Conformation-tunable ATP-competitive kinase inhibitors

激酶 化学 生物化学 蛋白激酶A 细胞周期蛋白依赖激酶9 丝裂原活化蛋白激酶激酶
作者
Michael P. Agius,Kristin S. Ko,Taylor K. Johnson,Sameer Phadke,Matthew B. Soellner
出处
期刊:Chemical Communications [Royal Society of Chemistry]
卷期号:58 (21): 3541-3544 被引量:2
标识
DOI:10.1039/d1cc06893h
摘要

Small molecule kinase inhibitors have shown immense clinical utility for diverse indications. While >60 kinase inhibitors have been approved (and many more in clinical trials), it remains unclear whether the clinical efficacy of a kinase inhibitor is solely dependent on enzymatic inhibition, or whether non-catalytic functions play a role in the efficacy of some kinase inhibitors. Here, we designed and synthesized a series of pyrazolopyrimidine kinase inhibitors that modulate the global kinase conformation of c-Src kinase. Expanding upon our findings from the pyrazolopyrimidine inhibitor series, we designed, synthesized, and evaluated three pair of conformation-selective kinase inhibitors, each with a unique hinge-binding scaffold. We profiled each pair of kinase inhibitors across 468 kinases and identified 38 kinases that could be studied using these pair of conformation-selective inhibitors. We also explore the binding of conformation-selective kinase inhibitors to mutant kinases of EGFR, FLT3, and KIT. Together, these studies yield important insight into the design of conformation-tunable kinase inhibitors and provide a toolset of compounds to study the role of protein conformation on kinase signaling.
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