Structure-guided design of potent and selective pyrimidylpyrrole inhibitors of extracellular signal-regulated kinase (ERK) using conformational control

利用构象控制进行结构引导设计强效且选择性的胞外信号调节激酶 (ERK) 嘧啶吡咯抑制剂

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作者：Alex M Aronov, Qing Tang, Gabriel Martinez-Botella, Guy W Bemis, Jingrong Cao, Guanjing Chen, Nigel P Ewing, Pamella J Ford, Ursula A Germann, Jeremy Green, Michael R Hale, Marc Jacobs, James W Janetka, Francois Maltais, William Markland, Mark N Namchuk, Suganthini Nanthakumar, Srinivasu Poondru, Ju

期刊：

Journal of Medicinal Chemistry

影响因子：

6.800

时间：

2009

起止号：

2009 Oct 22;52(20):6362-8.

doi：

10.1021/jm900630q

研究方向：

信号转导

信号通路：

MAPK/ERK

Abstract

The Ras/Raf/MEK/ERK signal transduction, an oncogenic pathway implicated in a variety of human cancers, is a key target in anticancer drug design. A novel series of pyrimidylpyrrole ERK inhibitors has been identified. Discovery of a conformational change for lead compound 2, when bound to ERK2 relative to antitarget GSK3, enabled structure-guided selectivity optimization, which led to the discovery of 11e, a potent, selective, and orally bioavailable inhibitor of ERK.

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