Litcius/Paper detail

The Role of GIP in the Regulation of GLP-1 Satiety and Nausea

Matthew R. Hayes, Tito Borner, Bart C. De Jonghe

2021Diabetes58 citationsDOIOpen Access PDF

Abstract

Gastric inhibitory peptide (GIP) is best known for its role as an incretin hormone in control of blood glucose concentrations. As a classic satiation signal, however, the literature illustrates a mixed picture of GIP involvement with an at best weak anorectic response profile being reported for GIP receptor (GIPR) signaling. Not surprisingly, the pursuit of exploiting the GIP system as a therapeutic target for diabetes and obesity has fallen behind that of the other gastrointestinal-derived incretin, glucagon-like peptide 1 (GLP-1). However, recent discoveries highlighted here support potential therapeutic advantages of combinatorial therapies targeting GIP and GLP-1 systems together, with perhaps the most surprising finding that GIPR agonism may have antiemetic properties. As nausea and vomiting are the most common side effects of all existing GLP-1 pharmacotherapies, the ability for GIP agonism to reduce GLP-1-induced illness behaviors but retain (if not enhance) weight loss and glycemic control may offer a new era in the treatment of obesity and diabetes.

Topics & Concepts

IncretinGlucagon-like peptide-1MedicineGastric inhibitory polypeptideNauseaGlycemicInternal medicineEndocrinologyExenatideGastrointestinal hormoneLiraglutideVomitingDiabetes mellitusHormoneType 2 diabetesGlucagonPeptide hormoneDiabetes Treatment and ManagementPharmacology and Obesity TreatmentNeuropeptides and Animal Physiology