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A unique hormonal recognition feature of the human glucagon-like peptide-2 receptor
Authors:Wen Sun  Li-Nan Chen  Qingtong Zhou  Li-Hua Zhao  Dehua Yang  Huibing Zhang  Zhaotong Cong  Dan-Dan Shen  Fenghui Zhao  Fulai Zhou  Xiaoqing Cai  Yan Chen  Yan Zhou  Sarina Gadgaard  Wijnand J. C. van der Velden  Suwen Zhao  Yi Jiang  Mette M. Rosenkilde  H. Eric Xu  Yan Zhang  Ming-Wei Wang
Abstract:Glucagon-like peptides (GLP-1 and GLP-2) are two proglucagon-derived intestinal hormones that mediate distinct physiological functions through two related receptors (GLP-1R and GLP-2R) which are important drug targets for metabolic disorders and Crohn’s disease, respectively. Despite great progress in GLP-1R structure determination, our understanding on the differences of peptide binding and signal transduction between these two receptors remains elusive. Here we report the electron microscopy structure of the human GLP-2R in complex with GLP-2 and a Gs heterotrimer. To accommodate GLP-2 rather than GLP-1, GLP-2R fine-tunes the conformations of the extracellular parts of transmembrane helices (TMs) 1, 5, 7 and extracellular loop 1 (ECL1). In contrast to GLP-1, the N-terminal histidine of GLP-2 penetrates into the receptor core with a unique orientation. The middle region of GLP-2 engages with TM1 and TM7 more extensively than with ECL2, and the GLP-2 C-terminus closely attaches to ECL1, which is the most protruded among 9 class B G protein-coupled receptors (GPCRs). Functional studies revealed that the above three segments of GLP-2 are essential for GLP-2 recognition and receptor activation, especially the middle region. These results provide new insights into the molecular basis of ligand specificity in class B GPCRs and may facilitate the development of more specific therapeutics.Subject terms: Cryoelectron microscopy, Hormone receptors
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