| Literature DB >> 33408414 |
Yu-Qi Ping1,2,3, Chunyou Mao4,5, Peng Xiao3, Ru-Jia Zhao3, Yi Jiang1, Zhao Yang3, Wen-Tao An3, Dan-Dan Shen4,5, Fan Yang3,6, Huibing Zhang4,5, Changxiu Qu2,3, Qingya Shen4,5, Caiping Tian7,8, Zi-Jian Li9, Shaolong Li3, Guang-Yu Wang3, Xiaona Tao3, Xin Wen3, Ya-Ni Zhong3, Jing Yang7, Fan Yi10, Xiao Yu6, H Eric Xu11, Yan Zhang12,13,14,15, Jin-Peng Sun16,17.
Abstract
Adhesion G-protein-coupled receptors (GPCRs) are a major family of GPCRs, but limited knowledge of their ligand regulation or structure is available1-3. Here we report that glucocorticoid stress hormones activate adhesion G-protein-coupled receptor G3 (ADGRG3; also known as GPR97)4-6, a prototypical adhesion GPCR. The cryo-electron microscopy structures of GPR97-Go complexes bound to the anti-inflammatory drug beclomethasone or the steroid hormone cortisol revealed that glucocorticoids bind to a pocket within the transmembrane domain. The steroidal core of glucocorticoids is packed against the 'toggle switch' residue W6.53, which senses the binding of a ligand and induces activation of the receptor. Active GPR97 uses a quaternary core and HLY motif to fasten the seven-transmembrane bundle and to mediate G protein coupling. The cytoplasmic side of GPR97 has an open cavity, where all three intracellular loops interact with the Go protein, contributing to the high basal activity of GRP97. Palmitoylation at the cytosolic tail of the Go protein was found to be essential for efficient engagement with GPR97 but is not observed in other solved GPCR complex structures. Our work provides a structural basis for ligand binding to the seven-transmembrane domain of an adhesion GPCR and subsequent G protein coupling.Entities:
Year: 2021 PMID: 33408414 DOI: 10.1038/s41586-020-03083-w
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962