Multiplicity and regulation of G-protein couplings.

E Hermans
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Abstract

During the last twenty years, molecular and biochemical data concerning G-protein coupled receptors have accumulated, providing a detailed characterisation of the structure and functions of this large family of receptors. Initially viewed as simple transducing proteins interacting with intracellular adapters which confer signalling specificity and amplification, the last decade has revealed the extreme complexity and flexibility offered by these membrane receptors. Indeed, there is accumulating evidence that these receptors can interact with several unrelated G-proteins and that some ligands can specifically orientate the functional response. This article summarizes my contributions to the study of the multiplicity and regulation of cell signallings associated with three unrelated systems: the neurotensin receptor, the type 1 metabotropic glutamate receptor and the type 1 cannabinoid receptor. Along with other studies, these experimental data emphasise on the importance of the emerging concept of functional selectivity which should lead to the development of drugs showing enhanced clinical efficacy with lower unwanted side effects.

g蛋白偶联的多样性和调控。
在过去的二十年中,关于g蛋白偶联受体的分子和生化数据的积累,提供了这一大家族受体的结构和功能的详细特征。最初被视为与细胞内适配器相互作用的简单转导蛋白,赋予信号特异性和扩增,过去十年揭示了这些膜受体提供的极端复杂性和灵活性。事实上,越来越多的证据表明,这些受体可以与几种不相关的g蛋白相互作用,并且一些配体可以特异性地定向功能反应。本文综述了笔者在神经紧张素受体、1型代谢性谷氨酸受体和1型大麻素受体这三个不相关系统的细胞信号的多样性和调控方面的研究成果。与其他研究一起,这些实验数据强调了功能选择性这一新兴概念的重要性,它将导致开发出具有更高临床疗效和更低不良副作用的药物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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