.244;
12.AJ.157.243; 12.AJ.157.247; 12.AJ.196.157; 12.AJ.196.158;
12.AJ.196.196; 12.AJ.196.223; 12.AJ.196.240; 12.AJ.196.244;
12.AJ.196.243; 12.AJ.196.247; 12.AJ.223.157; 12.AJ.223.158;
12.AJ.223.196; 12.AJ.223.223; 12.AJ.223.240; 12.AJ.223.244;
12.AJ.223.243; 12.AJ.223.247; 12.AJ.240.157; 12.AJ.240.158;
12.AJ.240.196; 12.AJ.240.223; 12.AJ.240.240; 12.AJ.240.244;
12.AJ.240.243; 12.AJ.240.247; 12.AJ.244.157; 12.AJ.244.158;
12.AJ.244.196; 12.AJ.244.223; 12.AJ.244.240; 12.AJ.244.244;
12.AJ.244.243; 12.AJ.244.247; 12.AJ.247.157; 12.AJ.247.158;
12.AJ.247.196; 12.AJ.247.223; 12.AJ.247.240; 12.AJ.247.244;
12.AJ.247.243; 12.AJ.247.247; Prodrugs of 12.AN 12.AN.4.157;
12.AN.4.158; 12.AN.4.196; 12.AN.4.223; 12.AN.4.240; 12.AN.4.244;
12.AN.4.243; 12.AN.4.247; 12.AN.5.157; 12.AN.5.158; 12.AN.5.196;
12.AN.5.223; 12.AN.5.240; 12.AN.5.244; 12.AN.5.243; 12.AN.5.247;
12.AN.7.157; 12.AN.7.158; 12.AN.7.196; 12.AN.7.223; 12.AN.7.240;
12.AN.7.244; 12.AN.7.243; 12.AN.7.247; 12.AN.15.157; 12.AN.15.158;
12.AN.15.196; 12.AN.15.223; 12.AN.15.240; 12.AN.15.244;
12.AN.15.243; 12.AN.15.247; 12.AN.16.157; 12.AN.16.158;
12.AN.16.196; 12.AN.16.223; 12.AN.16.240; 12.AN.16.244;
12.AN.16.243; 12.AN.16.247; 12.AN.18.157; 12.AN.18.158;
12.AN.18.196; 12.AN.18.223; 12.AN.18.240; 12.AN.18.244;
12.AN.18.243; 12.AN.18.247; 12.AN.26.157; 12.AN.26.158;
12.AN.26.196; 12.AN.26.223; 12.AN.26.240; 12.AN.26.244;
12.AN.26.243; 12.AN.26.247; 12.AN.27.157; 12.AN.27.158;
12.AN.27.196; 12.AN.27.223; 12.AN.27.240; 12.AN.27.244;
12.AN.27.243; 12.AN.27.247; 12.AN.29.157; 12.AN.29.158;
12.AN.29.196; 12.AN.29.223; 12.AN.29.240; 12.AN.29.244;
12.AN.29.243; 12.AN.29.247; 12.AN.54.157; 12.AN.54.158;
12.AN.54.196; 12.AN.54.223; 12.AN.54.240; 12.AN.54.244;
12.AN.54.243; 12.AN.54.247; 12.AN.55.157; 12.AN.55.158;
12.AN.55.196; 12.AN.55.223; 12.AN.55.240; 12.AN.55.244;
12.AN.55.243; 12.AN.55.247; 12.AN.56.157; 12.AN.56.158;
12.AN.56.196; 12.AN.56.223; 12.AN.56.240; 12.AN.56.244;
12.AN.56.243; 12.AN.56.247; 12.AN.157.157; 12.AN.157.158;
12.AN.157.196; 12.AN.157.223; 12.AN.157.240; 12.AN.157.244;
12.AN.157.243; 12.AN.157.247; 12.AN.196.157; 12.AN.196.158;
12.AN.196.196; 12.AN.196.223; 12.AN.196.240; 12.AN.196.244;
12.AN.196.243; 12.AN.196.247; 12.AN.223.157; 12.AN.223.158;
12.AN.223.196; 12.AN.223.223; 12.AN.223.240; 12.AN.223.244;
12.AN.223.243; 12.AN.223.247; 12.AN.240.157; 12.AN.240.158;
12.AN.240.196; 12.AN.240.223; 12.AN.240.240; 12.AN.240.244;
12.AN.240.243; 12.AN.240.247; 12.AN.244.157; 12.AN.244.158;
12.AN.244.196; 12.AN.244.223; 12.AN.244.240; 12.AN.244.244;
12.AN.244.243; 12.AN.244.247; 12.AN.247.157; 12.AN.247.158;
12.AN.247.196; 12.AN.247.223; 12.AN.247.240; 12.AN.247.244;
12.AN.247.243; 12.AN.247.247; Prodrugs of 12.AP 12.AP.4.157;
12.AP.4.158; 12.AP.4.196; 12.AP.4.223; 12.AP.4.240; 12.AP.4.244;
12.AP.4.243; 12.AP.4.247; 12.AP.5.157; 12.AP.5.158; 12.AP.5.196;
12.AP.5.223; 12.AP.5.240; 12.AP.5.244; 12.AP.5.243; 12.AP.5.247;
12.AP.7.157; 12.AP.7.158; 12.AP.7.196; 12.AP.7.223; 12.AP.7.240;
12.AP.7.244; 12.AP.7.243; 12.AP.7.247; 12.AP.15.157; 12.AP.15.158;
12.AP.15.196; 12.AP.15.223; 12.AP.15.240; 12.AP.15.244;
12.AP.15.243; 12.AP.15.247; 12.AP.16.157; 12.AP.16.158;
12.AP.16.196; 12.AP.16.223; 12.AP.16.240; 12.AP.16.244;
12.AP.16.243; 12.AP.16.247; 12.AP.18.157; 12.AP.18.158;
12.AP.18.196; 12.AP.18.223; 12.AP.18.240; 12.AP.18.244;
12.AP.18.243; 12.AP.18.247; 12.AP.26.157; 12.AP.26.158;
12.AP.26.196; 12.AP.26.223; 12.AP.26.240; 12.AP.26.244;
12.AP.26.243; 12.AP.26.247; 12.AP.27.157; 12.AP.27.158;
12.AP.27.196; 12.AP.27.223; 12.AP.27.240; 12.AP.27.244;
12.AP.27.243; 12.AP.27.247; 12.AP.29.157; 12.AP.29.158;
12.AP.29.196; 12.AP.29.223; 12.AP.29.240; 12.AP.29.244;
12.AP.29.243; 12.AP.29.247; 12.AP.54.157; 12.AP.54.158;
12.AP.54.196; 12.AP.54.223; 12.AP.54.240; 12.AP.54.244;
12.AP.54.243; 12.AP.54.247; 12.AP.55.157; 12.AP.55.158;
12.AP.55.196; 12.AP.55.223; 12.AP.55.240; 12.AP.55.244;
12.AP.55.243; 12.AP.55.247; 12.AP.56.157; 12.AP.56.158;
12.AP.56.196; 12.AP.56.223; 12.AP.56.240; 12.AP.56.244;
12.AP.56.243; 12.AP.56.247; 12.AP.157.157; 12.AP.157.158;
12.AP.157.196; 12.AP.157.223; 12.AP.157.240; 12.AP.157.244;
12.AP.157.243; 12.AP.157.247; 12.AP.196.157; 12.AP.196.158;
12.AP.196.196; 12.AP.196.223; 12.AP.196.240; 12.AP.196.244;
12.AP.196.243; 12.AP.196.247; 12.AP.223.157; 12.AP.223.158;
12.AP.223.196; 12.AP.223.223; 12.AP.223.240; 12.AP.223.244;
12.AP.223.243; 12.AP.223.247; 12.AP.240.157; 12.AP.240.158;
12.AP.240.196; 12.AP.240.223; 12.AP.240.240; 12.AP.240.244;
12.AP.240.243; 12.AP.240.247; 12.AP.244.157; 12.AP.244.158;
12.AP.244.196; 12.AP.244.223; 12.AP.244.240; 12.AP.244.244;
12.AP.244.243; 12.AP.244.247; 12.AP.247.157; 12.AP.247.158;
12.AP.247.196; 12.AP.247.223; 12.AP.247.240; 12.AP.247.244;
12.AP.247.243; 12.AP.247.247; Prodrugs of 12.AZ 12.AZ.4.157;
12.AZ.4.158; 12.AZ.4.196; 12.AZ.4.223; 12.AZ.4.240; 12.AZ.4.244;
12.AZ.4.243; 12.AZ.4.247; 12.AZ.5.157; 12.AZ.5.158; 12.AZ.5.196;
12.AZ.5.223; 12.AZ.5.240; 12.AZ.5.244; 12.AZ.5.243; 12.AZ.5.247;
12.AZ.7.157; 12.AZ.7.158; 12.AZ.7.196; 12.AZ.7.223; 12.AZ.7.240;
12.AZ.7.244; 12.AZ.7.243; 12.AZ.7.247; 12.AZ.15.157; 12.AZ.15.158;
12.AZ.15.196; 12.AZ.15.223; 12.AZ.15.240; 12.AZ.15.244;
12.AZ.15.243; 12.AZ.15.247; 12.AZ.16.157; 12.AZ.16.158;
12.AZ.16.196; 12.AZ.16.223; 12.AZ.16.240; 12.AZ.16.244;
12.AZ.16.243; 12.AZ.16.247; 12.AZ.18.157; 12.AZ.18.158;
12.AZ.18.196; 12.AZ.18.223; 12.AZ.18.240; 12.AZ.18.244;
12.AZ.18.243; 12.AZ.18.247; 12.AZ.26.157; 12.AZ.26.158;
12.AZ.26.196; 12.AZ.26.223; 12.AZ.26.240; 12.AZ.26.244;
12.AZ.26.243; 12.AZ.26.247; 12.AZ.27.157; 12.AZ.27.158;
12.AZ.27.196; 12.AZ.27.223; 12.AZ.27.240; 12.AZ.27.244;
12.AZ.27.243; 12.AZ.27.247; 12.AZ.29.157; 12.AZ.29.158;
12.AZ.29.196; 12.AZ.29.223; 12.AZ.29.240; 12.AZ.29.244;
12.AZ.29.243; 12.AZ.29.247; 12.AZ.54.157; 12.AZ.54.158;
12.AZ.54.196; 12.AZ.54.223; 12.AZ.54.240; 12.AZ.54.244;
12.AZ.54.243; 12.AZ.54.247; 12.AZ.55.157; 12.AZ.55.158;
12.AZ.55.196; 12.AZ.55.223; 12.AZ.55.240; 12.AZ.55.244;
12.AZ.55.243; 12.AZ.55.247; 12.AZ.56.157; 12.AZ.56.158;
12.AZ.56.196; 12.AZ.56.223; 12.AZ.56.240; 12.AZ.56.244;
12.AZ.56.243; 12.AZ.56.247; 12.AZ.157.157; 12.AZ.157.158;
12.AZ.157.196; 12.AZ.157.223; 12.AZ.157.240; 12.AZ.157.244;
12.AZ.157.243; 12.AZ.157.247; 12.AZ.196.157; 12.AZ.196.158;
12.AZ.196.196; 12.AZ.196.223; 12.AZ.196.240; 12.AZ.196.244;
12.AZ.196.243; 12.AZ.196.247; 12.AZ.223.157; 12.AZ.223.158;
12.AZ.223.196; 12.AZ.223.223; 12.AZ.223.240; 12.AZ.223.244;
12.AZ.223.243; 12.AZ.223.247; 12.AZ.240.157; 12.AZ.240.158;
12.AZ.240.196; 12.AZ.240.223; 12.AZ.240.240; 12.AZ.240.244;
12.AZ.240.243; 12.AZ.240.247; 12.AZ.244.157; 12.AZ.244.158;
12.AZ.244.196; 12.AZ.244.223; 12.AZ.244.240; 12.AZ.244.244;
12.AZ.244.243; 12.AZ.244.247; 12.AZ.247.157; 12.AZ.247.158;
12.AZ.247.196; 12.AZ.247.223; 12.AZ.247.240; 12.AZ.247.244;
12.AZ.247.243; 12.AZ.247.247; Prodrugs of 12.BF 12.BF.4.157;
12.BF.4.158; 12.BF.4.196; 12.BF.4.223; 12.BF.4.240; 12.BF.4.244;
12.BF.4.243; 12.BF.4.247; 12.BF.5.157; 12.BF.5.158; 12.BF.5.196;
12.BF.5.223; 12.BF.5.240; 12.BF.5.244; 12.BF.5.243; 12.BF.5.247;
12.BF.7.157; 12.BF.7.158; 12.BF.7.196; 12.BF.7.223; 12.BF.7.240;
12.BF.7.244; 12.BF.7.243; 12.BF.7.247; 12.BF.15.157; 12.BF.15.158;
12.BF.15.196; 12.BF.15.223; 12.BF.15.240; 12.BF.15.244;
12.BF.15.243; 12.BF.15.247; 12.BF.16.157; 12.BF.16.158;
12.BF.16.196; 12.BF.16.223; 12.BF.16.240; 12.BF.16.244;
12.BF.16.243; 12.BF.16.247; 12.BF.18.157; 12.BF.18.158;
12.BF.18.196; 12.BF.18.223; 12.BF.18.240; 12.BF.18.244;
12.BF.18.243; 12.BF.18.247; 12.BF.26.157; 12.BF.26.158;
12.BF.26.196; 12.BF.26.223; 12.BF.26.240; 12.BF.26.244;
12.BF.26.243; 12.BF.26.247; 12.BF.27.157; 12.BF.27.158;
12.BF.27.196; 12.BF.27.223; 12.BF.27.240; 12.BF.27.244;
12.BF.27.243; 12.BF.27.247; 12.BF.29.157; 12.BF.29.158;
12.BF.29.196; 12.BF.29.223; 12.BF.29.240; 12.BF.29.244;
12.BF.29.243; 12.BF.29.247; 12.BF.54.157; 12.BF.54.158;
12.BF.54.196; 12.BF.54.223; 12.BF.54.240; 12.BF.54.244;
12.BF.54.243; 12.BF.54.247; 12.BF.55.157; 12.BF.55.158;
12.BF.55.196; 12.BF.55.223; 12.BF.55.240; 12.BF.55.244;
12.BF.55.243; 12.BF.55.247; 12.BF.56.157; 12.BF.56.158;
12.BF.56.196; 12.BF.56.223; 12.BF.56.240; 12.BF.56.244;
12.BF.56.243; 12.BF.56.247; 12.BF.157.157; 12.BF.157.158;
12.BF.157.196; 12.BF.157.223; 12.BF.157.240; 12.BF.157.244;
12.BF.157.243; 12.BF.157.247; 12.BF.196.157; 12.BF.196.158;
12.BF.196.196; 12.BF.196.223; 12.BF.196.240; 12.BF.196.244;
12.BF.196.243; 12.BF.196.247; 12.BF.223.157; 12.BF.223.158;
12.BF.223.196; 12.BF.223.223; 12.BF.223.240; 12.BF.223.244;
12.BF.223.243; 12.BF.223.247; 12.BF.240.157; 12.BF.240.158;
12.BF.240.196; 12.BF.240.223; 12.BF.240.240; 12.BF.240.244;
12.BF.240.243; 12.BF.240.247; 12.BF.244.157; 12.BF.244.158;
12.BF.244.196; 12.BF.244.223; 12.BF.244.240; 12.BF.244.244;
12.BF.244.243; 12.BF.244.247; 12.BF.247.157; 12.BF.247.158;
12.BF.247.196; 12.BF.247.223; 12.BF.247.240; 12.BF.247.244;
12.BF.247.243; 12.BF.247.247; Prodrugs of 12.CI 12.CI.4.157;
12.CI.4.158; 12.CI.4.196; 12.CI.4.223; 12.CI.4.240; 12.CI.4.244;
12.CI.4.243; 12.CI.4.247; 12.CI.5.157; 12.CI.5.158; 12.CI.5.196;
12.CI.5.223; 12.CI.5.240; 12.CI.5.244; 12.CI.5.243; 12.CI.5.247;
12.CI.7.157; 12.CI.7.158; 12.CI.7.196; 12.CI.7.223; 12.CI.7.240;
12.CI.7.244; 12.CI.7.243; 12.CI.7.247; 12.CI.15.157; 12.CI.15.158;
12.CI.15.196; 12.CI.15.223; 12.CI.15.240; 12.CI.15.244;
12.CI.15.243; 12.CI.15.247; 12.CI.16.157; 12.CI.16.158;
12.CI.16.196; 12.CI.16.223; 12.CI.16.240; 12.CI.16.244;
12.CI.16.243; 12.CI.16.247; 12.CI.18.157; 12.CI.18.158;
12.CI.18.196; 12.CI.18.223; 12.CI.18.240; 12.CI.18.244;
12.CI.18.243; 12.CI.18.247; 12.CI.26.157; 12.CI.26.158;
12.CI.26.196; 12.CI.26.223; 12.CI.26.240; 12.CI.26.244;
12.CI.26.243; 12.CI.26.247; 12.CI.27.157; 12.CI.27.158;
12.CI.27.196; 12.CI.27.223; 12.CI.27.240; 12.CI.27.244;
12.CI.27.243; 12.CI.27.247; 12.CI.29.157; 12.CI.29.158;
12.CI.29.196; 12.CI.29.223; 12.CI.29.240; 12.CI.29.244;
12.CI.29.243; 12.CI.29.247; 12.CI.54.157; 12.CI.54.158;
12.CI.54.196; 12.CI.54.223; 12.CI.54.240; 12.CI.54.244;
12.CI.54.243; 12.CI.54.247; 12.CI.55.157; 12.CI.55.158;
12.CI.55.196; 12.CI.55.223; 12.CI.55.240; 12.CI.55.244;
12.CI.55.243; 12.CI.55.247; 12.CI.56.157; 12.CI.56.158;
12.CI.56.196; 12.CI.56.223; 12.CI.56.240; 12.CI.56.244;
12.CI.56.243; 12.CI.56.247; 12.CI.157.157; 12.CI.157.158;
12.CI.157.196;
12.CI.157.223; 12.CI.157.240; 12.CI.157.244; 12.CI.157.243;
12.CI.157.247; 12.CI.196.157; 12.CI.196.158; 12.CI.196.196;
12.CI.196.223; 12.CI.196.240; 12.CI.196.244; 12.CI.196.243;
12.CI.196.247; 12.CI.223.157; 12.CI.223.158; 12.CI.223.196;
12.CI.223.223; 12.CI.223.240; 12.CI.223.244; 12.CI.223.243;
12.CI.223.247; 12.CI.240.157; 12.CI.240.158; 12.CI.240.196;
12.CI.240.223; 12.CI.240.240; 12.CI.240.244; 12.CI.240.243;
12.CI.240.247; 12.CI.244.157; 12.CI.244.158; 12.CI.244.196;
12.CI.244.223; 12.CI.244.240; 12.CI.244.244; 12.CI.244.243;
12.CI.244.247; 12.CI.247.157; 12.CI.247.158; 12.CI.247.196;
12.CI.247.223; 12.CI.247.240; 12.CI.247.244; 12.CI.247.243;
12.CI.247.247; Prodrugs of 12.CO 12.CO.4.157; 12.CO.4.158;
12.CO.4.196; 12.CO.4.223; 12.CO.4.240; 12.CO.4.244; 12.CO.4.243;
12.CO.4.247; 12.CO.5.157; 12.CO.5.158; 12.CO.5.196; 12.CO.5.223;
12.CO.5.240; 12.CO.5.244; 12.CO.5.243; 12.CO.5.247; 12.CO.7.157;
12.CO.7.158; 12.CO.7.196; 12.CO.7.223; 12.CO.7.240; 12.CO.7.244;
12.CO.7.243; 12.CO.7.247; 12.CO.15.157; 12.CO.15.158; 12.CO.15.196;
12.CO.15.223; 12.CO.15.240; 12.CO.15.244; 12.CO.15.243;
12.CO.15.247; 12.CO.16.157; 12.CO.16.158; 12.CO.16.196;
12.CO.16.223; 12.CO.16.240; 12.CO.16.244; 12.CO.16.243;
12.CO.16.247; 12.CO.18.157; 12.CO.18.158; 12.CO.18.196;
12.CO.18.223; 12.CO.18.240; 12.CO.18.244; 12.CO.18.243;
12.CO.18.247; 12.CO.26.157; 12.CO.26.158; 12.CO.26.196;
12.CO.26.223; 12.CO.26.240; 12.CO.26.244; 12.CO.26.243;
12.CO.26.247; 12.CO.27.157; 12.CO.27.158; 12.CO.27.196;
12.CO.27.223; 12.CO.27.240; 12.CO.27.244; 12.CO.27.243;
12.CO.27.247; 12.CO.29.157; 12.CO.29.158; 12.CO.29.196;
12.CO.29.223; 12.CO.29.240; 12.CO.29.244; 12.CO.29.243;
12.CO.29.247; 12.CO.54.157; 12.CO.54.158; 12.CO.54.196;
12.CO.54.223; 12.CO.54.240; 12.CO.54.244; 12.CO.54.243;
12.CO.54.247; 12.CO.55.157; 12.CO.55.158; 12.CO.55.196;
12.CO.55.223; 12.CO.55.240; 12.CO.55.244; 12.CO.55.243;
12.CO.55.247; 12.CO.56.157; 12.CO.56.158; 12.CO.56.196;
12.CO.56.223; 12.CO.56.240; 12.CO.56.244; 12.CO.56.243;
12.CO.56.247; 12.CO.157.157; 12.CO.157.158; 12.CO.157.196;
12.CO.157.223; 12.CO.157.240; 12.CO.157.244; 12.CO.157.243;
12.CO.157.247; 12.CO.196.157; 12.CO.196.158; 12.CO.196.196;
12.CO.196.223; 12.CO.196.240; 12.CO.196.244; 12.CO.196.243;
12.CO.196.247; 12.CO.223.157; 12.CO.223.158; 12.CO.223.196;
12.CO.223.223; 12.CO.223.240; 12.CO.223.244; 12.CO.223.243;
12.CO.223.247; 12.CO.240.157; 12.CO.240.158; 12.CO.240.196;
12.CO.240.223; 12.CO.240.240; 12.CO.240.244; 12.CO.240.243;
12.CO.240.247; 12.CO.244.157; 12.CO.244.158; 12.CO.244.196;
12.CO.244.223; 12.CO.244.240; 12.CO.244.244; 12.CO.244.243;
12.CO.244.247; 12.CO.247.157; 12.CO.247.158; 12.CO.247.196;
12.CO.247.223; 12.CO.247.240; 12.CO.247.244; 12.CO.247.243;
12.CO.247.247. Prodrugs of 13.B 13.B.228.228; 13.B.228.229;
13.B.228.230; 13.B.228.231; 13.B.228.236; 13.B.228.237;
13.B.228.238; 13.B.228.239; 13.B.228.154; 13.B.228.157;
13.B.228.166; 13.B.228.169; 13.B.228.172; 13.B.228.175;
13.B.228.240; 13.B.228.244; 13.B.229.228; 13.B.229.229;
13.B.229.230; 13.B.229.231; 13.B.229.236; 13.B.229.237;
13.B.229.238; 13.B.229.239; 13.B.229.154; 13.B.229.157;
13.B.229.166; 13.B.229.169; 13.B.229.172; 13.B.229.175;
13.B.229.240; 13.B.229.244; 13.B.230.228; 13.B.230.229;
13.B.230.230; 13.B.230.231; 13.B.230.236; 13.B.230.237;
13.B.230.238; 13.B.230.239; 13.B.230.154; 13.B.230.157;
13.B.230.166; 13.B.230.169; 13.B.230.172; 13.B.230.175;
13.B.230.240; 13.B.230.244; 13.B.231.228; 13.B.231.229;
13.B.231.230; 13.B.231.231; 13.B.231.236; 13.B.231.237;
13.B.231.238; 13.B.231.239; 13.B.231.154; 13.B.231.157;
13.B.231.166; 13.B.231.169; 13.B.231.172; 13.B.231.175;
13.B.231.240; 13.B.231.244; 13.B.236.228; 13.B.236.229;
13.B.236.230; 13.B.236.231; 13.B.236.236; 13.B.236.237;
13.B.236.238; 13.B.236.239; 13.B.236.154; 13.B.236.157;
13.B.236.166; 13.B.236.169; 13.B.236.172; 13.B.236.175;
13.B.236.240; 13.B.236.244; 13.B.237.228; 13.B.237.229;
13.B.237.230; 13.B.237.231; 13.B.237.236; 13.B.237.237;
13.B.237.238; 13.B.237.239; 13.B.237.154; 13.B.237.157;
13.B.237.166; 13.B.237.169; 13.B.237.172; 13.B.237.175;
13.B.237.240; 13.B.237.244; 13.B.238.228; 13.B.238.229;
13.B.238.230; 13.B.238.231; 13.B.238.236; 13.B.238.237;
13.B.238.238; 13.B.238.239; 13.B.238.154; 13.B.238.157;
13.B.238.166; 13.B.238.169; 13.B.238.172; 13.B.238.175;
13.B.238.240; 13.B.238.244; 13.B.239.228; 13.B.239.229;
13.B.239.230; 13.B.239.231; 13.B.239.236; 13.B.239.237;
13.B.239.238; 13.B.239.239; 13.B.239.154; 13.B.239.157;
13.B.239.166; 13.B.239.169; 13.B.239.172; 13.B.239.175;
13.B.239.240; 13.B.239.244; 13.B.154.228; 13.B.154.229;
13.B.154.230; 13.B.154.231; 13.B.154.236; 13.B.154.237;
13.B.154.238; 13.B.154.239; 13.B.154.154; 13.B.154.157;
13.B.154.166; 13.B.154.169; 13.B.154.172; 13.B.154.175;
13.B.154.240; 13.B.154.244; 13.B.157.228; 13.B.157.229;
13.B.157.230; 13.B.157.231; 13.B.157.236; 13.B.157.237;
13.B.157.238; 13.B.157.239; 13.B.157.154; 13.B.157.157;
13.B.157.166; 13.B.157.169; 13.B.157.172; 13.B.157.175;
13.B.157.240; 13.B.157.244; 13.B.166.228; 13.B.166.229;
13.B.166.230; 13.B.166.231; 13.B.166.236; 13.B.166.237;
13.B.166.238; 13.B.166.239; 13.B.166.154; 13.B.166.157;
13.B.166.166; 13.B.166.169; 13.B.166.172; 13.B.166.175;
13.B.166.240; 13.B.166.244; 13.B.169.228; 13.B.169.229;
13.B.169.230; 13.B.169.231; 13.B.169.236; 13.B.169.237;
13.B.169.238; 13.B.169.239; 13.B.169.154; 13.B.169.157;
13.B.169.166; 13.B.169.169; 13.B.169.172; 13.B.169.175;
13.B.169.240; 13.B.169.244; 13.B.172.228; 13.B.172.229;
13.B.172.230; 13.B.172.231; 13.B.172.236; 13.B.172.237;
13.B.172.238; 13.B.172.239; 13.B.172.154; 13.B.172.157;
13.B.172.166; 13.B.172.169; 13.B.172.172; 13.B.172.175;
13.B.172.240; 13.B.172.244; 13.B.175.228; 13.B.175.229;
13.B.175.230; 13.B.175.231; 13.B.175.236; 13.B.175.237;
13.B.175.238; 13.B.175.239; 13.B.175.154; 13.B.175.157;
13.B.175.166; 13.B.175.169; 13.B.175.172; 13.B.175.175;
13.B.175.240; 13.B.175.244; 13.B.240.228; 13.B.240.229;
13.B.240.230; 13.B.240.231; 13.B.240.236; 13.B.240.237;
13.B.240.238; 13.B.240.239; 13.B.240.154; 13.B.240.157;
13.B.240.166; 13.B.240.169; 13.B.240.172; 13.B.240.175;
13.B.240.240; 13.B.240.244; 13.B.244.228; 13.B.244.229;
13.B.244.230; 13.B.244.231; 13.B.244.236; 13.B.244.237;
13.B.244.238; 13.B.244.239; 13.B.244.154; 13.B.244.157;
13.B.244.166; 13.B.244.169; 13.B.244.172; 13.B.244.175;
13.B.244.240; 13.B.244.244; Prodrugs of 13.D 13.D.228.228;
13.D.228.229; 13.D.228.230; 13.D.228.231; 13.D.228.236;
13.D.228.237; 13.D.228.238; 13.D.228.239; 13.D.228.154;
13.D.228.157; 13.D.228.166; 13.D.228.169; 13.D.228.172;
13.D.228.175; 13.D.228.240; 13.D.228.244; 13.D.229.228;
13.D.229.229; 13.D.229.230; 13.D.229.231; 13.D.229.236;
13.D.229.237; 13.D.229.238; 13.D.229.239; 13.D.229.154;
13.D.229.157; 13.D.229.166; 13.D.229.169; 13.D.229.172;
13.D.229.175; 13.D.229.240; 13.D.229.244; 13.D.230.228;
13.D.230.229; 13.D.230.230; 13.D.230.231; 13.D.230.236;
13.D.230.237; 13.D.230.238; 13.D.230.239; 13.D.230.154;
13.D.230.157; 13.D.230.166; 13.D.230.169; 13.D.230.172;
13.D.230.175; 13.D.230.240; 13.D.230.244; 13.D.231.228;
13.D.231.229; 13.D.231.230; 13.D.231.231; 13.D.231.236;
13.D.231.237; 13.D.231.238; 13.D.231.239; 13.D.231.154;
13.D.231.157; 13.D.231.166; 13.D.231.169; 13.D.231.172;
13.D.231.175; 13.D.231.240; 13.D.231.244; 13.D.236.228;
13.D.236.229; 13.D.236.230; 13.D.236.231; 13.D.236.236;
13.D.236.237; 13.D.236.238; 13.D.236.239; 13.D.236.154;
13.D.236.157; 13.D.236.166; 13.D.236.169; 13.D.236.172;
13.D.236.175; 13.D.236.240; 13.D.236.244; 13.D.237.228;
13.D.237.229; 13.D.237.230; 13.D.237.231; 13.D.237.236;
13.D.237.237; 13.D.237.238; 13.D.237.239; 13.D.237.154;
13.D.237.157; 13.D.237.166; 13.D.237.169; 13.D.237.172;
13.D.237.175; 13.D.237.240; 13.D.237.244; 13.D.238.228;
13.D.238.229; 13.D.238.230; 13.D.238.231; 13.D.238.236;
13.D.238.237; 13.D.238.238; 13.D.238.239; 13.D.238.154;
13.D.238.157; 13.D.238.166; 13.D.238.169; 13.D.238.172;
13.D.238.175; 13.D.238.240; 13.D.238.244; 13.D.239.228;
13.D.239.229; 13.D.239.230; 13.D.239.231; 13.D.239.236;
13.D.239.237; 13.D.239.238; 13.D.239.239; 13.D.239.154;
13.D.239.157; 13.D.239.166; 13.D.239.169; 13.D.239.172;
13.D.239.175; 13.D.239.240; 13.D.239.244; 13.D.154.228;
13.D.154.229; 13.D.154.230; 13.D.154.231; 13.D.154.236;
13.D.154.237; 13.D.154.238; 13.D.154.239; 13.D.154.154;
13.D.154.157; 13.D.154.166; 13.D.154.169; 13.D.154.172;
13.D.154.175; 13.D.154.240; 13.D.154.244; 13.D.157.228;
13.D.157.229; 13.D.157.230; 13.D.157.231; 13.D.157.236;
13.D.157.237; 13.D.157.238; 13.D.157.239; 13.D.157.154;
13.D.157.157; 13.D.157.166; 13.D.157.169; 13.D.157.172;
13.D.157.175; 13.D.157.240; 13.D.157.244; 13.D.166.228;
13.D.166.229; 13.D.166.230; 13.D.166.231; 13.D.166.236;
13.D.166.237; 13.D.166.238; 13.D.166.239; 13.D.166.154;
13.D.166.157; 13.D.166.166; 13.D.166.169; 13.D.166.172;
13.D.166.175; 13.D.166.240; 13.D.166.244; 13.D.169.228;
13.D.169.229; 13.D.169.230; 13.D.169.231; 13.D.169.236;
13.D.169.237; 13.D.169.238; 13.D.169.239; 13.D.169.154;
13.D.169.157; 13.D.169.166; 13.D.169.169; 13.D.169.172;
13.D.169.175; 13.D.169.240; 13.D.169.244; 13.D.172.228;
13.D.172.229; 13.D.172.230; 13.D.172.231; 13.D.172.236;
13.D.172.237; 13.D.172.238; 13.D.172.239; 13.D.172.154;
13.D.172.157; 13.D.172.166; 13.D.172.169; 13.D.172.172;
13.D.172.175; 13.D.172.240; 13.D.172.244; 13.D.175.228;
13.D.175.229; 13.D.175.230; 13.D.175.231; 13.D.175.236;
13.D.175.237; 13.D.175.238; 13.D.175.239; 13.D.175.154;
13.D.175.157; 13.D.175.166; 13.D.175.169; 13.D.175.172;
13.D.175.175; 13.D.175.240; 13.D.175.244; 13.D.240.228;
13.D.240.229; 13.D.240.230; 13.D.240.231; 13.D.240.236;
13.D.240.237; 13.D.240.238; 13.D.240.239; 13.D.240.154;
13.D.240.157; 13.D.240.166; 13.D.240.169; 13.D.240.172;
13.D.240.175; 13.D.240.240; 13.D.240.244; 13.D.244.228;
13.D.244.229; 13.D.244.230; 13.D.244.231; 13.D.244.236;
13.D.244.237; 13.D.244.238; 13.D.244.239; 13.D.244.154;
13.D.244.157; 13.D.244.166; 13.D.244.169; 13.D.244.172;
13.D.244.175; 13.D.244.240; 13.D.244.244; Prodrugs of 13.E
13.E.228.228; 13.E.228.229; 13.E.228.230; 13.E.228.231;
13.E.228.236; 13.E.228.237; 13.E.228.238; 13.E.228.239;
13.E.228.154; 13.E.228.157; 13.E.228.166; 13.E.228.169;
13.E.228.172; 13.E.228.175; 13.E.228.240; 13.E.228.244;
13.E.229.228; 13.E.229.229; 13.E.229.230; 13.E.229.231;
13.E.229.236; 13.E.229.237; 13.E.229.238; 13.E.229.239;
13.E.229.154; 13.E.229.157; 13.E.229.166; 13.E.229.169;
13.E.229.172; 13.E.229.175; 13.E.229.240; 13.E.229.244;
13.E.230.228; 13.E.230.229; 13.E.230.230; 13.E.230.231;
13.E.230.236; 13.E.230.237; 13.E.230.238; 13.E.230.239;
13.E.230.154; 13.E.230.157; 13.E.230.166; 13.E.230.169;
13.E.230.172; 13.E.230.175; 13.E.230.240; 13.E.230.244;
13.E.231.228; 13.E.231.229; 13.E.231.230; 13.E.231.231;
13.E.231.236; 13.E.231.237; 13.E.231.238; 13.E.231.239;
13.E.231.154; 13.E.231.157; 13.E.231.166; 13.E.231.169;
13.E.231.172; 13.E.231.175; 13.E.231.240; 13.E.231.244;
13.E.236.228; 13.E.236.229; 13.E.236.230; 13.E.236.231;
13.E.236.236; 13.E.236.237; 13.E.236.238; 13.E.236.239;
13.E.236.154; 13.E.236.157; 13.E.236.166; 13.E.236.169;
13.E.236.172; 13.E.236.175; 13.E.236.240; 13.E.236.244;
13.E.237.228; 13.E.237.229; 13.E.237.230; 13.E.237.231;
13.E.237.236; 13.E.237.237; 13.E.237.238; 13.E.237.239;
13.E.237.154; 13.E.237.157; 13.E.237.166; 13.E.237.169;
13.E.237.172; 13.E.237.175; 13.E.237.240; 13.E.237.244;
13.E.238.228; 13.E.238.229; 13.E.238.230; 13.E.238.231;
13.E.238.236; 13.E.238.237; 13.E.238.238; 13.E.238.239;
13.E.238.154; 13.E.238.157; 13.E.238.166; 13.E.238.169;
13.E.238.172; 13.E.238.175; 13.E.238.240; 13.E.238.244;
13.E.239.228; 13.E.239.229; 13.E.239.230; 13.E.239.231;
13.E.239.236; 13.E.239.237; 13.E.239.238; 13.E.239.239;
13.E.239.154; 13.E.239.157; 13.E.239.166; 13.E.239.169;
13.E.239.172; 13.E.239.175; 13.E.239.240; 13.E.239.244;
13.E.154.228; 13.E.154.229; 13.E.154.230; 13.E.154.231;
13.E.154.236; 13.E.154.237; 13.E.154.238; 13.E.154.239;
13.E.154.154; 13.E.154.157; 13.E.154.166; 13.E.154.169;
13.E.154.172; 13.E.154.175; 13.E.154.240; 13.E.154.244;
13.E.157.228; 13.E.157.229; 13.E.157.230; 13.E.157.231;
13.E.157.236; 13.E.157.237; 13.E.157.238; 13.E.157.239;
13.E.157.154; 13.E.157.157; 13.E.157.166; 13.E.157.169;
13.E.157.172; 13.E.157.175; 13.E.157.240; 13.E.157.244;
13.E.166.228; 13.E.166.229; 13.E.166.230; 13.E.166.231;
13.E.166.236; 13.E.166.237; 13.E.166.238; 13.E.166.239;
13.E.166.154; 13.E.166.157; 13.E.166.166; 13.E.166.169;
13.E.166.172; 13.E.166.175; 13.E.166.240; 13.E.166.244;
13.E.169.228; 13.E.169.229; 13.E.169.230; 13.E.169.231;
13.E.169.236; 13.E.169.237; 13.E.169.238; 13.E.169.239;
13.E.169.154; 13.E.169.157; 13.E.169.166; 13.E.169.169;
13.E.169.172; 13.E.169.175; 13.E.169.240; 13.E.169.244;
13.E.172.228; 13.E.172.229; 13.E.172.230; 13.E.172.231;
13.E.172.236; 13.E.172.237; 13.E.172.238; 13.E.172.239;
13.E.172.154; 13.E.172.157; 13.E.172.166; 13.E.172.169;
13.E.172.172; 13.E.172.175; 13.E.172.240; 13.E.172.244;
13.E.175.228; 13.E.175.229; 13.E.175.230; 13.E.175.231;
13.E.175.236; 13.E.175.237; 13.E.175.238; 13.E.175.239;
13.E.175.154; 13.E.175.157; 13.E.175.166; 13.E.175.169;
13.E.175.172; 13.E.175.175; 13.E.175.240; 13.E.175.244;
13.E.240.228; 13.E.240.229; 13.E.240.230; 13.E.240.231;
13.E.240.236; 13.E.240.237; 13.E.240.238; 13.E.240.239;
13.E.240.154; 13.E.240.157; 13.E.240.166; 13.E.240.169;
13.E.240.172; 13.E.240.175; 13.E.240.240; 13.E.240.244;
13.E.244.228; 13.E.244.229; 13.E.244.230; 13.E.244.231;
13.E.244.236; 13.E.244.237; 13.E.244.238; 13.E.244.239;
13.E.244.154; 13.E.244.157; 13.E.244.166; 13.E.244.169;
13.E.244.172; 13.E.244.175; 13.E.244.240; 13.E.244.244; Prodrugs of
13.G 13.G.228.228; 13.G.228.229; 13.G.228.230; 13.G.228.231;
13.G.228.236; 13.G.228.237; 13.G.228.238; 13.G.228.239;
13.G.228.154; 13.G.228.157; 13.G.228.166; 13.G.228.169;
13.G.228.172; 13.G.228.175; 13.G.228.240; 13.G.228.244;
13.G.229.228; 13.G.229.229; 13.G.229.230; 13.G.229.231;
13.G.229.236; 13.G.229.237; 13.G.229.238; 13.G.229.239;
13.G.229.154; 13.G.229.157; 13.G.229.166; 13.G.229.169;
13.G.229.172; 13.G.229.175; 13.G.229.240; 13.G.229.244;
13.G.230.228; 13.G.230.229; 13.G.230.230; 13.G.230.231;
13.G.230.236; 13.G.230.237; 13.G.230.238; 13.G.230.239;
13.G.230.154; 13.G.230.157; 13.G.230.166; 13.G.230.169;
13.G.230.172; 13.G.230.175; 13.G.230.240; 13.G.230.244;
13.G.231.228; 13.G.231.229; 13.G.231.230; 13.G.231.231;
13.G.231.236; 13.G.231.237; 13.G.231.238; 13.G.231.239;
13.G.231.154; 13.G.231.157; 13.G.231.166; 13.G.231.169;
13.G.231.172; 13.G.231.175; 13.G.231.240; 13.G.231.244;
13.G.236.228; 13.G.236.229; 13.G.236.230; 13.G.236.231;
13.G.236.236; 13.G.236.237; 13.G.236.238; 13.G.236.239;
13.G.236.154; 13.G.236.157; 13.G.236.166; 13.G.236.169;
13.G.236.172; 13.G.236.175; 13.G.236.240; 13.G.236.244;
13.G.237.228; 13.G.237.229; 13.G.237.230; 13.G.237.231;
13.G.237.236; 13.G.237.237; 13.G.237.238; 13.G.237.239;
13.G.237.154; 13.G.237.157; 13.G.237.166; 13.G.237.169;
13.G.237.172; 13.G.237.175; 13.G.237.240; 13.G.237.244;
13.G.238.228; 13.G.238.229; 13.G.238.230; 13.G.238.231;
13.G.238.236; 13.G.238.237; 13.G.238.238; 13.G.238.239;
13.G.238.154; 13.G.238.157; 13.G.238.166; 13.G.238.169;
13.G.238.172; 13.G.238.175; 13.G.238.240; 13.G.238.244;
13.G.239.228; 13.G.239.229; 13.G.239.230; 13.G.239.231;
13.G.239.236; 13.G.239.237; 13.G.239.238; 13.G.239.239;
13.G.239.154; 13.G.239.157; 13.G.239.166; 13.G.239.169;
13.G.239.172; 13.G.239.175; 13.G.239.240; 13.G.239.244;
13.G.154.228; 13.G.154.229; 13.G.154.230; 13.G.154.231;
13.G.154.236; 13.G.154.237; 13.G.154.238; 13.G.154.239;
13.G.154.154; 13.G.154.157; 13.G.154.166; 13.G.154.169;
13.G.154.172; 13.G.154.175; 13.G.154.240; 13.G.154.244;
13.G.157.228; 13.G.157.229; 13.G.157.230; 13.G.157.231;
13.G.157.236; 13.G.157.237; 13.G.157.238; 13.G.157.239;
13.G.157.154; 13.G.157.157; 13.G.157.166; 13.G.157.169;
13.G.157.172; 13.G.157.175; 13.G.157.240; 13.G.157.244;
13.G.166.228; 13.G.166.229; 13.G.166.230; 13.G.166.231;
13.G.166.236; 13.G.166.237; 13.G.166.238; 13.G.166.239;
13.G.166.154; 13.G.166.157; 13.G.166.166; 13.G.166.169;
13.G.166.172; 13.G.166.175; 13.G.166.240; 13.G.166.244;
13.G.169.228; 13.G.169.229; 13.G.169.230; 13.G.169.231;
13.G.169.236; 13.G.169.237; 13.G.169.238; 13.G.169.239;
13.G.169.154; 13.G.169.157; 13.G.169.166; 13.G.169.169;
13.G.169.172; 13.G.169.175; 13.G.169.240; 13.G.169.244;
13.G.172.228; 13.G.172.229; 13.G.172.230; 13.G.172.231;
13.G.172.236; 13.G.172.237; 13.G.172.238; 13.G.172.239;
13.G.172.154; 13.G.172.157; 13.G.172.166; 13.G.172.169;
13.G.172.172; 13.G.172.175; 13.G.172.240; 13.G.172.244;
13.G.175.228; 13.G.175.229; 13.G.175.230; 13.G.175.231;
13.G.175.236; 13.G.175.237; 13.G.175.238; 13.G.175.239;
13.G.175.154; 13.G.175.157; 13.G.175.166; 13.G.175.169;
13.G.175.172; 13.G.175.175; 13.G.175.240; 13.G.175.244;
13.G.240.228; 13.G.240.229; 13.G.240.230; 13.G.240.231;
13.G.240.236; 13.G.240.237; 13.G.240.238; 13.G.240.239;
13.G.240.154; 13.G.240.157; 13.G.240.166; 13.G.240.169;
13.G.240.172; 13.G.240.175; 13.G.240.240; 13.G.240.244;
13.G.244.228; 13.G.244.229; 13.G.244.230; 13.G.244.231;
13.G.244.236; 13.G.244.237; 13.G.244.238; 13.G.244.239;
13.G.244.154; 13.G.244.157; 13.G.244.166; 13.G.244.169;
13.G.244.172; 13.G.244.175; 13.G.244.240; 13.G.244.244; Prodrugs of
13.I 13.I.228.228; 13.I.228.229; 13.I.228.230; 13.I.228.231;
13.I.228.236; 13.I.228.237; 13.I.228.238; 13.I.228.239;
13.I.228.154; 13.I.228.157; 13.I.228.166; 13.I.228.169;
13.I.228.172; 13.I.228.175; 13.I.228.240; 13.I.228.244;
13.I.229.228; 13.I.229.229; 13.I.229.230; 13.I.229.231;
13.I.229.236; 13.I.229.237; 13.I.229.238; 13.I.229.239;
13.I.229.154; 13.I.229.157; 13.I.229.166; 13.I.229.169;
13.I.229.172; 13.I.229.175; 13.I.229.240; 13.I.229.244;
13.I.230.228; 13.I.230.229; 13.I.230.230; 13.I.230.231;
13.I.230.236; 13.I.230.237; 13.I.230.238; 13.I.230.239;
13.I.230.154; 13.I.230.157; 13.I.230.166; 13.I.230.169;
13.I.230.172; 13.I.230.175; 13.I.230.240; 13.I.230.244;
13.I.231.228; 13.I.231.229; 13.I.231.230; 13.I.231.231;
13.I.231.236; 13.I.231.237; 13.I.231.238; 13.I.231.239;
13.I.231.154; 13.I.231.157; 13.I.231.166; 13.I.231.169;
13.I.231.172; 13.I.231.175; 13.I.231.240; 13.I.231.244;
13.I.236.228; 13.I.236.229; 13.I.236.230; 13.I.236.231;
13.I.236.236; 13.I.236.237; 13.I.236.238; 13.I.236.239;
13.I.236.154; 13.I.236.157; 13.I.236.166; 13.I.236.169;
13.I.236.172; 13.I.236.175; 13.I.236.240; 13.I.236.244;
13.I.237.228; 13.I.237.229; 13.I.237.230; 13.I.237.231;
13.I.237.236; 13.I.237.237; 13.I.237.238; 13.I.237.239;
13.I.237.154; 13.I.237.157; 13.I.237.166; 13.I.237.169;
13.I.237.172; 13.I.237.175; 13.I.237.240; 13.I.237.244;
13.I.238.228; 13.I.238.229; 13.I.238.230; 13.I.238.231;
13.I.238.236; 13.I.238.237; 13.I.238.238; 13.I.238.239;
13.I.238.154; 13.I.238.157; 13.I.238.166; 13.I.238.169;
13.I.238.172; 13.I.238.175; 13.I.238.240; 13.I.238.244;
13.I.239.228; 13.I.239.229; 13.I.239.230; 13.I.239.231;
13.I.239.236; 13.I.239.237; 13.I.239.238; 13.I.239.239;
13.I.239.154; 13.I.239.157; 13.I.239.166; 13.I.239.169;
13.I.239.172; 13.I.239.175; 13.I.239.240; 13.I.239.244;
13.I.154.228; 13.I.154.229; 13.I.154.230; 13.I.154.231;
13.I.154.236; 13.I.154.237; 13.I.154.238; 13.I.154.239;
13.I.154.154; 13.I.154.157; 13.I.154.166; 13.I.154.169;
13.I.154.172; 13.I.154.175; 13.I.154.240; 13.I.154.244;
13.I.157.228; 13.I.157.229; 13.I.157.230; 13.I.157.231;
13.I.157.236; 13.I.157.237; 13.I.157.238; 13.I.157.239;
13.I.157.154; 13.I.157.157; 13.I.157.166; 13.I.157.169;
13.I.157.172; 13.I.157.175; 13.I.157.240; 13.I.157.244;
13.I.166.228; 13.I.166.229; 13.I.166.230; 13.I.166.231;
13.I.166.236; 13.I.166.237; 13.I.166.238; 13.I.166.239;
13.I.166.154; 13.I.166.157; 13.I.166.166; 13.I.166.169;
13.I.166.172; 13.I.166.175; 13.I.166.240; 13.I.166.244;
13.I.169.228; 13.I.169.229; 13.I.169.230; 13.I.169.231;
13.I.169.236; 13.I.169.237; 13.I.169.238; 13.I.169.239;
13.I.169.154; 13.I.169.157; 13.I.169.166; 13.I.169.169;
13.I.169.172; 13.I.169.175; 13.I.169.240; 13.I.169.244;
13.I.172.228; 13.I.172.229; 13.I.172.230; 13.I.172.231;
13.I.172.236; 13.I.172.237; 13.I.172.238; 13.I.172.239;
13.I.172.154; 13.I.172.157; 13.I.172.166; 13.I.172.169;
13.I.172.172; 13.I.172.175; 13.I.172.240; 13.I.172.244;
13.I.175.228; 13.I.175.229; 13.I.175.230; 13.I.175.231;
13.I.175.236; 13.I.175.237; 13.I.175.238; 13.I.175.239;
13.I.175.154; 13.I.175.157; 13.I.175.166; 13.I.175.169;
13.I.175.172; 13.I.175.175; 13.I.175.240; 13.I.175.244;
13.I.240.228; 13.I.240.229; 13.I.240.230; 13.I.240.231;
13.I.240.236; 13.I.240.237; 13.I.240.238; 13.I.240.239;
13.I.240.154; 13.I.240.157; 13.I.240.166; 13.I.240.169;
13.I.240.172; 13.I.240.175; 13.I.240.240; 13.I.240.244;
13.I.244.228; 13.I.244.229; 13.I.244.230; 13.I.244.231;
13.I.244.236; 13.I.244.237; 13.I.244.238; 13.I.244.239;
13.I.244.154; 13.I.244.157; 13.I.244.166; 13.I.244.169;
13.I.244.172; 13.I.244.175; 13.I.244.240; 13.I.244.244; Prodrugs of
13.J 13.J.228.228; 13.J.228.229; 13.J.228.230; 13.J.228.231;
13.J.228.236; 13.J.228.237; 13.J.228.238; 13.J.228.239;
13.J.228.154; 13.J.228.157; 13.J.228.166; 13.J.228.169;
13.J.228.172; 13.J.228.175; 13.J.228.240; 13.J.228.244;
13.J.229.228; 13.J.229.229; 13.J.229.230; 13.J.229.231;
13.J.229.236; 13.J.229.237; 13.J.229.238; 13.J.229.239;
13.J.229.154; 13.J.229.157; 13.J.229.166; 13.J.229.169;
13.J.229.172; 13.J.229.175; 13.J.229.240; 13.J.229.244;
13.J.230.228; 13.J.230.229; 13.J.230.230; 13.J.230.231;
13.J.230.236; 13.J.230.237; 13.J.230.238; 13.J.230.239;
13.J.230.154; 13.J.230.157; 13.J.230.166; 13.J.230.169;
13.J.230.172; 13.J.230.175; 13.J.230.240; 13.J.230.244;
13.J.231.228; 13.J.231.229; 13.J.231.230; 13.J.231.231;
13.J.231.236; 13.J.231.237; 13.J.231.238; 13.J.231.239;
13.J.231.154; 13.J.231.157; 13.J.231.166; 13.J.231.169;
13.J.231.172; 13.J.231.175; 13.J.231.240; 13.J.231.244;
13.J.236.228; 13.J.236.229; 13.J.236.230; 13.J.236.231;
13.J.236.236; 13.J.236.237; 13.J.236.238; 13.J.236.239;
13.J.236.154; 13.J.236.157; 13.J.236.166; 13.J.236.169;
13.J.236.172; 13.J.236.175; 13.J.236.240; 13.J.236.244;
13.J.237.228; 13.J.237.229; 13.J.237.230; 13.J.237.231;
13.J.237.236; 13.J.237.237; 13.J.237.238; 13.J.237.239;
13.J.237.154; 13.J.237.157; 13.J.237.166; 13.J.237.169;
13.J.237.172; 13.J.237.175; 13.J.237.240; 13.J.237.244;
13.J.238.228; 13.J.238.229; 13.J.238.230; 13.J.238.231;
13.J.238.236; 13.J.238.237; 13.J.238.238; 13.J.238.239;
13.J.238.154; 13.J.238.157; 13.J.238.166; 13.J.238.169;
13.J.238.172; 13.J.238.175; 13.J.238.240; 13.J.238.244;
13.J.239.228; 13.J.239.229; 13.J.239.230; 13.J.239.231;
13.J.239.236; 13.J.239.237; 13.J.239.238; 13.J.239.239;
13.J.239.154; 13.J.239.157; 13.J.239.166; 13.J.239.169;
13.J.239.172; 13.J.239.175; 13.J.239.240; 13.J.239.244;
13.J.154.228; 13.J.154.229; 13.J.154.230; 13.J.154.231;
13.J.154.236; 13.J.154.237; 13.J.154.238; 13.J.154.239;
13.J.154.154; 13.J.154.157; 13.J.154.166; 13.J.154.169;
13.J.154.172; 13.J.154.175; 13.J.154.240; 13.J.154.244;
13.J.157.228; 13.J.157.229; 13.J.157.230; 13.J.157.231;
13.J.157.236; 13.J.157.237; 13.J.157.238; 13.J.157.239;
13.J.157.154; 13.J.157.157; 13.J.157.166; 13.J.157.169;
13.J.157.172; 13.J.157.175; 13.J.157.240; 13.J.157.244;
13.J.166.228; 13.J.166.229; 13.J.166.230; 13.J.166.231;
13.J.166.236; 13.J.166.237; 13.J.166.238; 13.J.166.239;
13.J.166.154; 13.J.166.157; 13.J.166.166; 13.J.166.169;
13.J.166.172; 13.J.166.175; 13.J.166.240; 13.J.166.244;
13.J.169.228; 13.J.169.229; 13.J.169.230; 13.J.169.231;
13.J.169.236; 13.J.169.237; 13.J.169.238; 13.J.169.239;
13.J.169.154; 13.J.169.157; 13.J.169.166; 13.J.169.169;
13.J.169.172; 13.J.169.175; 13.J.169.240; 13.J.169.244;
13.J.172.228; 13.J.172.229; 13.J.172.230; 13.J.172.231;
13.J.172.236; 13.J.172.237; 13.J.172.238; 13.J.172.239;
13.J.172.154; 13.J.172.157; 13.J.172.166; 13.J.172.169;
13.J.172.172; 13.J.172.175; 13.J.172.240; 13.J.172.244;
13.J.175.228; 13.J.175.229; 13.J.175.230; 13.J.175.231;
13.J.175.236; 13.J.175.237; 13.J.175.238; 13.J.175.239;
13.J.175.154; 13.J.175.157; 13.J.175.166; 13.J.175.169;
13.J.175.172; 13.J.175.175; 13.J.175.240; 13.J.175.244;
13.J.240.228; 13.J.240.229; 13.J.240.230; 13.J.240.231;
13.J.240.236; 13.J.240.237; 13.J.240.238; 13.J.240.239;
13.J.240.154; 13.J.240.157; 13.J.240.166; 13.J.240.169;
13.J.240.172; 13.J.240.175; 13.J.240.240; 13.J.240.244;
13.J.244.228; 13.J.244.229; 13.J.244.230; 13.J.244.231;
13.J.244.236; 13.J.244.237; 13.J.244.238; 13.J.244.239;
13.J.244.154; 13.J.244.157; 13.J.244.166; 13.J.244.169;
13.J.244.172; 13.J.244.175; 13.J.244.240; 13.J.244.244; Prodrugs of
13.L 13.L.228.228; 13.L.228.229; 13.L.228.230; 13.L.228.231;
13.L.228.236; 13.L.228.237; 13.L.228.238; 13.L.228.239;
13.L.228.154; 13.L.228.157; 13.L.228.166; 13.L.228.169;
13.L.228.172; 13.L.228.175; 13.L.228.240; 13.L.228.244;
13.L.229.228; 13.L.229.229; 13.L.229.230; 13.L.229.231;
13.L.229.236; 13.L.229.237; 13.L.229.238; 13.L.229.239;
13.L.229.154; 13.L.229.157; 13.L.229.166; 13.L.229.169;
13.L.229.172; 13.L.229.175; 13.L.229.240; 13.L.229.244;
13.L.230.228; 13.L.230.229; 13.L.230.230; 13.L.230.231;
13.L.230.236; 13.L.230.237; 13.L.230.238; 13.L.230.239;
13.L.230.154; 13.L.230.157; 13.L.230.166; 13.L.230.169;
13.L.230.172; 13.L.230.175; 13.L.230.240; 13.L.230.244;
13.L.231.228; 13.L.231.229; 13.L.231.230; 13.L.231.231;
13.L.231.236; 13.L.231.237; 13.L.231.238; 13.L.231.239;
13.L.231.154; 13.L.231.157; 13.L.231.166; 13.L.231.169;
13.L.231.172; 13.L.231.175; 13.L.231.240; 13.L.231.244;
13.L.236.228; 13.L.236.229; 13.L.236.230; 13.L.236.231;
13.L.236.236; 13.L.236.237; 13.L.236.238; 13.L.236.239;
13.L.236.154; 13.L.236.157; 13.L.236.166; 13.L.236.169;
13.L.236.172; 13.L.236.175; 13.L.236.240; 13.L.236.244;
13.L.237.228; 13.L.237.229; 13.L.237.230; 13.L.237.231;
13.L.237.236; 13.L.237.237; 13.L.237.238; 13.L.237.239;
13.L.237.154; 13.L.237.157; 13.L.237.166; 13.L.237.169;
13.L.237.172; 13.L.237.175; 13.L.237.240; 13.L.237.244;
13.L.238.228; 13.L.238.229; 13.L.238.230; 13.L.238.231;
13.L.238.236; 13.L.238.237; 13.L.238.238; 13.L.238.239;
13.L.238.154; 13.L.238.157; 13.L.238.166; 13.L.238.169;
13.L.238.172; 13.L.238.175; 13.L.238.240; 13.L.238.244;
13.L.239.228; 13.L.239.229; 13.L.239.230; 13.L.239.231;
13.L.239.236; 13.L.239.237; 13.L.239.238; 13.L.239.239;
13.L.239.154; 13.L.239.157; 13.L.239.166; 13.L.239.169;
13.L.239.172; 13.L.239.175; 13.L.239.240; 13.L.239.244;
13.L.154.228; 13.L.154.229; 13.L.154.230; 13.L.154.231;
13.L.154.236; 13.L.154.237; 13.L.154.238; 13.L.154.239;
13.L.154.154; 13.L.154.157; 13.L.154.166; 13.L.154.169;
13.L.154.172; 13.L.154.175; 13.L.154.240; 13.L.154.244;
13.L.157.228; 13.L.157.229; 13.L.157.230; 13.L.157.231;
13.L.157.236; 13.L.157.237; 13.L.157.238; 13.L.157.239;
13.L.157.154; 13.L.157.157; 13.L.157.166; 13.L.157.169;
13.L.157.172; 13.L.157.175; 13.L.157.240; 13.L.157.244;
13.L.166.228; 13.L.166.229; 13.L.166.230; 13.L.166.231;
13.L.166.236; 13.L.166.237; 13.L.166.238; 13.L.166.239;
13.L.166.154; 13.L.166.157; 13.L.166.166; 13.L.166.169;
13.L.166.172; 13.L.166.175; 13.L.166.240; 13.L.166.244;
13.L.169.228; 13.L.169.229; 13.L.169.230; 13.L.169.231;
13.L.169.236; 13.L.169.237; 13.L.169.238; 13.L.169.239;
13.L.169.154; 13.L.169.157; 13.L.169.166; 13.L.169.169;
13.L.169.172; 13.L.169.175; 13.L.169.240; 13.L.169.244;
13.L.172.228; 13.L.172.229; 13.L.172.230; 13.L.172.231;
13.L.172.236; 13.L.172.237; 13.L.172.238; 13.L.172.239;
13.L.172.154; 13.L.172.157; 13.L.172.166; 13.L.172.169;
13.L.172.172; 13.L.172.175; 13.L.172.240; 13.L.172.244;
13.L.175.228; 13.L.175.229; 13.L.175.230; 13.L.175.231;
13.L.175.236; 13.L.175.237; 13.L.175.238; 13.L.175.239;
13.L.175.154; 13.L.175.157; 13.L.175.166; 13.L.175.169;
13.L.175.172; 13.L.175.175; 13.L.175.240; 13.L.175.244;
13.L.240.228; 13.L.240.229; 13.L.240.230; 13.L.240.231;
13.L.240.236; 13.L.240.237; 13.L.240.238; 13.L.240.239;
13.L.240.154; 13.L.240.157; 13.L.240.166; 13.L.240.169;
13.L.240.172; 13.L.240.175; 13.L.240.240; 13.L.240.244;
13.L.244.228; 13.L.244.229; 13.L.244.230; 13.L.244.231;
13.L.244.236; 13.L.244.237; 13.L.244.238; 13.L.244.239;
13.L.244.154; 13.L.244.157; 13.L.244.166; 13.L.244.169;
13.L.244.172; 13.L.244.175; 13.L.244.240; 13.L.244.244; Prodrugs of
13.O 13.O.228.228; 13.O.228.229; 13.O.228.230; 13.O.228.231;
13.O.228.236; 13.O.228.237; 13.O.228.238; 13.O.228.239;
13.O.228.154; 13.O.228.157; 13.O.228.166; 13.O.228.169;
13.O.228.172; 13.O.228.175; 13.O.228.240; 13.O.228.244;
13.O.229.228; 13.O.229.229; 13.O.229.230; 13.O.229.231;
13.O.229.236; 13.O.229.237; 13.O.229.238; 13.O.229.239;
13.O.229.154; 13.O.229.157; 13.O.229.166; 13.O.229.169;
13.O.229.172; 13.O.229.175; 13.O.229.240; 13.O.229.244;
13.O.230.228; 13.O.230.229; 13.O.230.230; 13.O.230.231;
13.O.230.236; 13.O.230.237; 13.O.230.238; 13.O.230.239;
13.O.230.154; 13.O.230.157; 13.O.230.166; 13.O.230.169;
13.O.230.172; 13.O.230.175; 13.O.230.240; 13.O.230.244;
13.O.231.228; 13.O.231.229; 13.O.231.230; 13.O.231.231;
13.O.231.236; 13.O.231.237; 13.O.231.238; 13.O.231.239;
13.O.231.154; 13.O.231.157; 13.O.231.166; 13.O.231.169;
13.O.231.172; 13.O.231.175; 13.O.231.240; 13.O.231.244;
13.O.236.228; 13.O.236.229; 13.O.236.230; 13.O.236.231;
13.O.236.236; 13.O.236.237; 13.O.236.238; 13.O.236.239;
13.O.236.154; 13.O.236.157; 13.O.236.166; 13.O.236.169;
13.O.236.172; 13.O.236.175; 13.O.236.240; 13.O.236.244;
13.O.237.228; 13.O.237.229; 13.O.237.230; 13.O.237.231;
13.O.237.236; 13.O.237.237; 13.O.237.238; 13.O.237.239;
13.O.237.154; 13.O.237.157; 13.O.237.166; 13.O.237.169;
13.O.237.172; 13.O.237.175; 13.O.237.240; 13.O.237.244;
13.O.238.228; 13.O.238.229; 13.O.238.230; 13.O.238.231;
13.O.238.236; 13.O.238.237; 13.O.238.238; 13.O.238.239;
13.O.238.154; 13.O.238.157; 13.O.238.166; 13.O.238.169;
13.O.238.172; 13.O.238.175; 13.O.238.240; 13.O.238.244;
13.O.239.228; 13.O.239.229; 13.O.239.230; 13.O.239.231;
13.O.239.236; 13.O.239.237; 13.O.239.238; 13.O.239.239;
13.O.239.154; 13.O.239.157; 13.O.239.166; 13.O.239.169;
13.O.239.172; 13.O.239.175; 13.O.239.240; 13.O.239.244;
13.O.154.228; 13.O.154.229; 13.O.154.230; 13.O.154.231;
13.O.154.236; 13.O.154.237; 13.O.154.238; 13.O.154.239;
13.O.154.154; 13.O.154.157; 13.O.154.166; 13.O.154.169;
13.O.154.172; 13.O.154.175; 13.O.154.240; 13.O.154.244;
13.O.157.228; 13.O.157.229; 13.O.157.230; 13.O.157.231;
13.O.157.236; 13.O.157.237; 13.O.157.238; 13.O.157.239;
13.O.157.154; 13.O.157.157; 13.O.157.166; 13.O.157.169;
13.O.157.172; 13.O.157.175; 13.O.157.240; 13.O.157.244;
13.O.166.228; 13.O.166.229; 13.O.166.230; 13.O.166.231;
13.O.166.236; 13.O.166.237; 13.O.166.238; 13.O.166.239;
13.O.166.154; 13.O.166.157; 13.O.166.166; 13.O.166.169;
13.O.166.172; 13.O.166.175; 13.O.166.240; 13.O.166.244;
13.O.169.228; 13.O.169.229; 13.O.169.230; 13.O.169.231;
13.O.169.236; 13.O.169.237; 13.O.169.238; 13.O.169.239;
13.O.169.154; 13.O.169.157; 13.O.169.166; 13.O.169.169;
13.O.169.172; 13.O.169.175; 13.O.169.240; 13.O.169.244;
13.O.172.228; 13.O.172.229; 13.O.172.230; 13.O.172.231;
13.O.172.236; 13.O.172.237; 13.O.172.238; 13.O.172.239;
13.O.172.154; 13.O.172.157; 13.O.172.166; 13.O.172.169;
13.O.172.172; 13.O.172.175; 13.O.172.240; 13.O.172.244;
13.O.175.228; 13.O.175.229; 13.O.175.230; 13.O.175.231;
13.O.175.236; 13.O.175.237; 13.O.175.238; 13.O.175.239;
13.O.175.154; 13.O.175.157; 13.O.175.166; 13.O.175.169;
13.O.175.172; 13.O.175.175; 13.O.175.240; 13.O.175.244;
13.O.240.228; 13.O.240.229; 13.O.240.230; 13.O.240.231;
13.O.240.236; 13.O.240.237; 13.O.240.238; 13.O.240.239;
13.O.240.154; 13.O.240.157; 13.O.240.166; 13.O.240.169;
13.O.240.172; 13.O.240.175; 13.O.240.240; 13.O.240.244;
13.O.244.228; 13.O.244.229; 13.O.244.230; 13.O.244.231;
13.O.244.236; 13.O.244.237; 13.O.244.238; 13.O.244.239;
13.O.244.154; 13.O.244.157; 13.O.244.166; 13.O.244.169;
13.O.244.172; 13.O.244.175; 13.O.244.240; 13.O.244.244; Prodrugs of
13.P 13.P.228.228; 13.P.228.229; 13.P.228.230; 13.P.228.231;
13.P.228.236; 13.P.228.237; 13.P.228.238; 13.P.228.239;
13.P.228.154; 13.P.228.157; 13.P.228.166; 13.P.228.169;
13.P.228.172; 13.P.228.175; 13.P.228.240; 13.P.228.244;
13.P.229.228; 13.P.229.229; 13.P.229.230; 13.P.229.231;
13.P.229.236; 13.P.229.237; 13.P.229.238; 13.P.229.239;
13.P.229.154; 13.P.229.157; 13.P.229.166; 13.P.229.169;
13.P.229.172; 13.P.229.175;
13.P.229.240; 13.P.229.244; 13.P.230.228; 13.P.230.229;
13.P.230.230; 13.P.230.231; 13.P.230.236; 13.P.230.237;
13.P.230.238; 13.P.230.239; 13.P.230.154; 13.P.230.157;
13.P.230.166; 13.P.230.169; 13.P.230.172; 13.P.230.175;
13.P.230.240; 13.P.230.244; 13.P.231.228; 13.P.231.229;
13.P.231.230; 13.P.231.231; 13.P.231.236; 13.P.231.237;
13.P.231.238; 13.P.231.239; 13.P.231.154; 13.P.231.157;
13.P.231.166; 13.P.231.169; 13.P.231.172; 13.P.231.175;
13.P.231.240; 13.P.231.244; 13.P.236.228; 13.P.236.229;
13.P.236.230; 13.P.236.231; 13.P.236.236; 13.P.236.237;
13.P.236.238; 13.P.236.239; 13.P.236.154; 13.P.236.157;
13.P.236.166; 13.P.236.169; 13.P.236.172; 13.P.236.175;
13.P.236.240; 13.P.236.244; 13.P.237.228; 13.P.237.229;
13.P.237.230; 13.P.237.231; 13.P.237.236; 13.P.237.237;
13.P.237.238; 13.P.237.239; 13.P.237.154; 13.P.237.157;
13.P.237.166; 13.P.237.169; 13.P.237.172; 13.P.237.175;
13.P.237.240; 13.P.237.244; 13.P.238.228; 13.P.238.229;
13.P.238.230; 13.P.238.231; 13.P.238.236; 13.P.238.237;
13.P.238.238; 13.P.238.239; 13.P.238.154; 13.P.238.157;
13.P.238.166; 13.P.238.169; 13.P.238.172; 13.P.238.175;
13.P.238.240; 13.P.238.244; 13.P.239.228; 13.P.239.229;
13.P.239.230; 13.P.239.231; 13.P.239.236; 13.P.239.237;
13.P.239.238; 13.P.239.239; 13.P.239.154; 13.P.239.157;
13.P.239.166; 13.P.239.169; 13.P.239.172; 13.P.239.175;
13.P.239.240; 13.P.239.244; 13.P.154.228; 13.P.154.229;
13.P.154.230; 13.P.154.231; 13.P.154.236; 13.P.154.237;
13.P.154.238; 13.P.154.239; 13.P.154.154; 13.P.154.157;
13.P.154.166; 13.P.154.169; 13.P.154.172; 13.P.154.175;
13.P.154.240; 13.P.154.244; 13.P.157.228; 13.P.157.229;
13.P.157.230; 13.P.157.231; 13.P.157.236; 13.P.157.237;
13.P.157.238; 13.P.157.239; 13.P.157.154; 13.P.157.157;
13.P.157.166; 13.P.157.169; 13.P.157.172; 13.P.157.175;
13.P.157.240; 13.P.157.244; 13.P.166.228; 13.P.166.229;
13.P.166.230; 13.P.166.231; 13.P.166.236; 13.P.166.237;
13.P.166.238; 13.P.166.239; 13.P.166.154; 13.P.166.157;
13.P.166.166; 13.P.166.169; 13.P.166.172; 13.P.166.175;
13.P.166.240; 13.P.166.244; 13.P.169.228; 13.P.169.229;
13.P.169.230; 13.P.169.231; 13.P.169.236; 13.P.169.237;
13.P.169.238; 13.P.169.239; 13.P.169.154; 13.P.169.157;
13.P.169.166; 13.P.169.169; 13.P.169.172; 13.P.169.175;
13.P.169.240; 13.P.169.244; 13.P.172.228; 13.P.172.229;
13.P.172.230; 13.P.172.231; 13.P.172.236; 13.P.172.237;
13.P.172.238; 13.P.172.239; 13.P.172.154; 13.P.172.157;
13.P.172.166; 13.P.172.169; 13.P.172.172; 13.P.172.175;
13.P.172.240; 13.P.172.244; 13.P.175.228; 13.P.175.229;
13.P.175.230; 13.P.175.231; 13.P.175.236; 13.P.175.237;
13.P.175.238; 13.P.175.239; 13.P.175.154; 13.P.175.157;
13.P.175.166; 13.P.175.169; 13.P.175.172; 13.P.175.175;
13.P.175.240; 13.P.175.244; 13.P.240.228; 13.P.240.229;
13.P.240.230; 13.P.240.231; 13.P.240.236; 13.P.240.237;
13.P.240.238; 13.P.240.239; 13.P.240.154; 13.P.240.157;
13.P.240.166; 13.P.240.169; 13.P.240.172; 13.P.240.175;
13.P.240.240; 13.P.240.244; 13.P.244.228; 13.P.244.229;
13.P.244.230; 13.P.244.231; 13.P.244.236; 13.P.244.237;
13.P.244.238; 13.P.244.239; 13.P.244.154; 13.P.244.157;
13.P.244.166; 13.P.244.169; 13.P.244.172; 13.P.244.175;
13.P.244.240; 13.P.244.244; Prodrugs of 13.U 13.U.228.228;
13.U.228.229; 13.U.228.230; 13.U.228.231; 13.U.228.236;
13.U.228.237; 13.U.228.238; 13.U.228.239; 13.U.228.154;
13.U.228.157; 13.U.228.166; 13.U.228.169; 13.U.228.172;
13.U.228.175; 13.U.228.240; 13.U.228.244; 13.U.229.228;
13.U.229.229; 13.U.229.230; 13.U.229.231; 13.U.229.236;
13.U.229.237; 13.U.229.238; 13.U.229.239; 13.U.229.154;
13.U.229.157; 13.U.229.166; 13.U.229.169; 13.U.229.172;
13.U.229.175; 13.U.229.240; 13.U.229.244; 13.U.230.228;
13.U.230.229; 13.U.230.230; 13.U.230.231; 13.U.230.236;
13.U.230.237; 13.U.230.238; 13.U.230.239; 13.U.230.154;
13.U.230.157; 13.U.230.166; 13.U.230.169; 13.U.230.172;
13.U.230.175; 13.U.230.240; 13.U.230.244; 13.U.231.228;
13.U.231.229; 13.U.231.230; 13.U.231.231; 13.U.231.236;
13.U.231.237; 13.U.231.238; 13.U.231.239; 13.U.231.154;
13.U.231.157; 13.U.231.166; 13.U.231.169; 13.U.231.172;
13.U.231.175; 13.U.231.240; 13.U.231.244; 13.U.236.228;
13.U.236.229; 13.U.236.230; 13.U.236.231; 13.U.236.236;
13.U.236.237; 13.U.236.238; 13.U.236.239; 13.U.236.154;
13.U.236.157; 13.U.236.166; 13.U.236.169; 13.U.236.172;
13.U.236.175; 13.U.236.240; 13.U.236.244; 13.U.237.228;
13.U.237.229; 13.U.237.230; 13.U.237.231; 13.U.237.236;
13.U.237.237; 13.U.237.238; 13.U.237.239; 13.U.237.154;
13.U.237.157; 13.U.237.166; 13.U.237.169; 13.U.237.172;
13.U.237.175; 13.U.237.240; 13.U.237.244; 13.U.238.228;
13.U.238.229; 13.U.238.230; 13.U.238.231; 13.U.238.236;
13.U.238.237; 13.U.238.238; 13.U.238.239; 13.U.238.154;
13.U.238.157; 13.U.238.166; 13.U.238.169; 13.U.238.172;
13.U.238.175; 13.U.238.240; 13.U.238.244; 13.U.239.228;
13.U.239.229; 13.U.239.230; 13.U.239.231; 13.U.239.236;
13.U.239.237; 13.U.239.238; 13.U.239.239; 13.U.239.154;
13.U.239.157; 13.U.239.166; 13.U.239.169; 13.U.239.172;
13.U.239.175; 13.U.239.240; 13.U.239.244; 13.U.154.228;
13.U.154.229; 13.U.154.230; 13.U.154.231; 13.U.154.236;
13.U.154.237; 13.U.154.238; 13.U.154.239; 13.U.154.154;
13.U.154.157; 13.U.154.166; 13.U.154.169; 13.U.154.172;
13.U.154.175; 13.U.154.240; 13.U.154.244; 13.U.157.228;
13.U.157.229; 13.U.157.230; 13.U.157.231; 13.U.157.236;
13.U.157.237; 13.U.157.238; 13.U.157.239; 13.U.157.154;
13.U.157.157; 13.U.157.166; 13.U.157.169; 13.U.157.172;
13.U.157.175; 13.U.157.240; 13.U.157.244; 13.U.166.228;
13.U.166.229; 13.U.166.230; 13.U.166.231; 13.U.166.236;
13.U.166.237; 13.U.166.238; 13.U.166.239; 13.U.166.154;
13.U.166.157; 13.U.166.166; 13.U.166.169; 13.U.166.172;
13.U.166.175; 13.U.166.240; 13.U.166.244; 13.U.169.228;
13.U.169.229; 13.U.169.230; 13.U.169.231; 13.U.169.236;
13.U.169.237; 13.U.169.238; 13.U.169.239; 13.U.169.154;
13.U.169.157; 13.U.169.166; 13.U.169.169; 13.U.169.172;
13.U.169.175; 13.U.169.240; 13.U.169.244; 13.U.172.228;
13.U.172.229; 13.U.172.230; 13.U.172.231; 13.U.172.236;
13.U.172.237; 13.U.172.238; 13.U.172.239; 13.U.172.154;
13.U.172.157; 13.U.172.166; 13.U.172.169; 13.U.172.172;
13.U.172.175; 13.U.172.240; 13.U.172.244; 13.U.175.228;
13.U.175.229; 13.U.175.230; 13.U.175.231; 13.U.175.236;
13.U.175.237; 13.U.175.238; 13.U.175.239; 13.U.175.154;
13.U.175.157; 13.U.175.166; 13.U.175.169; 13.U.175.172;
13.U.175.175; 13.U.175.240; 13.U.175.244; 13.U.240.228;
13.U.240.229; 13.U.240.230; 13.U.240.231; 13.U.240.236;
13.U.240.237; 13.U.240.238; 13.U.240.239; 13.U.240.154;
13.U.240.157; 13.U.240.166; 13.U.240.169; 13.U.240.172;
13.U.240.175; 13.U.240.240; 13.U.240.244; 13.U.244.228;
13.U.244.229; 13.U.244.230; 13.U.244.231; 13.U.244.236;
13.U.244.237; 13.U.244.238; 13.U.244.239; 13.U.244.154;
13.U.244.157; 13.U.244.166; 13.U.244.169; 13.U.244.172;
13.U.244.175; 13.U.244.240; 13.U.244.244; Prodrugs of 13.W
13.W.228.228; 13.W.228.229; 13.W.228.230; 13.W.228.231;
13.W.228.236; 13.W.228.237; 13.W.228.238; 13.W.228.239;
13.W.228.154; 13.W.228.157; 13.W.228.166; 13.W.228.169;
13.W.228.172; 13.W.228.175; 13.W.228.240; 13.W.228.244;
13.W.229.228; 13.W.229.229; 13.W.229.230; 13.W.229.231;
13.W.229.236; 13.W.229.237; 13.W.229.238; 13.W.229.239;
13.W.229.154; 13.W.229.157; 13.W.229.166; 13.W.229.169;
13.W.229.172; 13.W.229.175; 13.W.229.240; 13.W.229.244;
13.W.230.228; 13.W.230.229; 13.W.230.230; 13.W.230.231;
13.W.230.236; 13.W.230.237; 13.W.230.238; 13.W.230.239;
13.W.230.154; 13.W.230.157; 13.W.230.166; 13.W.230.169;
13.W.230.172; 13.W.230.175; 13.W.230.240; 13.W.230.244;
13.W.231.228; 13.W.231.229; 13.W.231.230; 13.W.231.231;
13.W.231.236; 13.W.231.237; 13.W.231.238; 13.W.231.239;
13.W.231.154; 13.W.231.157; 13.W.231.166; 13.W.231.169;
13.W.231.172; 13.W.231.175; 13.W.231.240; 13.W.231.244;
13.W.236.228; 13.W.236.229; 13.W.236.230; 13.W.236.231;
13.W.236.236; 13.W.236.237; 13.W.236.238; 13.W.236.239;
13.W.236.154; 13.W.236.157; 13.W.236.166; 13.W.236.169;
13.W.236.172; 13.W.236.175; 13.W.236.240; 13.W.236.244;
13.W.237.228; 13.W.237.229; 13.W.237.230; 13.W.237.231;
13.W.237.236; 13.W.237.237; 13.W.237.238; 13.W.237.239;
13.W.237.154; 13.W.237.157; 13.W.237.166; 13.W.237.169;
13.W.237.172; 13.W.237.175; 13.W.237.240; 13.W.237.244;
13.W.238.228; 13.W.238.229; 13.W.238.230; 13.W.238.231;
13.W.238.236; 13.W.238.237; 13.W.238.238; 13.W.238.239;
13.W.238.154; 13.W.238.157; 13.W.238.166; 13.W.238.169;
13.W.238.172; 13.W.238.175; 13.W.238.240; 13.W.238.244;
13.W.239.228; 13.W.239.229; 13.W.239.230; 13.W.239.231;
13.W.239.236; 13.W.239.237; 13.W.239.238; 13.W.239.239;
13.W.239.154; 13.W.239.157; 13.W.239.166; 13.W.239.169;
13.W.239.172; 13.W.239.175; 13.W.239.240; 13.W.239.244;
13.W.154.228; 13.W.154.229; 13.W.154.230; 13.W.154.231;
13.W.154.236; 13.W.154.237; 13.W.154.238; 13.W.154.239;
13.W.154.154; 13.W.154.157; 13.W.154.166; 13.W.154.169;
13.W.154.172; 13.W.154.175; 13.W.154.240; 13.W.154.244;
13.W.157.228; 13.W.157.229; 13.W.157.230; 13.W.157.231;
13.W.157.236; 13.W.157.237; 13.W.157.238; 13.W.157.239;
13.W.157.154; 13.W.157.157; 13.W.157.166; 13.W.157.169;
13.W.157.172; 13.W.157.175; 13.W.157.240; 13.W.157.244;
13.W.166.228; 13.W.166.229; 13.W.166.230; 13.W.166.231;
13.W.166.236; 13.W.166.237; 13.W.166.238; 13.W.166.239;
13.W.166.154; 13.W.166.157; 13.W.166.166; 13.W.166.169;
13.W.166.172; 13.W.166.175; 13.W.166.240; 13.W.166.244;
13.W.169.228; 13.W.169.229; 13.W.169.230; 13.W.169.231;
13.W.169.236; 13.W.169.237; 13.W.169.238; 13.W.169.239;
13.W.169.154; 13.W.169.157; 13.W.169.166; 13.W.169.169;
13.W.169.172; 13.W.169.175; 13.W.169.240; 13.W.169.244;
13.W.172.228; 13.W.172.229; 13.W.172.230; 13.W.172.231;
13.W.172.236; 13.W.172.237; 13.W.172.238; 13.W.172.239;
13.W.172.154; 13.W.172.157; 13.W.172.166; 13.W.172.169;
13.W.172.172; 13.W.172.175; 13.W.172.240; 13.W.172.244;
13.W.175.228; 13.W.175.229; 13.W.175.230; 13.W.175.231;
13.W.175.236; 13.W.175.237; 13.W.175.238; 13.W.175.239;
13.W.175.154; 13.W.175.157; 13.W.175.166; 13.W.175.169;
13.W.175.172; 13.W.175.175; 13.W.175.240; 13.W.175.244;
13.W.240.228; 13.W.240.229; 13.W.240.230; 13.W.240.231;
13.W.240.236; 13.W.240.237; 13.W.240.238; 13.W.240.239;
13.W.240.154; 13.W.240.157; 13.W.240.166; 13.W.240.169;
13.W.240.172; 13.W.240.175; 13.W.240.240; 13.W.240.244;
13.W.244.228; 13.W.244.229; 13.W.244.230; 13.W.244.231;
13.W.244.236; 13.W.244.237; 13.W.244.238; 13.W.244.239;
13.W.244.154; 13.W.244.157; 13.W.244.166; 13.W.244.169;
13.W.244.172; 13.W.244.175; 13.W.244.240; 13.W.244.244; Prodrugs of
13.Y 13.Y.228.228; 13.Y.228.229; 13.Y.228.230; 13.Y.228.231;
13.Y.228.236; 13.Y.228.237; 13.Y.228.238; 13.Y.228.239;
13.Y.228.154; 13.Y.228.157; 13.Y.228.166; 13.Y.228.169;
13.Y.228.172; 13.Y.228.175; 13.Y.228.240; 13.Y.228.244;
13.Y.229.228; 13.Y.229.229; 13.Y.229.230; 13.Y.229.231;
13.Y.229.236; 13.Y.229.237; 13.Y.229.238; 13.Y.229.239;
13.Y.229.154; 13.Y.229.157; 13.Y.229.166; 13.Y.229.169;
13.Y.229.172; 13.Y.229.175; 13.Y.229.240; 13.Y.229.244;
13.Y.230.228; 13.Y.230.229; 13.Y.230.230; 13.Y.230.231;
13.Y.230.236; 13.Y.230.237; 13.Y.230.238; 13.Y.230.239;
13.Y.230.154; 13.Y.230.157; 13.Y.230.166; 13.Y.230.169;
13.Y.230.172; 13.Y.230.175; 13.Y.230.240; 13.Y.230.244;
13.Y.231.228; 13.Y.231.229; 13.Y.231.230; 13.Y.231.231;
13.Y.231.236; 13.Y.231.237; 13.Y.231.238; 13.Y.231.239;
13.Y.231.154; 13.Y.231.157; 13.Y.231.166; 13.Y.231.169;
13.Y.231.172; 13.Y.231.175; 13.Y.231.240; 13.Y.231.244;
13.Y.236.228; 13.Y.236.229; 13.Y.236.230; 13.Y.236.231;
13.Y.236.236; 13.Y.236.237; 13.Y.236.238; 13.Y.236.239;
13.Y.236.154; 13.Y.236.157; 13.Y.236.166; 13.Y.236.169;
13.Y.236.172; 13.Y.236.175; 13.Y.236.240; 13.Y.236.244;
13.Y.237.228; 13.Y.237.229; 13.Y.237.230; 13.Y.237.231;
13.Y.237.236; 13.Y.237.237; 13.Y.237.238; 13.Y.237.239;
13.Y.237.154; 13.Y.237.157; 13.Y.237.166; 13.Y.237.169;
13.Y.237.172; 13.Y.237.175; 13.Y.237.240; 13.Y.237.244;
13.Y.238.228; 13.Y.238.229; 13.Y.238.230; 13.Y.238.231;
13.Y.238.236; 13.Y.238.237; 13.Y.238.238; 13.Y.238.239;
13.Y.238.154; 13.Y.238.157; 13.Y.238.166; 13.Y.238.169;
13.Y.238.172; 13.Y.238.175; 13.Y.238.240; 13.Y.238.244;
13.Y.239.228; 13.Y.239.229; 13.Y.239.230; 13.Y.239.231;
13.Y.239.236; 13.Y.239.237; 13.Y.239.238; 13.Y.239.239;
13.Y.239.154; 13.Y.239.157; 13.Y.239.166; 13.Y.239.169;
13.Y.239.172; 13.Y.239.175; 13.Y.239.240; 13.Y.239.244;
13.Y.154.228; 13.Y.154.229; 13.Y.154.230; 13.Y.154.231;
13.Y.154.236; 13.Y.154.237; 13.Y.154.238; 13.Y.154.239;
13.Y.154.154; 13.Y.154.157; 13.Y.154.166; 13.Y.154.169;
13.Y.154.172; 13.Y.154.175; 13.Y.154.240; 13.Y.154.244;
13.Y.157.228; 13.Y.157.229; 13.Y.157.230; 13.Y.157.231;
13.Y.157.236; 13.Y.157.237; 13.Y.157.238; 13.Y.157.239;
13.Y.157.154; 13.Y.157.157; 13.Y.157.166; 13.Y.157.169;
13.Y.157.172; 13.Y.157.175; 13.Y.157.240; 13.Y.157.244;
13.Y.166.228; 13.Y.166.229; 13.Y.166.230; 13.Y.166.231;
13.Y.166.236; 13.Y.166.237; 13.Y.166.238; 13.Y.166.239;
13.Y.166.154; 13.Y.166.157; 13.Y.166.166; 13.Y.166.169;
13.Y.166.172; 13.Y.166.175; 13.Y.166.240; 13.Y.166.244;
13.Y.169.228; 13.Y.169.229; 13.Y.169.230; 13.Y.169.231;
13.Y.169.236; 13.Y.169.237; 13.Y.169.238; 13.Y.169.239;
13.Y.169.154; 13.Y.169.157; 13.Y.169.166; 13.Y.169.169;
13.Y.169.172; 13.Y.169.175; 13.Y.169.240; 13.Y.169.244;
13.Y.172.228; 13.Y.172.229; 13.Y.172.230; 13.Y.172.231;
13.Y.172.236; 13.Y.172.237; 13.Y.172.238; 13.Y.172.239;
13.Y.172.154; 13.Y.172.157; 13.Y.172.166; 13.Y.172.169;
13.Y.172.172; 13.Y.172.175; 13.Y.172.240; 13.Y.172.244;
13.Y.175.228; 13.Y.175.229; 13.Y.175.230; 13.Y.175.231;
13.Y.175.236; 13.Y.175.237; 13.Y.175.238; 13.Y.175.239;
13.Y.175.154; 13.Y.175.157; 13.Y.175.166; 13.Y.175.169;
13.Y.175.172; 13.Y.175.175; 13.Y.175.240; 13.Y.175.244;
13.Y.240.228; 13.Y.240.229; 13.Y.240.230; 13.Y.240.231;
13.Y.240.236; 13.Y.240.237; 13.Y.240.238; 13.Y.240.239;
13.Y.240.154; 13.Y.240.157; 13.Y.240.166; 13.Y.240.169;
13.Y.240.172; 13.Y.240.175; 13.Y.240.240; 13.Y.240.244;
13.Y.244.228; 13.Y.244.229; 13.Y.244.230; 13.Y.244.231;
13.Y.244.236; 13.Y.244.237; 13.Y.244.238; 13.Y.244.239;
13.Y.244.154; 13.Y.244.157; 13.Y.244.166; 13.Y.244.169;
13.Y.244.172; 13.Y.244.175; 13.Y.244.240; 13.Y.244.244; Prodrugs of
14.AH 14.AH.4.157; 14.AH.4.158; 14.AH.4.196; 14.AH.4.223;
14.AH.4.240; 14.AH.4.244; 14.AH.4.243; 14.AH.4.247; 14.AH.5.157;
14.AH.5.158; 14.AH.5.196; 14.AH.5.223; 14.AH.5.240; 14.AH.5.244;
14.AH.5.243; 14.AH.5.247; 14.AH.7.157; 14.AH.7.158; 14.AH.7.196;
14.AH.7.223; 14.AH.7.240; 14.AH.7.244; 14.AH.7.243; 14.AH.7.247;
14.AH.15.157; 14.AH.15.158; 14.AH.15.196; 14.AH.15.223;
14.AH.15.240; 14.AH.15.244; 14.AH.15.243; 14.AH.15.247;
14.AH.16.157; 14.AH.16.158; 14.AH.16.196; 14.AH.16.223;
14.AH.16.240; 14.AH.16.244; 14.AH.16.243; 14.AH.16.247;
14.AH.18.157; 14.AH.18.158; 14.AH.18.196; 14.AH.18.223;
14.AH.18.240; 14.AH.18.244; 14.AH.18.243; 14.AH.18.247;
14.AH.26.157; 14.AH.26.158; 14.AH.26.196; 14.AH.26.223;
14.AH.26.240; 14.AH.26.244; 14.AH.26.243; 14.AH.26.247;
14.AH.27.157; 14.AH.27.158; 14.AH.27.196; 14.AH.27.223;
14.AH.27.240; 14.AH.27.244; 14.AH.27.243; 14.AH.27.247;
14.AH.29.157; 14.AH.29.158; 14.AH.29.196; 14.AH.29.223;
14.AH.29.240; 14.AH.29.244; 14.AH.29.243; 14.AH.29.247;
14.AH.54.157; 14.AH.54.158; 14.AH.54.196; 14.AH.54.223;
14.AH.54.240; 14.AH.54.244; 14.AH.54.243; 14.AH.54.247;
14.AH.55.157; 14.AH.55.158; 14.AH.55.196; 14.AH.55.223;
14.AH.55.240; 14.AH.55.244; 14.AH.55.243; 14.AH.55.247;
14.AH.56.157; 14.AH.56.158; 14.AH.56.196; 14.AH.56.223;
14.AH.56.240; 14.AH.56.244; 14.AH.56.243; 14.AH.56.247;
14.AH.157.157; 14.AH.157.158; 14.AH.157.196; 14.AH.157.223;
14.AH.157.240; 14.AH.157.244; 14.AH.157.243; 14.AH.157.247;
14.AH.196.157; 14.AH.196.158; 14.AH.196.196; 14.AH.196.223;
14.AH.196.240; 14.AH.196.244; 14.AH.196.243; 14.AH.196.247;
14.AH.223.157; 14.AH.223.158; 14.AH.223.196; 14.AH.223.223;
14.AH.223.240; 14.AH.223.244; 14.AH.223.243; 14.AH.223.247;
14.AH.240.157; 14.AH.240.158; 14.AH.240.196; 14.AH.240.223;
14.AH.240.240; 14.AH.240.244; 14.AH.240.243; 14.AH.240.247;
14.AH.244.157; 14.AH.244.158; 14.AH.244.196; 14.AH.244.223;
14.AH.244.240; 14.AH.244.244; 14.AH.244.243; 14.AH.244.247;
14.AH.247.157; 14.AH.247.158; 14.AH.247.196; 14.AH.247.223;
14.AH.247.240; 14.AH.247.244; 14.AH.247.243; 14.AH.247.247;
Prodrugs of 14.AJ 14.AJ.4.157; 14.AJ.4.158; 14.AJ.4.196;
14.AJ.4.223; 14.AJ.4.240; 14.AJ.4.244; 14.AJ.4.243; 14.AJ.4.247;
14.AJ.5.157; 14.AJ.5.158; 14.AJ.5.196; 14.AJ.5.223; 14.AJ.5.240;
14.AJ.5.244; 14.AJ.5.243; 14.AJ.5.247; 14.AJ.7.157; 14.AJ.7.158;
14.AJ.7.196; 14.AJ.7.223; 14.AJ.7.240; 14.AJ.7.244; 14.AJ.7.243;
14.AJ.7.247; 14.AJ.15.157; 14.AJ.15.158; 14.AJ.15.196;
14.AJ.15.223; 14.AJ.15.240; 14.AJ.15.244;
14.AJ.15.243; 14.AJ.15.247; 14.AJ.16.157; 14.AJ.16.158;
14.AJ.16.196; 14.AJ.16.223; 14.AJ.16.240; 14.AJ.16.244;
14.AJ.16.243; 14.AJ.16.247; 14.AJ.18.157; 14.AJ.18.158;
14.AJ.18.196; 14.AJ.18.223; 14.AJ.18.240; 14.AJ.18.244;
14.AJ.18.243; 14.AJ.18.247; 14.AJ.26.157; 14.AJ.26.158;
14.AJ.26.196; 14.AJ.26.223; 14.AJ.26.240; 14.AJ.26.244;
14.AJ.26.243; 14.AJ.26.247; 14.AJ.27.157; 14.AJ.27.158;
14.AJ.27.196; 14.AJ.27.223; 14.AJ.27.240; 14.AJ.27.244;
14.AJ.27.243; 14.AJ.27.247; 14.AJ.29.157; 14.AJ.29.158;
14.AJ.29.196; 14.AJ.29.223; 14.AJ.29.240; 14.AJ.29.244;
14.AJ.29.243; 14.AJ.29.247; 14.AJ.54.157; 14.AJ.54.158;
14.AJ.54.196; 14.AJ.54.223; 14.AJ.54.240; 14.AJ.54.244;
14.AJ.54.243; 14.AJ.54.247; 14.AJ.55.157; 14.AJ.55.158;
14.AJ.55.196; 14.AJ.55.223; 14.AJ.55.240; 14.AJ.55.244;
14.AJ.55.243; 14.AJ.55.247; 14.AJ.56.157; 14.AJ.56.158;
14.AJ.56.196; 14.AJ.56.223; 14.AJ.56.240; 14.AJ.56.244;
14.AJ.56.243; 14.AJ.56.247; 14.AJ.157.157; 14.AJ.157.158;
14.AJ.157.196; 14.AJ.157.223; 14.AJ.157.240; 14.AJ.157.244;
14.AJ.157.243; 14.AJ.157.247; 14.AJ.196.157; 14.AJ.196.158;
14.AJ.196.196; 14.AJ.196.223; 14.AJ.196.240; 14.AJ.196.244;
14.AJ.196.243; 14.AJ.196.247; 14.AJ.223.157; 14.AJ.223.158;
14.AJ.223.196; 14.AJ.223.223; 14.AJ.223.240; 14.AJ.223.244;
14.AJ.223.243; 14.AJ.223.247; 14.AJ.240.157; 14.AJ.240.158;
14.AJ.240.196; 14.AJ.240.223; 14.AJ.240.240; 14.AJ.240.244;
14.AJ.240.243; 14.AJ.240.247; 14.AJ.244.157; 14.AJ.244.158;
14.AJ.244.196; 14.AJ.244.223; 14.AJ.244.240; 14.AJ.244.244;
14.AJ.244.243; 14.AJ.244.247; 14.AJ.247.157; 14.AJ.247.158;
14.AJ.247.196; 14.AJ.247.223; 14.AJ.247.240; 14.AJ.247.244;
14.AJ.247.243; 14.AJ.247.247; Prodrugs of 14.AN 14.AN.4.157;
14.AN.4.158; 14.AN.4.196; 14.AN.4.223; 14.AN.4.240; 14.AN.4.244;
14.AN.4.243; 14.AN.4.247; 14.AN.5.157; 14.AN.5.158; 14.AN.5.196;
14.AN.5.223; 14.AN.5.240; 14.AN.5.244; 14.AN.5.243; 14.AN.5.247;
14.AN.7.157; 14.AN.7.158; 14.AN.7.196; 14.AN.7.223; 14.AN.7.240;
14.AN.7.244; 14.AN.7.243; 14.AN.7.247; 14.AN.15.157; 14.AN.15.158;
14.AN.15.196; 14.AN.15.223; 14.AN.15.240; 14.AN.15.244;
14.AN.15.243; 14.AN.15.247; 14.AN.16.157; 14.AN.16.158;
14.AN.16.196; 14.AN.16.223; 14.AN.16.240; 14.AN.16.244;
14.AN.16.243; 14.AN.16.247; 14.AN.18.157; 14.AN.18.158;
14.AN.18.196; 14.AN.18.223; 14.AN.18.240; 14.AN.18.244;
14.AN.18.243; 14.AN.18.247; 14.AN.26.157; 14.AN.26.158;
14.AN.26.196; 14.AN.26.223; 14.AN.26.240; 14.AN.26.244;
14.AN.26.243; 14.AN.26.247; 14.AN.27.157; 14.AN.27.158;
14.AN.27.196; 14.AN.27.223; 14.AN.27.240; 14.AN.27.244;
14.AN.27.243; 14.AN.27.247; 14.AN.29.157; 14.AN.29.158;
14.AN.29.196; 14.AN.29.223; 14.AN.29.240; 14.AN.29.244;
14.AN.29.243; 14.AN.29.247; 14.AN.54.157; 14.AN.54.158;
14.AN.54.196; 14.AN.54.223; 14.AN.54.240; 14.AN.54.244;
14.AN.54.243; 14.AN.54.247; 14.AN.55.157; 14.AN.55.158;
14.AN.55.196; 14.AN.55.223; 14.AN.55.240; 14.AN.55.244;
14.AN.55.243; 14.AN.55.247; 14.AN.56.157; 14.AN.56.158;
14.AN.56.196; 14.AN.56.223; 14.AN.56.240; 14.AN.56.244;
14.AN.56.243; 14.AN.56.247; 14.AN.157.157; 14.AN.157.158;
14.AN.157.196; 14.AN.157.223; 14.AN.157.240; 14.AN.157.244;
14.AN.157.243; 14.AN.157.247; 14.AN.196.157; 14.AN.196.158;
14.AN.196.196; 14.AN.196.223; 14.AN.196.240; 14.AN.196.244;
14.AN.196.243; 14.AN.196.247; 14.AN.223.157; 14.AN.223.158;
14.AN.223.196; 14.AN.223.223; 14.AN.223.240; 14.AN.223.244;
14.AN.223.243; 14.AN.223.247; 14.AN.240.157; 14.AN.240.158;
14.AN.240.196; 14.AN.240.223; 14.AN.240.240; 14.AN.240.244;
14.AN.240.243; 14.AN.240.247; 14.AN.244.157; 14.AN.244.158;
14.AN.244.196; 14.AN.244.223; 14.AN.244.240; 14.AN.244.244;
14.AN.244.243; 14.AN.244.247; 14.AN.247.157; 14.AN.247.158;
14.AN.247.196; 14.AN.247.223; 14.AN.247.240; 14.AN.247.244;
14.AN.247.243; 14.AN.247.247; Prodrugs of 14.AP 14.AP.4.157;
14.AP.4.158; 14.AP.4.196; 14.AP.4.223; 14.AP.4.240; 14.AP.4.244;
14.AP.4.243; 14.AP.4.247; 14.AP.5.157; 14.AP.5.158; 14.AP.5.196;
14.AP.5.223; 14.AP.5.240; 14.AP.5.244; 14.AP.5.243; 14.AP.5.247;
14.AP.7.157; 14.AP.7.158; 14.AP.7.196; 14.AP.7.223; 14.AP.7.240;
14.AP.7.244; 14.AP.7.243; 14.AP.7.247; 14.AP.15.157; 14.AP.15.158;
14.AP.15.196; 14.AP.15.223; 14.AP.15.240; 14.AP.15.244;
14.AP.15.243; 14.AP.15.247; 14.AP.16.157; 14.AP.16.158;
14.AP.16.196; 14.AP.16.223; 14.AP.16.240; 14.AP.16.244;
14.AP.16.243; 14.AP.16.247; 14.AP.18.157; 14.AP.18.158;
14.AP.18.196; 14.AP.18.223; 14.AP.18.240; 14.AP.18.244;
14.AP.18.243; 14.AP.18.247; 14.AP.26.157; 14.AP.26.158;
14.AP.26.196; 14.AP.26.223; 14.AP.26.240; 14.AP.26.244;
14.AP.26.243; 14.AP.26.247; 14.AP.27.157; 14.AP.27.158;
14.AP.27.196; 14.AP.27.223; 14.AP.27.240; 14.AP.27.244;
14.AP.27.243; 14.AP.27.247; 14.AP.29.157; 14.AP.29.158;
14.AP.29.196; 14.AP.29.223; 14.AP.29.240; 14.AP.29.244;
14.AP.29.243; 14.AP.29.247; 14.AP.54.157; 14.AP.54.158;
14.AP.54.196; 14.AP.54.223; 14.AP.54.240; 14.AP.54.244;
14.AP.54.243; 14.AP.54.247; 14.AP.55.157; 14.AP.55.158;
14.AP.55.196; 14.AP.55.223; 14.AP.55.240; 14.AP.55.244;
14.AP.55.243; 14.AP.55.247; 14.AP.56.157; 14.AP.56.158;
14.AP.56.196; 14.AP.56.223; 14.AP.56.240; 14.AP.56.244;
14.AP.56.243; 14.AP.56.247; 14.AP.157.157; 14.AP.157.158;
14.AP.157.196; 14.AP.157.223; 14.AP.157.240; 14.AP.157.244;
14.AP.157.243; 14.AP.157.247; 14.AP.196.157; 14.AP.196.158;
14.AP.196.196; 14.AP.196.223; 14.AP.196.240; 14.AP.196.244;
14.AP.196.243; 14.AP.196.247; 14.AP.223.157; 14.AP.223.158;
14.AP.223.196; 14.AP.223.223; 14.AP.223.240; 14.AP.223.244;
14.AP.223.243; 14.AP.223.247; 14.AP.240.157; 14.AP.240.158;
14.AP.240.196; 14.AP.240.223; 14.AP.240.240; 14.AP.240.244;
14.AP.240.243; 14.AP.240.247; 14.AP.244.157; 14.AP.244.158;
14.AP.244.196; 14.AP.244.223; 14.AP.244.240; 14.AP.244.244;
14.AP.244.243; 14.AP.244.247; 14.AP.247.157; 14.AP.247.158;
14.AP.247.196; 14.AP.247.223; 14.AP.247.240; 14.AP.247.244;
14.AP.247.243; 14.AP.247.247; Prodrugs of 14.AZ 14.AZ.4.157;
14.AZ.4.158; 14.AZ.4.196; 14.AZ.4.223; 14.AZ.4.240; 14.AZ.4.244;
14.AZ.4.243; 14.AZ.4.247; 14.AZ.5.157; 14.AZ.5.158; 14.AZ.5.196;
14.AZ.5.223; 14.AZ.5.240; 14.AZ.5.244; 14.AZ.5.243; 14.AZ.5.247;
14.AZ.7.157; 14.AZ.7.158; 14.AZ.7.196; 14.AZ.7.223; 14.AZ.7.240;
14.AZ.7.244; 14.AZ.7.243; 14.AZ.7.247; 14.AZ.15.157; 14.AZ.15.158;
14.AZ.15.196; 14.AZ.15.223; 14.AZ.15.240; 14.AZ.15.244;
14.AZ.15.243; 14.AZ.15.247; 14.AZ.16.157; 14.AZ.16.158;
14.AZ.16.196; 14.AZ.16.223; 14.AZ.16.240; 14.AZ.16.244;
14.AZ.16.243; 14.AZ.16.247; 14.AZ.18.157; 14.AZ.18.158;
14.AZ.18.196; 14.AZ.18.223; 14.AZ.18.240; 14.AZ.18.244;
14.AZ.18.243; 14.AZ.18.247; 14.AZ.26.157; 14.AZ.26.158;
14.AZ.26.196; 14.AZ.26.223; 14.AZ.26.240; 14.AZ.26.244;
14.AZ.26.243; 14.AZ.26.247; 14.AZ.27.157; 14.AZ.27.158;
14.AZ.27.196; 14.AZ.27.223; 14.AZ.27.240; 14.AZ.27.244;
14.AZ.27.243; 14.AZ.27.247; 14.AZ.29.157; 14.AZ.29.158;
14.AZ.29.196; 14.AZ.29.223; 14.AZ.29.240; 14.AZ.29.244;
14.AZ.29.243; 14.AZ.29.247; 14.AZ.54.157; 14.AZ.54.158;
14.AZ.54.196; 14.AZ.54.223; 14.AZ.54.240; 14.AZ.54.244;
14.AZ.54.243; 14.AZ.54.247; 14.AZ.55.157; 14.AZ.55.158;
14.AZ.55.196; 14.AZ.55.223; 14.AZ.55.240; 14.AZ.55.244;
14.AZ.55.243; 14.AZ.55.247; 14.AZ.56.157; 14.AZ.56.158;
14.AZ.56.196; 14.AZ.56.223; 14.AZ.56.240; 14.AZ.56.244;
14.AZ.56.243; 14.AZ.56.247; 14.AZ.157.157; 14.AZ.157.158;
14.AZ.157.196; 14.AZ.157.223; 14.AZ.157.240; 14.AZ.157.244;
14.AZ.157.243; 14.AZ.157.247; 14.AZ.196.157; 14.AZ.196.158;
14.AZ.196.196; 14.AZ.196.223; 14.AZ.196.240; 14.AZ.196.244;
14.AZ.196.243; 14.AZ.196.247; 14.AZ.223.157; 14.AZ.223.158;
14.AZ.223.196; 14.AZ.223.223; 14.AZ.223.240; 14.AZ.223.244;
14.AZ.223.243; 14.AZ.223.247; 14.AZ.240.157; 14.AZ.240.158;
14.AZ.240.196; 14.AZ.240.223; 14.AZ.240.240; 14.AZ.240.244;
14.AZ.240.243; 14.AZ.240.247; 14.AZ.244.157; 14.AZ.244.158;
14.AZ.244.196; 14.AZ.244.223; 14.AZ.244.240; 14.AZ.244.244;
14.AZ.244.243; 14.AZ.244.247; 14.AZ.247.157; 14.AZ.247.158;
14.AZ.247.196; 14.AZ.247.223; 14.AZ.247.240; 14.AZ.247.244;
14.AZ.247.243; 14.AZ.247.247; Prodrugs of 14.BF 14.BF.4.157;
14.BF.4.158; 14.BF.4.196; 14.BF.4.223; 14.BF.4.240; 14.BF.4.244;
14.BF.4.243; 14.BF.4.247; 14.BF.5.157; 14.BF.5.158; 14.BF.5.196;
14.BF.5.223; 14.BF.5.240; 14.BF.5.244; 14.BF.5.243; 14.BF.5.247;
14.BF.7.157; 14.BF.7.158; 14.BF.7.196; 14.BF.7.223; 14.BF.7.240;
14.BF.7.244; 14.BF.7.243; 14.BF.7.247; 14.BF.15.157; 14.BF.15.158;
14.BF.15.196; 14.BF.15.223; 14.BF.15.240; 14.BF.15.244;
14.BF.15.243; 14.BF.15.247; 14.BF.16.157; 14.BF.16.158;
14.BF.16.196; 14.BF.16.223; 14.BF.16.240; 14.BF.16.244;
14.BF.16.243; 14.BF.16.247; 14.BF.18.157; 14.BF.18.158;
14.BF.18.196; 14.BF.18.223; 14.BF.18.240; 14.BF.18.244;
14.BF.18.243; 14.BF.18.247; 14.BF.26.157; 14.BF.26.158;
14.BF.26.196; 14.BF.26.223; 14.BF.26.240; 14.BF.26.244;
14.BF.26.243; 14.BF.26.247; 14.BF.27.157; 14.BF.27.158;
14.BF.27.196; 14.BF.27.223; 14.BF.27.240; 14.BF.27.244;
14.BF.27.243; 14.BF.27.247; 14.BF.29.157; 14.BF.29.158;
14.BF.29.196; 14.BF.29.223; 14.BF.29.240; 14.BF.29.244;
14.BF.29.243; 14.BF.29.247; 14.BF.54.157; 14.BF.54.158;
14.BF.54.196; 14.BF.54.223; 14.BF.54.240; 14.BF.54.244;
14.BF.54.243; 14.BF.54.247; 14.BF.55.157; 14.BF.55.158;
14.BF.55.196; 14.BF.55.223; 14.BF.55.240; 14.BF.55.244;
14.BF.55.243; 14.BF.55.247; 14.BF.56.157; 14.BF.56.158;
14.BF.56.196; 14.BF.56.223; 14.BF.56.240; 14.BF.56.244;
14.BF.56.243; 14.BF.56.247; 14.BF.157.157; 14.BF.157.158;
14.BF.157.196; 14.BF.157.223; 14.BF.157.240; 14.BF.157.244;
14.BF.157.243; 14.BF.157.247; 14.BF.196.157; 14.BF.196.158;
14.BF.196.196; 14.BF.196.223; 14.BF.196.240; 14.BF.196.244;
14.BF.196.243; 14.BF.196.247; 14.BF.223.157; 14.BF.223.158;
14.BF.223.196; 14.BF.223.223; 14.BF.223.240; 14.BF.223.244;
14.BF.223.243; 14.BF.223.247; 14.BF.240.157; 14.BF.240.158;
14.BF.240.196; 14.BF.240.223; 14.BF.240.240; 14.BF.240.244;
14.BF.240.243; 14.BF.240.247; 14.BF.244.157; 14.BF.244.158;
14.BF.244.196; 14.BF.244.223; 14.BF.244.240; 14.BF.244.244;
14.BF.244.243; 14.BF.244.247; 14.BF.247.157; 14.BF.247.158;
14.BF.247.196; 14.BF.247.223; 14.BF.247.240; 14.BF.247.244;
14.BF.247.243; 14.BF.247.247; Prodrugs of 14.CI 14.CI.4.157;
14.CI.4.158; 14.CI.4.196; 14.CI.4.223; 14.CI.4.240; 14.CI.4.244;
14.CI.4.243; 14.CI.4.247; 14.CI.5.157; 14.CI.5.158; 14.CI.5.196;
14.CI.5.223; 14.CI.5.240; 14.CI.5.244; 14.CI.5.243; 14.CI.5.247;
14.CI.7.157; 14.CI.7.158; 14.CI.7.196; 14.CI.7.223; 14.CI.7.240;
14.CI.7.244; 14.CI.7.243; 14.CI.7.247; 14.CI.15.157; 14.CI.15.158;
14.CI.15.196; 14.CI.15.223; 14.CI.15.240; 14.CI.15.244;
14.CI.15.243; 14.CI.15.247; 14.CI.16.157; 14.CI.16.158;
14.CI.16.196; 14.CI.16.223; 14.CI.16.240; 14.CI.16.244;
14.CI.16.243; 14.CI.16.247; 14.CI.18.157; 14.CI.18.158;
14.CI.18.196; 14.CI.18.223; 14.CI.18.240; 14.CI.18.244;
14.CI.18.243; 14.CI.18.247; 14.CI.26.157; 14.CI.26.158;
14.CI.26.196; 14.CI.26.223; 14.CI.26.240; 14.CI.26.244;
14.CI.26.243; 14.CI.26.247; 14.CI.27.157; 14.CI.27.158;
14.CI.27.196; 14.CI.27.223; 14.CI.27.240; 14.CI.27.244;
14.CI.27.243; 14.CI.27.247; 14.CI.29.157; 14.CI.29.158;
14.CI.29.196; 14.CI.29.223; 14.CI.29.240; 14.CI.29.244;
14.CI.29.243; 14.CI.29.247; 14.CI.54.157; 14.CI.54.158;
14.CI.54.196; 14.CI.54.223; 14.CI.54.240; 14.CI.54.244;
14.CI.54.243; 14.CI.54.247; 14.CI.55.157; 14.CI.55.158;
14.CI.55.196; 14.CI.55.223; 14.CI.55.240; 14.CI.55.244;
14.CI.55.243; 14.CI.55.247; 14.CI.56.157; 14.CI.56.158;
14.CI.56.196; 14.CI.56.223; 14.CI.56.240; 14.CI.56.244;
14.CI.56.243; 14.CI.56.247; 14.CI.157.157; 14.CI.157.158;
14.CI.157.196; 14.CI.157.223; 14.CI.157.240; 14.CI.157.244;
14.CI.157.243; 14.CI.157.247; 14.CI.196.157; 14.CI.196.158;
14.CI.196.196; 14.CI.196.223; 14.CI.196.240; 14.CI.196.244;
14.CI.196.243; 14.CI.196.247; 14.CI.223.157; 14.CI.223.158;
14.CI.223.196; 14.CI.223.223; 14.CI.223.240; 14.CI.223.244;
14.CI.223.243; 14.CI.223.247; 14.CI.240.157; 14.CI.240.158;
14.CI.240.196; 14.CI.240.223; 14.CI.240.240; 14.CI.240.244;
14.CI.240.243; 14.CI.240.247; 14.CI.244.157; 14.CI.244.158;
14.CI.244.196; 14.CI.244.223; 14.CI.244.240; 14.CI.244.244;
14.CI.244.243; 14.CI.244.247; 14.CI.247.157; 14.CI.247.158;
14.CI.247.196; 14.CI.247.223; 14.CI.247.240; 14.CI.247.244;
14.CI.247.243; 14.CI.247.247; Prodrugs of 14.CO 14.CO.4.157;
14.CO.4.158; 14.CO.4.196; 14.CO.4.223; 14.CO.4.240; 14.CO.4.244;
14.CO.4.243; 14.CO.4.247; 14.CO.5.157; 14.CO.5.158; 14.CO.5.196;
14.CO.5.223; 14.CO.5.240; 14.CO.5.244; 14.CO.5.243; 14.CO.5.247;
14.CO.7.157; 14.CO.7.158; 14.CO.7.196; 14.CO.7.223; 14.CO.7.240;
14.CO.7.244; 14.CO.7.243; 14.CO.7.247; 14.CO.15.157; 14.CO.15.158;
14.CO.15.196; 14.CO.15.223; 14.CO.15.240; 14.CO.15.244;
14.CO.15.243; 14.CO.15.247; 14.CO.16.157; 14.CO.16.158;
14.CO.16.196; 14.CO.16.223; 14.CO.16.240; 14.CO.16.244;
14.CO.16.243; 14.CO.16.247; 14.CO.18.157; 14.CO.18.158;
14.CO.18.196; 14.CO.18.223; 14.CO.18.240; 14.CO.18.244;
14.CO.18.243; 14.CO.18.247; 14.CO.26.157; 14.CO.26.158;
14.CO.26.196; 14.CO.26.223; 14.CO.26.240; 14.CO.26.244;
14.CO.26.243; 14.CO.26.247; 14.CO.27.157; 14.CO.27.158;
14.CO.27.196; 14.CO.27.223; 14.CO.27.240; 14.CO.27.244;
14.CO.27.243; 14.CO.27.247; 14.CO.29.157; 14.CO.29.158;
14.CO.29.196; 14.CO.29.223; 14.CO.29.240; 14.CO.29.244;
14.CO.29.243; 14.CO.29.247; 14.CO.54.157; 14.CO.54.158;
14.CO.54.196; 14.CO.54.223; 14.CO.54.240; 14.CO.54.244;
14.CO.54.243; 14.CO.54.247; 14.CO.55.157; 14.CO.55.158;
14.CO.55.196; 14.CO.55.223; 14.CO.55.240; 14.CO.55.244;
14.CO.55.243; 14.CO.55.247; 14.CO.56.157; 14.CO.56.158;
14.CO.56.196; 14.CO.56.223; 14.CO.56.240; 14.CO.56.244;
14.CO.56.243; 14.CO.56.247; 14.CO.157.157; 14.CO.157.158;
14.CO.157.196; 14.CO.157.223; 14.CO.157.240; 14.CO.157.244;
14.CO.157.243; 14.CO.157.247; 14.CO.196.157;
14.CO.196.158; 14.CO.196.196; 14.CO.196.223; 14.CO.196.240;
14.CO.196.244; 14.CO.196.243; 14.CO.196.247; 14.CO.223.157;
14.CO.223.158; 14.CO.223.196; 14.CO.223.223; 14.CO.223.240;
14.CO.223.244; 14.CO.223.243; 14.CO.223.247; 14.CO.240.157;
14.CO.240.158; 14.CO.240.196; 14.CO.240.223; 14.CO.240.240;
14.CO.240.244; 14.CO.240.243; 14.CO.240.247; 14.CO.244.157;
14.CO.244.158; 14.CO.244.196; 14.CO.244.223; 14.CO.244.240;
14.CO.244.244; 14.CO.244.243; 14.CO.244.247; 14.CO.4.157;
14.CO.4.158; 14.CO.4.196; 14.CO.4.223; 14.CO.4.240; 14.CO.4.244;
14.CO.4.243; 14.CO.4.247;
Prodrugs of 8.BF
[1806] All literature and patent citations above are hereby
expressly incorporated by reference at the locations of their
citation. Specifically cited sections or pages of the above cited
works are incorporated by reference with specificity. The invention
has been described in detail sufficient to allow one of ordinary
skill in the art to make and use the subject matter of the
following Claims. It is apparent that certain modifications of the
methods and compositions of the following Claims can be made within
the scope and spirit of the invention.
[1807] In the claims hereinbelow, the subscript and superscripts of
a given variable are distinct. For example, R.sub.1 is distinct
from R.sup.1.
* * * * *