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首页> 外文期刊>Molecular pharmacology. >Receptor-mediated activation of heterotrimeric G-proteins: current structural insights.
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Receptor-mediated activation of heterotrimeric G-proteins: current structural insights.

机译:受体介导的异三聚体G蛋白的激活:当前的结构见解。

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摘要

G-protein-coupled receptors (GPCRs) serve as catalytic activators of heterotrimeric G-proteins (Galphabetagamma) by exchanging GTP for the bound GDP on the Galpha subunit. This guanine nucleotide exchange factor activity of GPCRs is the initial step in the G-protein cycle and determines the onset of various intracellular signaling pathways that govern critical physiological responses to extracellular cues. Although the structural basis for many steps in the G-protein nucleotide cycle have been made clear over the past decade, the precise mechanism for receptor-mediated G-protein activation remains incompletely defined. Given that these receptors have historically represented a set of rich drug targets, a more complete understanding of their mechanism of action should provide further avenues for drug discovery. Several models have been proposed to explain the communication between activated GPCRs and Galphabetagamma leading to the structural changes required for guanine nucleotide exchange. This review is focused on the structural biology of G-protein signal transduction with an emphasis on the current hypotheses regarding Galphabetagamma activation. We highlight several recent results shedding new light on the structural changes in Galpha that may underlie GDP release.
机译:通过将GTP交换为Galpha亚基上的结合GDP,G蛋白偶联受体(GPCR)充当异源三聚G蛋白(Galphabetagamma)的催化激活剂。 GPCR的这种鸟嘌呤核苷酸交换因子活性是G蛋白循环的第一步,它决定了控制对细胞外信号的关键生理反应的各种细胞内信号通路的发生。尽管在过去十年中已经明确了G蛋白核苷酸循环中许多步骤的结构基础,但是受体介导的G蛋白活化的精确机制仍未完全确定。鉴于这些受体在历史上代表了一组丰富的药物靶标,对其作用机理的更全面了解应该为药物发现提供更多途径。已经提出了几种模型来解释激活的GPCR和Galphabetagamma之间的通讯,从而导致鸟嘌呤核苷酸交换所需的结构变化。这篇评论集中在G蛋白信号转导的结构生物学,重点是关于Galphabetagamma激活的当前假设。我们重点介绍了近期的一些结果,为可能释放GDP的Galpha结构变化提供了新的思路。

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