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G蛋白信号调节蛋白:新型多功能药物靶点。

Regulator of G protein signaling proteins: novel multifunctional drug targets.

作者信息

Zhong H, Neubig R R

机构信息

Department of Pharmacology, The University of Michigan, Ann Arbor, Michigan 48109-0632, USA.

出版信息

J Pharmacol Exp Ther. 2001 Jun;297(3):837-45.

PMID:11356902
Abstract

G protein-coupled receptors (GPCRs) play a major role in signal transduction and are targets of many therapeutic drugs. The regulator of G protein signaling (RGS) proteins form a recently identified protein family, and they strongly modulate the activity of G proteins. Their best known function is to inhibit G protein signaling by accelerating GTP hydrolysis [GTPase activating protein (GAP)] thus turning off G protein signals. RGS proteins also possess non-GAP functions, through both their RGS domains and various non-RGS domains and motifs (e.g., GGL, DEP, DH/PH, PDZ domains and a cysteine string motif). They are a highly diverse protein family, have unique tissue distributions, are strongly regulated by signal transduction events, and will likely play diverse functional roles in living cells. Thus they represent intriguing, novel pharmacological/therapeutic targets. Drugs targeting RGS proteins can be divided into five groups: 1) potentiators of endogenous agonist function, 2) potentiators/desensitization blockers of exogenous GPCR agonists, 3) specificity enhancers of exogenous agonists, 4) antagonists of effector signaling by an RGS protein, and 5) RGS agonists. In addition, a novel subsite distinction within the RGS domain has been proposed with significant functional implications and defined herein as "A-site" and "B-site". Therefore, RGS proteins should provide exciting new opportunities for drug development.

摘要

G蛋白偶联受体(GPCRs)在信号转导中起主要作用,并且是许多治疗药物的靶点。G蛋白信号调节蛋白(RGS)构成了一个最近才被鉴定出的蛋白家族,它们能强烈调节G蛋白的活性。其最广为人知的功能是通过加速GTP水解[GTP酶激活蛋白(GAP)]来抑制G蛋白信号传导,从而关闭G蛋白信号。RGS蛋白还通过其RGS结构域以及各种非RGS结构域和基序(例如GGL、DEP、DH/PH、PDZ结构域和半胱氨酸串基序)具有非GAP功能。它们是一个高度多样化的蛋白家族,具有独特的组织分布,受到信号转导事件的强烈调控,并且可能在活细胞中发挥多种功能作用。因此,它们代表了引人关注的新型药理学/治疗靶点。靶向RGS蛋白的药物可分为五类:1)内源性激动剂功能增强剂,2)外源性GPCR激动剂的增强剂/脱敏阻滞剂,3)外源性激动剂的特异性增强剂,4)RGS蛋白效应器信号传导的拮抗剂,以及5)RGS激动剂。此外,有人提出了RGS结构域内一个具有重要功能意义的新亚位点区分,并在此定义为“A位点”和“B位点 ”。因此,RGS蛋白应该为药物开发提供令人兴奋的新机会。

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