The Evolution of Protein Kinase Inhibitors from Antagonists to Agonists of Cellular Signaling

激酶 变构调节 药物发现 化学 蛋白激酶A 生物化学 生物 细胞生物学 计算生物学 小分子
作者
Arvin C. Dar,Kevan M. Shokat
出处
期刊:Annual Review of Biochemistry [Annual Reviews]
卷期号:80 (1): 769-795 被引量:361
标识
DOI:10.1146/annurev-biochem-090308-173656
摘要

Kinases are highly regulated enzymes with diverse mechanisms controlling their catalytic output. Over time, chemical discovery efforts for kinases have produced ATP-competitive compounds, allosteric regulators, irreversible binders, and highly specific inhibitors. These distinct classes of small molecules have revealed many novel aspects about kinase-mediated signaling, and some have progressed from simple tool compounds into clinically validated therapeutics. This review explores several small-molecule inhibitors for kinases highlighting elaborate mechanisms by which kinase function is modulated. A complete surprise of targeted kinase drug discovery has been the finding of ATP-competitive inhibitors that behave as agonists, rather than antagonists, of their direct kinase target. These studies hint at a connection between ATP-binding site occupancy and networks of communication that are independent of kinase catalysis. Indeed, kinase inhibitors that induce changes in protein localization, protein-protein interactions, and even enhancement of catalytic activity of the target kinase have been found. The relevance of these findings to the therapeutic efficacy of kinase inhibitors and to the future identification of new classes of drug targets is discussed.
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