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Structure-activity relationship of GPR15L peptide analogues and investigation of their interaction with the GPR15 receptor

Basic Clin Pharmacol Toxicol. 2023-03; 
Yufang Deng, Claudia V Perez Almeria, Lieke van Gijzel, Kay Schaller, Line Vedel, David E Gloriam, Trond Ulven, Hans Bräuner-Osborne
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Abstract

The 57-mer full-length GPR15L(25-81) peptide has been identified as the principal endogenous agonist of the G protein-coupled receptor GPR15. Its main activity resides in the C-terminal 11-mer GPR15L(71-81), which has full efficacy but ~40-fold lower potency than the full-length peptide. Here, we systematically investigated the structure-activity relationship of GPR15L(71-81) by truncations/extensions, alanine-scanning, and N- and C-terminal capping. The synthesized peptide analogues were tested at GPR15 stably expressed in HEK293A cells using a homogenous time-resolved Förster resonance energy transfer-based G cAMP functional assay. We show that the C-terminal α carboxyl group and the residues Leu , Pro , Va... More

Keywords

GPR15 receptor, GPR15L peptide, agonist, receptor mutagenesis, structure-activity relationship