Literature DB >> 32371397

Cryo-electron microscopy structure of the glucagon receptor with a dual-agonist peptide.

Rulue Chang1, Xin Zhang2, Anna Qiao3,4, Antao Dai3,5, Matthew J Belousoff2, Qiuxiang Tan3,4, Lijun Shao3,4,6, Li Zhong3,4, Guangyao Lin3,4,6, Yi-Lynn Liang2, Limin Ma3, Shuo Han3, Dehua Yang3,5, Radostin Danev7, Ming-Wei Wang8,3,4,5,6, Denise Wootten9, Beili Wu10,4,6, Patrick M Sexton9.   

Abstract

Unimolecular dual agonists of the glucagon (GCG) receptor (GCGR) and glucagon-like peptide-1 receptor (GLP-1R) are a new class of drugs that are potentially superior to GLP-1R-specific agonists for the management of metabolic disease. The dual-agonist, peptide 15 (P15), is a glutamic acid 16 analog of GCG with GLP-1 peptide substitutions between amino acids 17 and 24 that has potency equivalent to those of the cognate peptide agonists at the GCGR and GLP-1R. Here, we have used cryo-EM to solve the structure of an active P15-GCGR-Gs complex and compared this structure to our recently published structure of the GCGR-Gs complex bound to GCG. This comparison revealed that P15 has a reduced interaction with the first extracellular loop (ECL1) and the top of transmembrane segment 1 (TM1) such that there is increased mobility of the GCGR extracellular domain and at the C terminus of the peptide compared with the GCG-bound receptor. We also observed a distinct conformation of ECL3 and could infer increased mobility of the far N-terminal His-1 residue in the P15-bound structure. These regions of conformational variance in the two peptide-bound GCGR structures were also regions that were distinct between GCGR structures and previously published peptide-bound structures of the GLP-1R, suggesting that greater conformational dynamics may contribute to the increased efficacy of P15 in activation of the GLP-1R compared with GCG. The variable domains in this receptor have previously been implicated in biased agonism at the GLP-1R and could result in altered signaling of P15 at the GCGR compared with GCG.
© 2020 Chang et al.

Entities:  

Keywords:  G protein–coupled receptor (GPCR); GLP-1 receptor; cryo-electron microscopy; dual agonist; glucagon; glucagon receptor; glucagon-like peptide-1 receptor; metabolic disorder; peptide 15 (P15); single particle analysis; structural biology; structure-function

Mesh:

Substances:

Year:  2020        PMID: 32371397      PMCID: PMC7363120          DOI: 10.1074/jbc.RA120.013793

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


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