Molecular insights into ago-allosteric modulation of the human glucagon-like peptide-1 receptor

Author:

Cong Zhaotong,Chen Li-Nan,Ma Honglei,Zhou Qingtong,Zou Xinyu,Ye Chenyu,Dai Antao,Liu QingORCID,Huang Wei,Sun Xianqiang,Wang Xi,Xu PeiyuORCID,Zhao Lihua,Xia Tian,Zhong Wenge,Yang DehuaORCID,Eric Xu H.ORCID,Zhang YanORCID,Wang Ming-WeiORCID

Abstract

AbstractThe glucagon-like peptide-1 (GLP-1) receptor is a validated drug target for metabolic disorders. Ago-allosteric modulators are capable of acting both as agonists on their own and as efficacy enhancers of orthosteric ligands. However, the molecular details of ago-allosterism remain elusive. Here, we report three cryo-electron microscopy structures of GLP-1R bound to (i) compound 2 (an ago-allosteric modulator); (ii) compound 2 and GLP-1; and (iii) compound 2 and LY3502970 (a small molecule agonist), all in complex with heterotrimeric Gs. The structures reveal that compound 2 is covalently bonded to C347 at the cytoplasmic end of TM6 and triggers its outward movement in cooperation with the ECD whose N terminus penetrates into the GLP-1 binding site. This allows compound 2 to execute positive allosteric modulation through enhancement of both agonist binding and G protein coupling. Our findings offer insights into the structural basis of ago-allosterism at GLP-1R and may aid the design of better therapeutics.

Funder

National Natural Science Foundation of China

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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