| Literature DB >> 32698187 |
Fan Yang1,2, Chunyou Mao3,4, Lulu Guo1,2, Jingyu Lin1,2, Qianqian Ming3,4,5, Peng Xiao1, Xiang Wu1, Qingya Shen3,4, Shimeng Guo6, Dan-Dan Shen3,4, Ruirui Lu1,7, Linqi Zhang8, Shenming Huang8, Yuqi Ping1, Chenlu Zhang6, Cheng Ma9, Kai Zhang1, Xiaoying Liang6, Yuemao Shen10, Fajun Nan6,11, Fan Yi12, Vincent C Luca5, Jiuyao Zhou7, Changtao Jiang8, Jin-Peng Sun13,14,15, Xin Xie16,17, Xiao Yu18,19, Yan Zhang20,21,22.
Abstract
The G-protein-coupled bile acid receptor (GPBAR) conveys the cross-membrane signalling of a vast variety of bile acids and is a signalling hub in the liver-bile acid-microbiota-metabolism axis1-3. Here we report the cryo-electron microscopy structures of GPBAR-Gs complexes stabilized by either the high-affinity P3954 or the semisynthesized bile acid derivative INT-7771,3 at 3 Å resolution. These structures revealed a large oval pocket that contains several polar groups positioned to accommodate the amphipathic cholic core of bile acids, a fingerprint of key residues to recognize diverse bile acids in the orthosteric site, a putative second bile acid-binding site with allosteric properties and structural features that contribute to bias properties. Moreover, GPBAR undertakes an atypical mode of activation and G protein coupling that features a different set of key residues connecting the ligand-binding pocket to the Gs-coupling site, and a specific interaction motif that is localized in intracellular loop 3. Overall, our study not only reveals unique structural features of GPBAR that are involved in bile acid recognition and allosteric effects, but also suggests the presence of distinct connecting mechanisms between the ligand-binding pocket and the G-protein-binding site in the G-protein-coupled receptor superfamily.Entities:
Year: 2020 PMID: 32698187 DOI: 10.1038/s41586-020-2569-1
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962