NOVEL STEROIDAL INHIBITORS OF HUMAN CYTOCHROME P450(17-ALPHA) (17-ALPHA-HYDROXYLASE-C-17,C-20-LYASE) - POTENTIAL AGENTS FOR THE TREATMENT OF PROSTATIC-CANCER

被引：321

作者：

POTTER, GA ^{[1
]}

BARRIE, SE ^{[1
]}

JARMAN, M ^{[1
]}

ROWLANDS, MG ^{[1
]}

机构：

[1] INST CANC RES,CTR CANC THERAPEUT,CANC RES CAMPAIGN LAB,SUTTON SM2 5NG,SURREY,ENGLAND

来源：

JOURNAL OF MEDICINAL CHEMISTRY | 1995年 / 38卷 / 13期

关键词：

D O I：

10.1021/jm00013a022

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

Steroidal compounds having a 17-(3-pyridyl) substituent together with a 16,17-double bond have been synthesized, using a palladium-catalyzed cross-coupling reaction of a 17-enol triflate with diethyl(3-pyridyl)borane, which are potent inhibitors of human testicular 17 alpha-hydroxylase-C-17,C-20-lyase. The requirement for these structural features is stringent: compounds having 2-pyridyl (9), 4-pyridyl (10), or 2-pyridylmethyl (11) substituents instead of the 3-pyridyl substituent were either poor inhibitors or noninhibitory. Reduction of the 16,17-double bond to give 17 beta-pyridyl derivatives diminished potency with 3-pyridyl substitution (3 --> 27; IC50 for lyase, 2.9 --> 23 nM) but increased it with a 4-pyridyl substituent present (10 --> 28; IC50 1 mu M --> 53 nM). In contrast, a variety of substitution patterns in rings A-C of the steroid skeleton afforded inhibitors having potencies similar to those most closely related structurally to the natural substrates pregnenolone and progesterone, respectively 17-(3-pyridyl)androsta-5,16-dien-3 beta-ol (3, K-iapp < 1 nM; IC50 for lyase, 2.9 nM) and 17-(3-pyridyl)androsta-4,16-dien-3-one (15; IC50 for lyase, 2.1 nM). Thus compounds having variously aromatic ring A (18), saturated rings A/B (21, 22), and oxygenated ring C (26) exhibited IC50 values for lyase (1.8-3.0 nM) falling within a 2-fold range. The most potent compounds are candidates for development as drugs for the treatment of hormone-dependent prostatic carcinoma.

引用

页码：2463 / 2471

页数：9

共 48 条

[1] 17-BETA-(CYCLOPROPYLAMINO)-ANDROST-5-EN-3-BETA-OL, A SELECTIVE MECHANISM-BASED INHIBITOR OF CYTOCHROME P45017-ALPHA (STEROID 17-ALPHA HYDROXYLASE-C17-20 LYASE) [J].

ANGELASTRO, MR ;

LAUGHLIN, ME ;

SCHATZMAN, GL ;

BEY, P ;

BLOHM, TR .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1989, 162 (03) :1571-1577

[2] STEROIDAL ANDROGEN BIOSYNTHESIS INHIBITORS [J].

ARTH, GE ;

PATCHETT, AA ;

JEFOPOULUS, T ;

BUGIANESI, RL ;

PETERSON, LH ;

HAM, EA ;

KUEHL, FA ;

BRINK, NG .

JOURNAL OF MEDICINAL CHEMISTRY, 1971, 14 (08) :675-+

[3] PHARMACOLOGY OF NOVEL STEROIDAL INHIBITORS OF CYTOCHROME P450(17-ALPHA) (17-ALPHA-HYDROXYLASE C17-20 LYASE) [J].

BARRIE, SE ;

POTTER, GA ;

GODDARD, PM ;

HAYNES, BP ;

DOWSETT, M ;

JARMAN, M .

JOURNAL OF STEROID BIOCHEMISTRY AND MOLECULAR BIOLOGY, 1994, 50 (5-6) :267-273

[4]

BARRIE SE, 1992, Patent No. 2253851

[5]

BEUMEL OF, 1974, SYNTHESIS-STUTTGART, P43

[6] CANCER STATISTICS, 1993 [J].

BORING, CC ;

SQUIRES, TS ;

TONG, T .

CA-A CANCER JOURNAL FOR CLINICIANS, 1993, 43 (01) :7-26

[7] MICROBIOLOGICAL HYDROXYLATION OF STEROIDS .1. PROTON MAGNETIC RESONANCE SPECTRA OF KETONES, ALCOHOLS, AND ACETATES IN ANDROSTANE, PREGNANE, AND CESTRANE SERIES [J].

BRIDGEMA.JE ;

CHERRY, PC ;

CLEGG, AS ;

EVANS, JM ;

JONES, ERH ;

KASAL, A ;

KUMAR, V ;

MEAKINS, GD ;

MORISAWA, Y ;

RICHARDS, EE ;

WOODGATE, PD .

JOURNAL OF THE CHEMICAL SOCIETY C-ORGANIC, 1970, (02) :250-&

[8]

CACCHI S, 1990, ORG SYNTH, V68, P138

[9]

CHAN FCY, 1993, J CHEM RES-S, P454

[10]

CHASALOW F, 1979, J BIOL CHEM, V254, P3000

← 1 2 3 4 5 →