| Literature DB >> 32193322 |
Anna Qiao1,2,3, Shuo Han1,2, Xinmei Li3,4, Zhixin Li5, Peishen Zhao6, Antao Dai1,7, Rulve Chang5, Linhua Tai3,4, Qiuxiang Tan1,2, Xiaojing Chu1,2, Limin Ma1,2, Thor Seneca Thorsen8, Steffen Reedtz-Runge8, Dehua Yang1,7, Ming-Wei Wang1,3,5,7,9, Patrick M Sexton5,6, Denise Wootten10,6, Fei Sun11,4,12, Qiang Zhao13,3,14, Beili Wu15,3,9,14.
Abstract
Class B G protein-coupled receptors, an important class of therapeutic targets, signal mainly through the Gs class of heterotrimeric G proteins, although they do display some promiscuity in G protein binding. Using cryo-electron microscopy, we determined the structures of the human glucagon receptor (GCGR) bound to glucagon and distinct classes of heterotrimeric G proteins, Gs or Gi1 These two structures adopt a similar open binding cavity to accommodate Gs and Gi1 The Gs binding selectivity of GCGR is explained by a larger interaction interface, but there are specific interactions that affect Gi more than Gs binding. Conformational differences in the receptor intracellular loops were found to be key selectivity determinants. These distinctions in transducer engagement were supported by mutagenesis and functional studies.Entities:
Year: 2020 PMID: 32193322 DOI: 10.1126/science.aaz5346
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728