17,20-Lyase inhibitors. Part 4: Design, synthesis and structure-activity relationships of naphthylmethylimidazole derivatives as novel 17,20-lyase inhibitors

被引：9

作者：

Kaku, Tomohiro ^{[1
]}

Matsunaga, Nobuyuki ^{[1
]}

Ojida, Akio ^{[5
]}

Tanaka, Toshimasa ^{[2
]}

Hara, Takahito ^{[3
]}

Yamaoka, Masuo ^{[3
]}

Kusaka, Masami ^{[3
]}

Tasaka, Akihiro ^{[4
]}

机构：

[1] Takeda Pharmaceut Co Ltd, Med Chem Res Labs, Yodogawa Ku, Osaka 5328686, Japan

[2] Takeda Pharmaceut Co Ltd, Discovery Res Ctr, Yodogawa Ku, Osaka 5328686, Japan

[3] Takeda Pharmaceut Co Ltd, Pharmacol Res Labs, Yodogawa Ku, Osaka 5328686, Japan

[4] Takeda Pharmaceut Co Ltd, Environm & Safety Dept, Yodogawa Ku, Osaka 5328686, Japan

[5] Kyushu Univ, Grad Sch Pharmaceut Sci, Higashi Ku, Fukuoka 8128582, Japan

来源：

BIOORGANIC & MEDICINAL CHEMISTRY | 2011年 / 19卷 / 05期

关键词：

17,20-Lyase; 11-Hydroxylase; Testosterone; Prostate cancer; HUMAN-LIVER-MICROSOMES; HUMAN 17-ALPHA-HYDROXYLASE-17,20-LYASE CYP17; 17-ALPHA-HYDROXYLASE-C17,20-LYASE P450 17; RESISTANT PROSTATE-CANCER; BIOLOGICAL EVALUATION; POTENTIAL AGENTS; ANDROGEN BIOSYNTHESIS; STEROIDAL INHIBITORS; IN-VITRO; C-17; C-20-LYASE INHIBITOR;

D O I：

10.1016/j.bmc.2011.01.017

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

A novel series of naphthylmethylimidazole derivatives and related compounds have been investigated as selective 17,20-lyase inhibitors. Optimization of the substituent at the 6-position on the naphthalene ring was performed to yield a methylcarbamoyl derivative, which exhibited potent inhibitory activity against human 17,20-lyase and promising selectivity (> 200-fold) for 17,20-lyase over CYP3A4. Further modifications of the methylcarbamoyl derivative led to the discovery of the corresponding tricyclic compound, which showed highly potent activity against human 17,20-lyase (IC50 19 nM) and good selectivity (> 1000-fold) for inhibition of 17,20-lyase over CYP3A4. Additional biological evaluation revealed that the tricyclic compound had potent in vivo efficacy in monkeys and favorable pharmacokinetic profiles when administered in rats. Asymmetric synthesis of the selective tricyclic inhibitor was also achieved using a chiral alpha-hydroxy ketone. (C) 2011 Elsevier Ltd. All rights reserved.

引用

页码：1751 / 1770

页数：20

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