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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Autores principales: Yang, Bin, Gelfanov, Vasily M., El, Kimberley, Chen, Alex, Rohlfs, Rebecca, DuBois, Barent, Kruse Hansen, Ann Maria, Perez-Tilve, Diego, Knerr, Patrick J., D'Alessio, David, Campbell, Jonathan E., Douros, Jonathan D., Finan, Brian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9719863/
https://www.ncbi.nlm.nih.gov/pubmed/36400403
http://dx.doi.org/10.1016/j.molmet.2022.101638
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author Yang, Bin
Gelfanov, Vasily M.
El, Kimberley
Chen, Alex
Rohlfs, Rebecca
DuBois, Barent
Kruse Hansen, Ann Maria
Perez-Tilve, Diego
Knerr, Patrick J.
D'Alessio, David
Campbell, Jonathan E.
Douros, Jonathan D.
Finan, Brian
author_facet Yang, Bin
Gelfanov, Vasily M.
El, Kimberley
Chen, Alex
Rohlfs, Rebecca
DuBois, Barent
Kruse Hansen, Ann Maria
Perez-Tilve, Diego
Knerr, Patrick J.
D'Alessio, David
Campbell, Jonathan E.
Douros, Jonathan D.
Finan, Brian
author_sort Yang, Bin
collection PubMed
description 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, [N(α)-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.
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spelling pubmed-97198632022-12-06 Discovery of a potent GIPR peptide antagonist that is effective in rodent and human systems Yang, Bin Gelfanov, Vasily M. El, Kimberley Chen, Alex Rohlfs, Rebecca DuBois, Barent Kruse Hansen, Ann Maria Perez-Tilve, Diego Knerr, Patrick J. D'Alessio, David Campbell, Jonathan E. Douros, Jonathan D. Finan, Brian Mol Metab Original Article 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, [N(α)-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. Elsevier 2022-11-15 /pmc/articles/PMC9719863/ /pubmed/36400403 http://dx.doi.org/10.1016/j.molmet.2022.101638 Text en © 2022 The Author(s) https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Article
Yang, Bin
Gelfanov, Vasily M.
El, Kimberley
Chen, Alex
Rohlfs, Rebecca
DuBois, Barent
Kruse Hansen, Ann Maria
Perez-Tilve, Diego
Knerr, Patrick J.
D'Alessio, David
Campbell, Jonathan E.
Douros, Jonathan D.
Finan, Brian
Discovery of a potent GIPR peptide antagonist that is effective in rodent and human systems
title Discovery of a potent GIPR peptide antagonist that is effective in rodent and human systems
title_full Discovery of a potent GIPR peptide antagonist that is effective in rodent and human systems
title_fullStr Discovery of a potent GIPR peptide antagonist that is effective in rodent and human systems
title_full_unstemmed Discovery of a potent GIPR peptide antagonist that is effective in rodent and human systems
title_short Discovery of a potent GIPR peptide antagonist that is effective in rodent and human systems
title_sort discovery of a potent gipr peptide antagonist that is effective in rodent and human systems
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9719863/
https://www.ncbi.nlm.nih.gov/pubmed/36400403
http://dx.doi.org/10.1016/j.molmet.2022.101638
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