Discovery of a potent, highly selective, and orally bioavailable inhibitor of CDK8 through a structure-based optimisation

被引：6

作者：

Yu, Mingfeng ^{[1
]}

Long, Yi ^{[1
]}

Yang, Yuchao ^{[1
]}

Li, Manjun ^{[1
]}

Teo, Theodosia ^{[1
]}

Noll, Benjamin ^{[1
]}

Philip, Stephen ^{[1
]}

Wang, Shudong ^{[1
]}

机构：

[1] Univ South Australia, Canc Res Inst, Clin & Hlth Sci, Drug Discovery & Dev, Adelaide, SA 5000, Australia

来源：

EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY | 2021年 / 218卷

关键词：

CDK8; inhibitor; Structure-based optimisation; Kinase selectivity; Oral bioavailability; Anti-proliferation mechanism; MV4-11; MEDIATOR COMPLEX; ACCURATE DOCKING; DUAL INHIBITORS; TARGETING CDK8; CANCER-CELLS; SAR ANALYSIS; PROLIFERATION; PHOSPHORYLATION; TRANSCRIPTION; CORTISTATIN;

D O I：

10.1016/j.ejmech.2021.113391

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

CDK8 is deregulated in multiple types of human cancer and is viewed as a therapeutic target for the treatment of the disease. Accordingly, the search for small-molecule inhibitors of CDK8 is being intensified. Capitalising on our initial discovery of AU1-100, a potent CDK8 inhibitor yet with a limited degree of kinase selectivity, a structure-based optimisation was carried out, with a series of new multi-substituted pyridines rationally designed, chemically prepared and biologically evaluated. Such endeavour has culminated in the identification of 42, a more potent CDK8 inhibitor with superior kinomic selectivity and oral bioavailability. The mechanism underlying the anti-proliferative effect of 42 on MV4-11 cells was studied, revealing that the compound arrested the G1 cell cycle and triggered apoptosis. The low risk of hepato- and cardio-toxicity of 42 was estimated. These findings merit further investigation of 42 as a targeted cancer therapeutic. (c) 2021 Elsevier Masson SAS. All rights reserved.

引用

页数：23

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