GSK114: A selective inhibitor for elucidating the biological role of TNNI3K

被引：13

作者：

Lawhorn, Brian G. ^{[1
]}

Philp, Joanne ^{[1
]}

Graves, Alan P. ^{[2
]}

Shewchuk, Lisa ^{[2
]}

Holt, Dennis A. ^{[1
]}

Gatto, Gregory J., Jr. ^{[1
]}

Kallander, Lara S. ^{[1
]}

机构：

[1] GlaxoSmithKline, Heart Failure DPU, 709 Swedeland Rd, King Of Prussia, PA 19406 USA

[2] GlaxoSmithKline, Platform Sci & Technol, 709 Swedeland Rd, King Of Prussia, PA 19406 USA

来源：

BIOORGANIC & MEDICINAL CHEMISTRY LETTERS | 2016年 / 26卷 / 14期

关键词：

TNNI3K; B-Raf; Quinazoline; Substituent effects; Kinase selectivity; CARDIAC-HYPERTROPHY; KINASE; OVEREXPRESSION;

D O I：

10.1016/j.bmcl.2016.05.033

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

A series of selective TNNI3K inhibitors were developed by modifying the hinge-binding heterocycle of a previously reported dual TNNI3K/B-Raf inhibitor. The resulting quinazoline-containing compounds exhibit a large preference (up to 250-fold) for binding to TNNI3K versus B-Raf, are useful probes for elucidating the biological pathways associated with TNNI3K, and are leads for discovering novel cardiac medicines. GSK114 emerged as a leading inhibitor, displaying significant bias (40-fold) for TNNI3K over B-Raf, exceptional broad spectrum kinase selectivity, and adequate oral exposure to enable its use in cellular and in vivo studies. (C) 2016 Elsevier Ltd. All rights reserved.

引用

页码：3355 / 3358

页数：4

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