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A new synthetic dual agonist of GPR120/GPR40 induces GLP-1 secretion and improves glucose homeostasis in mice

Gianluca Bianchini, Cecilia Nigro, Anna Sirico, Rubina Novelli, Immacolata Prevenzano, Claudia Miele, Francesco Bèguinot, Andrea Aramini

2021Biomedicine & Pharmacotherapy34 citationsDOIOpen Access PDF

Abstract

intracellular spikes and G protein-independent signaling via β-arrestin with the same activity. Compared to the endogenous ligand alpha-linolenic acid (ALA), a selective GPR120 agonist (TUG-891) and a well-known dual GPR40 and GPR120 agonist (GW9508), DFL23916 was the most effective in inducing GLP-1 secretion in human and murine enteroendocrine cells, and this could be due to the delayed internalization of the receptor (up to 3 h) that we observed after treatment with DFL23916. With a good pharmacokinetic/ADME profile, DFL23916 significantly increased GLP-1 portal vein levels in healthy mice, demonstrating that it can efficiently induce GLP-1 secretion in vivo. Contrary to the selective GPR120 agonist (TUG-891), DFL23916 significantly improved also glucose homeostasis in mice undergoing an oral glucose tolerance test (OGTT).

Topics & Concepts

Free fatty acid receptor 1AgonistGPR120Glucose homeostasisReceptorInternalizationInternal medicineEndocrinologyG protein-coupled receptorChemistryGlucagon-like peptide 1 receptorEndogenous agonistSignal transductionBiologyPharmacologyCell biologyInsulinMedicineInsulin resistanceDopamine receptor D1Diabetes Treatment and ManagementPancreatic function and diabetesReceptor Mechanisms and Signaling
A new synthetic dual agonist of GPR120/GPR40 induces GLP-1 secretion and improves glucose homeostasis in mice | Litcius