| Literature DB >> 32690941 |
Ana B Bueno1, Bingfa Sun2, Francis S Willard3, Dan Feng2, Joseph D Ho4, David B Wainscott3, Aaron D Showalter5, Michal Vieth4, Qi Chen6, Cynthia Stutsman5, Betty Chau4, James Ficorilli5, Francisco J Agejas1, Graham R Cumming1, Alma Jiménez1, Isabel Rojo1, Tong Sun Kobilka2, Brian K Kobilka7, Kyle W Sloop8.
Abstract
Drugs that promote the association of protein complexes are an emerging therapeutic strategy. We report discovery of a G protein-coupled receptor (GPCR) ligand that stabilizes an active state conformation by cooperatively binding both the receptor and orthosteric ligand, thereby acting as a 'molecular glue'. LSN3160440 is a positive allosteric modulator of the GLP-1R optimized to increase the affinity and efficacy of GLP-1(9-36), a proteolytic product of GLP-1(7-36). The compound enhances insulin secretion in a glucose-, ligand- and GLP-1R-dependent manner. Cryo-electron microscopy determined the structure of the GLP-1R bound to LSN3160440 in complex with GLP-1 and heterotrimeric Gs. The modulator binds high in the helical bundle at an interface between TM1 and TM2, allowing access to the peptide ligand. Pharmacological characterization showed strong probe dependence of LSN3160440 for GLP-1(9-36) versus oxyntomodulin that is driven by a single residue. Our findings expand protein-protein modulation drug discovery to uncompetitive, active state stabilizers for peptide hormone receptors.Entities:
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Year: 2020 PMID: 32690941 DOI: 10.1038/s41589-020-0589-7
Source DB: PubMed Journal: Nat Chem Biol ISSN: 1552-4450 Impact factor: 15.040