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Gβγ 将 Gα 与 GPCR 偶联的模型。

A model for how Gβγ couples Gα to GPCR.

机构信息

Department of Molecular Physiology and Biological Physics, University of Virginia Health System, Charlottesville, VA.

出版信息

J Gen Physiol. 2022 May 2;154(5). doi: 10.1085/jgp.202112982. Epub 2022 Mar 25.

Abstract

Representing ∼5% of the human genome, G-protein-coupled receptors (GPCRs) are a primary target for drug discovery; however, the molecular details of how they couple to heterotrimeric G protein subunits are incompletely understood. Here, I propose a hypothetical initial docking model for the encounter between GPCR and Gβγ that is defined by transient interactions between the cytosolic surface of the GPCR and the prenyl moiety and the tripeptide motif, asparagine-proline-phenylalanine (NPF), in the C-terminus of the Gγ subunit. Analysis of class A GPCRs reveals a conserved NPF binding site formed by the interaction of the TM1 and H8. Functional studies using differentially prenylated proteins and peptides further suggest that the intracellular hydrophobic core of the GPCR is a prenyl binding site. Upon binding TM1 and H8 of GPCRs, the propensity of the C-terminal region of Gγ to convert into an α helix allows it to extend into the hydrophobic core of the GPCR, facilitating the GPCR active state. Conservation of the NPF motif in Gγ isoforms and interacting residues in TM1 and H8 suggest that this is a general mechanism of GPCR-G protein signaling. Analysis of the rhodopsin dimer also suggests that Gγ-rhodopsin interactions may facilitate GPCR dimer transactivation.

摘要

G 蛋白偶联受体(GPCRs)约占人类基因组的 5%,是药物发现的主要靶点;然而,它们与异源三聚体 G 蛋白亚基偶联的分子细节尚不完全清楚。在这里,我提出了一个 GPCR 与 Gβγ 之间相互作用的假设初始对接模型,该模型由 GPCR 胞质表面与 Gγ 亚基 C 末端的异戊烯基部分和三肽基序天冬酰胺-脯氨酸-苯丙氨酸(NPF)之间的瞬时相互作用定义。对 A 类 GPCR 的分析揭示了一个保守的 NPF 结合位点,由 TM1 和 H8 的相互作用形成。使用差异异戊烯化蛋白和肽的功能研究进一步表明,GPCR 的细胞内疏水区是一个异戊烯结合位点。Gγ 亚基 C 末端的 TM1 和 H8 与 GPCR 结合后,其转化为α螺旋的倾向使其能够延伸到 GPCR 的疏水区,从而促进 GPCR 的激活状态。Gγ 同工型中的 NPF 基序和 TM1 和 H8 中的相互作用残基的保守性表明,这是 GPCR-G 蛋白信号转导的一般机制。对视紫红质二聚体的分析还表明,Gγ-视紫红质相互作用可能促进 GPCR 二聚体的反式激活。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/97eb/8961292/4723fe5929bc/JGP_202112982_Fig1.jpg

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