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The Open Question of How GPCRs Interact with GPCR Kinases (GRKs)

机译:GPCRS如何与GPCR激酶(RKS)互动的开放问题

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摘要

G protein-coupled receptors (GPCRs), which regulate a vast number of eukaryotic processes, are desensitized by various mechanisms but, most importantly, by the GPCR kinases (GRKs). Ever since GRKs were first identified, investigators have sought to determine which structural features of GRKs are used to select for the agonist-bound states of GPCRs and how this binding event in turn enhances GRK catalytic activity. Despite a wealth of molecular information from high-resolution crystal structures of GRKs, the mechanisms driving activation have remained elusive, in part because the GRK N-terminus and active site tether region, previously proposed to serve as a receptor docking site and to be key to kinase domain closure, are often disordered or adopt inconsistent conformations. However, two recent studies have implicated other regions of GRKs as being involved in direct interactions with active GPCRs. Atomic resolution structures of GPCR–GRK complexes would help refine these models but are, so far, lacking. Here, we assess three distinct models for how GRKs recognize activated GPCRs, discuss limitations in the approaches used to generate them, and then experimentally test a hypothetical GPCR interaction site in GRK2 suggested by the two newest models.
机译:G蛋白偶联受体(GPCR)通过各种机制脱敏,该受体(GPCR)调节大量真核过程,但最重要的是由GPCR激酶(GRKS)。自从首次被鉴定以来,研究人员试图确定胶羊的结构特征用于选择GPCR的激动剂 - 结合状态以及这种结合事件如何增强GRK催化活性。尽管从高分辨率的铜晶体结构具有丰富的分子信息,但是驱动激活的机制仍然是难以捉摸的,部分是因为先前提出的GRK N-末端和活性位点系列作为受体对接部位并成为关键对于激酶域闭合,通常是混乱的或采用不一致的构象。然而,最近的两个研究使款地区的其他地区涉及与活跃的GPCR直接相互作用。 GPCR-GRK复合物的原子分辨率结构将有助于改进这些模型,但到目前为止,缺乏。在这里,我们评估了三种不同的模型,了解麦克斯如何识别激活的GPCR,讨论用于生成它们的方法的限制,然后通过实验测试两个最新模型建议的GRK2中的假设GPCR交互站点。

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