Discovery of a Novel Piperidine-Based Inhibitor of Cholesteryl Ester Transfer Protein (CETP) That Retains Activity in Hypertriglyceridemic Plasma

被引：7

作者：

Yamada, Ken ^{[1
,3
]}

Brousseau, Margaret ^{[1
]}

Honma, Wataru ^{[3
,4
]}

Iimura, Akiko ^{[3
,4
]}

Imase, Hidetomo ^{[1
,3
]}

Iwaki, Yuki ^{[1
,3
,5
]}

Kawanami, Toshio ^{[1
,3
]}

LaSala, Daniel ^{[2
,6
]}

Liang, Guiqing ^{[1
]}

Mitani, Hironobu ^{[3
,4
]}

Nonomura, Kazuhiko ^{[3
,7
]}

Ohmori, Osamu ^{[3
,8
]}

Pan, Meihui ^{[1
]}

Rigel, Dean F. ^{[2
,9
]}

Umemura, Ichiro ^{[3
,4
]}

Yasoshima, Kayo ^{[1
,3
]}

Zhu, Guoming ^{[1
]}

Mogi, Muneto ^{[1
,3
]}

机构：

[1] Novartis Inst BioMed Res Inc, 250 Massachusetts Ave, Cambridge, MA 02139 USA

[2] Novartis Pharmaceut, Novartis Inst BioMed Res, 1 Hlth Plaza, E Hanover, NJ 07936 USA

[3] Novartis Pharma KK, Novartis Inst BioMed Res, Ohkubo 8, Tsukuba, Ibaraki 3002611, Japan

[4] Novartis Pharma KK, Minato Ku, Tokyo 10506333, Japan

[5] Janssen Pharmaceut KK, Shinjuku Ku, Tokyo 1620805, Japan

[6] Insmed Inc, Bridgewater, NJ 07034 USA

[7] Mochida Pharmaceut Co Ltd, Shinjuku Ku, Tokyo 1608515, Japan

[8] Asahi Kasei Pharma Corp, Izunokuni, Shizuoka 4102321, Japan

[9] Rigel BioPharma Consulting LLC, Berkeley Hts, NJ 07922 USA

来源：

JOURNAL OF MEDICINAL CHEMISTRY | 2017年 / 60卷 / 20期

关键词：

HIGH-DENSITY LIPOPROTEIN; CORONARY-HEART-DISEASE; HIGH-RISK; BLOOD-PRESSURE; TORCETRAPIB; ALDOSTERONE; TARGET; LIPOPHILICITY; ASSOCIATION; ANACETRAPIB;

D O I：

10.1021/acs.jmedchem.7b00900

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

Herein we describe the discovery and characterization of a novel, piperidine-based inhibitor of cholesteryl ester transfer protein (CETP) with a core structure distinct from other reported CETP inhibitors. A versatile synthesis starting from 4-methoxypyridine enabled an efficient exploration of the SAR, giving a lead molecule with potent CETP inhibition in human plasma. The subsequent optimization focused on improvement of pharmacokinetics and mitigation of off-target liabilities, such as CYP inhibition, whose improvement correlated with increased lipophilic efficiency. The effort led to the identification of an achiral, carboxylic acid-bearing compound 16 (TAP311) with excellent pharmacokinetics in rats and robust efficacy in hamsters. Compared to anacetrapib, the compound showed substantially reduced lipophilicity, had only modest distribution into adipose tissue, and retained potency in hypertriglyceridemic plasma in vitro and in vivo. Furthermore, in contrast to torcetrapib, the compound did not increase aldosterone secretion in human adrenocortical carcinoma cells nor in chronically cannulated rats. On the basis of its preclinical efficacy and safety profile, the compound was advanced into clinical trials.

引用

页码：8466 / 8481

页数：16

共 42 条

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