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Discovery of a potent GIPR peptide antagonist that is effective in rodent and human systems

Objective: Glucose-dependent insulinotropic polypeptide (GIP) is one of the two major incretin factors that regulate metabolic homeostasis. Genetic ablation of its receptor (GIPR) in mice confers protection against diet-induced obesity (DIO), while GIPR neutralizing antibodies produce additive weigh...

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Main Authors: Bin Yang (Author), Vasily M. Gelfanov (Author), Kimberley El (Author), Alex Chen (Author), Rebecca Rohlfs (Author), Barent DuBois (Author), Ann Maria Kruse Hansen (Author), Diego Perez-Tilve (Author), Patrick J. Knerr (Author), David D'Alessio (Author), Jonathan E. Campbell (Author), Jonathan D. Douros (Author), Brian Finan (Author)
Format: Book
Published: Elsevier, 2022-12-01T00:00:00Z.
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LEADER 00000 am a22000003u 4500
001 doaj_5be25854491f46ddb6f40e6afecdb0ce
042 |a dc 
100 1 0 |a Bin Yang  |e author 
700 1 0 |a Vasily M. Gelfanov  |e author 
700 1 0 |a Kimberley El  |e author 
700 1 0 |a Alex Chen  |e author 
700 1 0 |a Rebecca Rohlfs  |e author 
700 1 0 |a Barent DuBois  |e author 
700 1 0 |a Ann Maria Kruse Hansen  |e author 
700 1 0 |a Diego Perez-Tilve  |e author 
700 1 0 |a Patrick J. Knerr  |e author 
700 1 0 |a David D'Alessio  |e author 
700 1 0 |a Jonathan E. Campbell  |e author 
700 1 0 |a Jonathan D. Douros  |e author 
700 1 0 |a Brian Finan  |e author 
245 0 0 |a Discovery of a potent GIPR peptide antagonist that is effective in rodent and human systems 
260 |b Elsevier,   |c 2022-12-01T00:00:00Z. 
500 |a 2212-8778 
500 |a 10.1016/j.molmet.2022.101638 
520 |a Objective: Glucose-dependent insulinotropic polypeptide (GIP) is one of the two major incretin factors that regulate metabolic homeostasis. Genetic ablation of its receptor (GIPR) in mice confers protection against diet-induced obesity (DIO), while GIPR neutralizing antibodies produce additive weight reduction when combined with GLP-1R agonists in preclinical models and clinical trials. Conversely, GIPR agonists have been shown to promote weight loss in rodents, while dual GLP-1R/GIPR agonists have proven superior to GLP-1R monoagonists for weight reduction in clinical trials. We sought to develop a long-acting, specific GIPR peptide antagonist as a tool compound suitable for investigating GIPR pharmacology in both rodent and human systems. Methods: We report a structure-activity relationship of GIPR peptide antagonists based on the human and mouse GIP sequences with fatty acid-based protraction. We assessed these compounds in vitro, in vivo in DIO mice, and ex vivo in islets from human donors. Results: We report the discovery of a GIP(5-31) palmitoylated analogue, [Nα-Ac, L14, R18, E21] hGIP(5-31)-K11 (γE-C16), which potently inhibits in vitro GIP-mediated cAMP generation at both the hGIPR and mGIPR. In vivo, this peptide effectively blocks GIP-mediated reductions in glycemia in response to exogenous and endogenous GIP and displays a circulating pharmacokinetic profile amenable for once-daily dosing in rodents. Co-administration with the GLP-1R agonist semaglutide and this GIPR peptide antagonist potentiates weight loss compared to semaglutide alone. Finally, this antagonist inhibits GIP- but not GLP-1-stimulated insulin secretion in intact human islets. Conclusions: Our work demonstrates the discovery of a potent, specific, and long-acting GIPR peptide antagonist that effectively blocks GIP action in vitro, ex vivo in human islets, and in vivo in mice while producing additive weight-loss when combined with a GLP-1R agonist in DIO mice. 
546 |a EN 
690 |a Peptide antagonist 
690 |a GIP/GIPR 
690 |a GLP-1/GLP-1R 
690 |a Obesity 
690 |a Diabetes 
690 |a Internal medicine 
690 |a RC31-1245 
655 7 |a article  |2 local 
786 0 |n Molecular Metabolism, Vol 66, Iss , Pp 101638- (2022) 
787 0 |n http://www.sciencedirect.com/science/article/pii/S2212877822002071 
787 0 |n https://doaj.org/toc/2212-8778 
856 4 1 |u https://doaj.org/article/5be25854491f46ddb6f40e6afecdb0ce  |z Connect to this object online. 

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