| Literature DB >> 27924341 |
Alexandre Murza1, Xavier Sainsily1, Jérôme Côté1, Laurent Bruneau-Cossette1, Élie Besserer-Offroy1, Jean-Michel Longpré1, Richard Leduc1, Robert Dumaine2, Olivier Lesur3, Mannix Auger-Messier4, Philippe Sarret1, Éric Marsault1.
Abstract
Apelin is the endogenous ligand for the G protein-coupled receptor APJ and exerts a key role in regulating cardiovascular functions. We report herein a novel series of macrocyclic analogues of apelin-13 in which the N- and C-terminal residues as well as the macrocycle composition were chemically modified to modulate structure-activity relationships on the APJ receptor. To this end, the binding affinity and the ability to engage G protein-dependent and G protein-independent signalling pathways of the resulting analogues were assessed. In this series, the position and the nature of the C-terminal aromatic residue is a determinant for APJ interaction and β-arrestin recruitment, as previously demonstrated for linear apelin-13 derivatives. We finally discovered compounds 1, 4, 11 and 15, four potent G protein-biased apelin receptor agonists exhibiting affinity in the nanomolar range for APJ. These macrocyclic compounds represent very useful pharmacological tools to explore the therapeutic potential of the apelinergic system.Entities:
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Year: 2017 PMID: 27924341 DOI: 10.1039/c6ob02247b
Source DB: PubMed Journal: Org Biomol Chem ISSN: 1477-0520 Impact factor: 3.876