Role of the V2R-βarrestin-Gβγ complex in promoting G protein translocation to endosomes

V2R-βarrestin-Gβγ复合物在促进G蛋白转位至内体中的作用

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作者:Badr Sokrat #, Anthony H Nguyen #, Alex R B Thomsen, Li-Yin Huang, Hiroyuki Kobayashi, Alem W Kahsai, Jihee Kim, Bing X Ho, Symon Ma, John Little 4th, Catherine Ehrhart, Ian Pyne, Emmery Hammond, Michel Bouvier

Abstract

Classically, G protein-coupled receptors (GPCRs) promote signaling at the plasma membrane through activation of heterotrimeric Gαβγ proteins, followed by the recruitment of GPCR kinases and βarrestin (βarr) to initiate receptor desensitization and internalization. However, studies demonstrated that some GPCRs continue to signal from internalized compartments, with distinct cellular responses. Both βarr and Gβγ contribute to such non-canonical endosomal G protein signaling, but their specific roles and contributions remain poorly understood. Here, we demonstrate that the vasopressin V2 receptor (V2R)-βarr complex scaffolds Gβγ at the plasma membrane through a direct interaction with βarr, enabling its transport to endosomes. Gβγ subsequently potentiates Gαs endosomal translocation, presumably to regenerate an endosomal pool of heterotrimeric Gs. This work shines light on the mechanism underlying G protein subunits translocation from the plasma membrane to the endosomes and provides a basis for understanding the role of βarr in mediating sustained G protein signaling.

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