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5-羟色胺受体相关蛋白网络:精神障碍药物发现的新靶点?

5-HT receptor-associated protein networks: new targets for drug discovery in psychiatric disorders?

机构信息

Institut de Génomique Fonctionnelle, 141 Rue de la Cardonille, Montpellier F-34094 Montpellier Cedex 5, France.

出版信息

Curr Drug Targets. 2012 Jan;13(1):28-52. doi: 10.2174/138945012798868498.

DOI:10.2174/138945012798868498
PMID:21777185
Abstract

Serotonin (5-HT) is a phylogenetically ancient transmitter implicated in many vital functions in human such as sleep, food intake, reproduction, nociception, regulation of mood and emotions as well as cognitive functions. Correspondingly, dysfunction of serotonergic transmission has been implicated in numerous psychiatric disorders such as anxio-depressive states, psychoses and addiction, and serotonergic systems are targets for a large array of psychoactive compounds including antidepressants, antipsychotics and hallucinogens. 5-HT acts on numerous receptor subtypes (14). Except for 5-HT3 receptors, which are cationic channels, 5-HT receptors belong to the G protein-coupled receptor (GPCR) superfamily and allow an extraordinarily diverse and complex pattern of cellular signalling. Over the past ten years, the majority of metabotropic 5-HT receptors has been found to interact with specific protein partners in addition to the ubiquitous GPCR modulators, GPCR kinases and β-arrestins, mainly by mean of two-hybrid and proteomic screens. These proteins, called GPCR-interacting proteins (GIPs) were found to profoundly influence the targeting, trafficking and signal transduction properties of 5-HT receptors. This article first describes our current knowledge of the nature of GIPs that bind to the different metabotropic 5-HT receptor categories. It then focuses on their impact on receptor functional status at the cellular level and illustrates how GIPs permit G protein-independent signal transduction at G protein-coupled 5-HT receptors. Finally, it reports recent data dealing with the roles of GIPs in 5-HT-related behaviours and highlights the potential of manipulating 5-HT receptor-GIP interactions to design new treatments in psychiatric disorders related to perturbations of serotonergic systems.

摘要

血清素(5-HT)是一种在进化上古老的递质,涉及人类的许多重要功能,如睡眠、摄食、生殖、痛觉、情绪和认知功能的调节。相应地,5-羟色胺能传递功能障碍与许多精神障碍有关,如焦虑-抑郁状态、精神病和成瘾,5-羟色胺能系统是包括抗抑郁药、抗精神病药和致幻剂在内的大量精神活性化合物的靶点。5-HT 作用于许多受体亚型(14)。除了阳离子通道 5-HT3 受体外,5-HT 受体属于 G 蛋白偶联受体(GPCR)超家族,允许非常多样化和复杂的细胞信号转导模式。在过去的十年中,除了普遍存在的 GPCR 调节剂 GPCR 激酶和β-arrestins 外,大多数代谢型 5-HT 受体已被发现与特定的蛋白伴侣相互作用,主要通过双杂交和蛋白质组筛选。这些被称为 GPCR 相互作用蛋白(GIPs)的蛋白被发现深刻地影响 5-HT 受体的靶向、运输和信号转导特性。本文首先描述了我们目前对与不同代谢型 5-HT 受体类别结合的 GIP 性质的认识。然后,它重点介绍了它们对细胞水平上受体功能状态的影响,并说明了 GIP 如何允许 G 蛋白偶联 5-HT 受体的 G 蛋白独立信号转导。最后,它报告了最近关于 GIP 在与 5-HT 系统扰动相关的精神障碍中 5-HT 相关行为中的作用的数据,并强调了操纵 5-HT 受体-GIP 相互作用以设计治疗与 5-羟色胺系统相关的精神障碍的新方法的潜力。

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