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作为药物靶点的G蛋白信号调节蛋白的演变——历时20年:IUPHAR综述21

The evolution of regulators of G protein signalling proteins as drug targets - 20 years in the making: IUPHAR Review 21.

作者信息

Sjögren B

机构信息

Department of Pharmacology and Toxicology, Michigan State University, East Lansing, MI, USA.

出版信息

Br J Pharmacol. 2017 Mar;174(6):427-437. doi: 10.1111/bph.13716. Epub 2017 Feb 8.

Abstract

Regulators of G protein signalling (RGS) proteins are celebrating the 20th anniversary of their discovery. The unveiling of this new family of negative regulators of G protein signalling in the mid-1990s solved a persistent conundrum in the G protein signalling field, in which the rate of deactivation of signalling cascades in vivo could not be replicated in exogenous systems. Since then, there has been tremendous advancement in the knowledge of RGS protein structure, function, regulation and their role as novel drug targets. RGS proteins play an important modulatory role through their GTPase-activating protein (GAP) activity at active, GTP-bound Gα subunits of heterotrimeric G proteins. They also possess many non-canonical functions not related to G protein signalling. Here, an update on the status of RGS proteins as drug targets is provided, highlighting advances that have led to the inclusion of RGS proteins in the IUPHAR/BPS Guide to PHARMACOLOGY database of drug targets.

摘要

G蛋白信号调节(RGS)蛋白正在庆祝其被发现20周年。20世纪90年代中期,这个新的G蛋白信号负调节因子家族的发现解决了G蛋白信号领域一个长期存在的难题,即在体内信号级联失活的速率在外源系统中无法复制。从那时起,关于RGS蛋白的结构、功能、调节及其作为新型药物靶点的作用的知识有了巨大进展。RGS蛋白通过其在异源三聚体G蛋白的活性、GTP结合的Gα亚基上的GTP酶激活蛋白(GAP)活性发挥重要的调节作用。它们还具有许多与G蛋白信号无关的非经典功能。在此,提供了关于RGS蛋白作为药物靶点的最新情况,重点介绍了促使RGS蛋白被纳入IUPHAR/BPS药物靶点药理学指南数据库的进展。

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