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G-Protein-coupled receptor-protein interactions: basis for new concepts on receptor structure and function.

机译:G蛋白偶联的受体-蛋白质相互作用:受体结构和功能新概念的基础。

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摘要

1. G-Protein-coupled receptors (GPCRs) constitute a large family of cell surface proteins. Their primary function is to transmit extracellular stimuli to intracellular signals. It is estimated that the human genome contains more than 1000 genes that code for proteins of the GPCR structure. These receptors also comprise the most important class of therapeutic drug targets. 2. The mechanism of GPCR signalling was initially envisioned as involving coupling to the heterotrimeric G-proteins only. However, recent developments in the field suggest that such a simplistic model cannot be sustained any longer. The emerging view is that a wide range of accessory proteins are involved in the regulation of every aspect of GPCR activity. 3. G-Protein-coupled receptor-interacting proteins are implicated in the regulation of several aspects of GPCR biology, including receptor targeting to the respective sites of action, receptor anchoring, signalling and receptor desensitization. In some cases (e.g. receptor activity modifying proteins), they may contribute to the receptor structure and form a part of the ligand-binding domain. 4. These findings have contributed to new concepts of cellular organization in which modular protein-protein interactions provide a network through which signalling pathways are assembled and controlled.
机译:1. G蛋白偶联受体(GPCR)构成了细胞表面蛋白的一大家族。它们的主要功能是将细胞外刺激传递至细胞内信号。据估计,人类基因组包含1000多个编码GPCR结构蛋白的基​​因。这些受体还包括最重要的一类治疗药物靶标。 2.最初设想GPCR信号传导的机制仅涉及与异源三聚体G蛋白的偶联。但是,该领域的最新发展表明,这种简单化的模型不能再持续下去了。新兴的观点是,各种各样的辅助蛋白都参与了GPCR活性各个方面的调节。 3. G蛋白偶联的受体相互作用蛋白与GPCR生物学的多个方面有关,包括将受体靶向各自的作用位点,受体锚定,信号传导和受体脱敏。在某些情况下(例如受体活性修饰蛋白),它们可能有助于受体结构并形成配体结合结构域的一部分。 4.这些发现为细胞组织的新概念做出了贡献,在这些概念中,模块化的蛋白质-蛋白质相互作用提供了一个网络,通过该网络可以组装和控制信号通路。

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