Genetic and biased agonist-mediated reductions in β-arrestin recruitment prolong cAMP signaling at glucagon family receptors

Receptors for the peptide hormones glucagon-like peptide-1 (GLP-1R), glucose-dependent insulinotropic polypeptide (GIPR), and glucagon (GCGR) are important regulators of insulin secretion and energy metabolism. GLP-1R agonists have been successfully deployed for the treatment of type 2 diabetes, but...

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Autores principales: Jones, Ben, McGlone, Emma Rose, Fang, Zijian, Pickford, Phil, Corrêa, Ivan R., Oishi, Atsuro, Jockers, Ralf, Inoue, Asuka, Kumar, Sunil, Görlitz, Frederik, Dunsby, Chris, French, Paul M.W., Rutter, Guy A., Tan, Tricia, Tomas, Alejandra, Bloom, Stephen R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Biochemistry and Molecular Biology 2020
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7948418/
https://www.ncbi.nlm.nih.gov/pubmed/33268378
http://dx.doi.org/10.1074/jbc.RA120.016334
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author Jones, Ben
McGlone, Emma Rose
Fang, Zijian
Pickford, Phil
Corrêa, Ivan R.
Oishi, Atsuro
Jockers, Ralf
Inoue, Asuka
Kumar, Sunil
Görlitz, Frederik
Dunsby, Chris
French, Paul M.W.
Rutter, Guy A.
Tan, Tricia
Tomas, Alejandra
Bloom, Stephen R.
author_facet Jones, Ben
McGlone, Emma Rose
Fang, Zijian
Pickford, Phil
Corrêa, Ivan R.
Oishi, Atsuro
Jockers, Ralf
Inoue, Asuka
Kumar, Sunil
Görlitz, Frederik
Dunsby, Chris
French, Paul M.W.
Rutter, Guy A.
Tan, Tricia
Tomas, Alejandra
Bloom, Stephen R.
author_sort Jones, Ben
collection PubMed
description Receptors for the peptide hormones glucagon-like peptide-1 (GLP-1R), glucose-dependent insulinotropic polypeptide (GIPR), and glucagon (GCGR) are important regulators of insulin secretion and energy metabolism. GLP-1R agonists have been successfully deployed for the treatment of type 2 diabetes, but it has been suggested that their efficacy is limited by target receptor desensitization and downregulation due to recruitment of β-arrestins. Indeed, recently described GLP-1R agonists with reduced β-arrestin-2 recruitment have delivered promising results in preclinical and clinical studies. We therefore aimed to determine if the same phenomenon could apply to the closely related GIPR and GCGR. In HEK293 cells depleted of both β-arrestin isoforms the duration of G protein–dependent cAMP/PKA signaling was increased in response to the endogenous ligand for each receptor. Moreover, in wildtype cells, “biased” GLP-1, GCG, and GIP analogs with selective reductions in β-arrestin-2 recruitment led to reduced receptor endocytosis and increased insulin secretion over a prolonged stimulation period, although the latter effect was only seen at high agonist concentrations. Biased GCG analogs increased the duration of cAMP signaling, but this did not lead to increased glucose output from hepatocytes. Our study provides a rationale for the development of GLP-1R, GIPR, and GCGR agonists with reduced β-arrestin recruitment, but further work is needed to maximally exploit this strategy for therapeutic purposes.
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spelling pubmed-79484182021-03-19 Genetic and biased agonist-mediated reductions in β-arrestin recruitment prolong cAMP signaling at glucagon family receptors Jones, Ben McGlone, Emma Rose Fang, Zijian Pickford, Phil Corrêa, Ivan R. Oishi, Atsuro Jockers, Ralf Inoue, Asuka Kumar, Sunil Görlitz, Frederik Dunsby, Chris French, Paul M.W. Rutter, Guy A. Tan, Tricia Tomas, Alejandra Bloom, Stephen R. J Biol Chem Research Article Receptors for the peptide hormones glucagon-like peptide-1 (GLP-1R), glucose-dependent insulinotropic polypeptide (GIPR), and glucagon (GCGR) are important regulators of insulin secretion and energy metabolism. GLP-1R agonists have been successfully deployed for the treatment of type 2 diabetes, but it has been suggested that their efficacy is limited by target receptor desensitization and downregulation due to recruitment of β-arrestins. Indeed, recently described GLP-1R agonists with reduced β-arrestin-2 recruitment have delivered promising results in preclinical and clinical studies. We therefore aimed to determine if the same phenomenon could apply to the closely related GIPR and GCGR. In HEK293 cells depleted of both β-arrestin isoforms the duration of G protein–dependent cAMP/PKA signaling was increased in response to the endogenous ligand for each receptor. Moreover, in wildtype cells, “biased” GLP-1, GCG, and GIP analogs with selective reductions in β-arrestin-2 recruitment led to reduced receptor endocytosis and increased insulin secretion over a prolonged stimulation period, although the latter effect was only seen at high agonist concentrations. Biased GCG analogs increased the duration of cAMP signaling, but this did not lead to increased glucose output from hepatocytes. Our study provides a rationale for the development of GLP-1R, GIPR, and GCGR agonists with reduced β-arrestin recruitment, but further work is needed to maximally exploit this strategy for therapeutic purposes. American Society for Biochemistry and Molecular Biology 2020-12-04 /pmc/articles/PMC7948418/ /pubmed/33268378 http://dx.doi.org/10.1074/jbc.RA120.016334 Text en © 2020 The Authors https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Article
Jones, Ben
McGlone, Emma Rose
Fang, Zijian
Pickford, Phil
Corrêa, Ivan R.
Oishi, Atsuro
Jockers, Ralf
Inoue, Asuka
Kumar, Sunil
Görlitz, Frederik
Dunsby, Chris
French, Paul M.W.
Rutter, Guy A.
Tan, Tricia
Tomas, Alejandra
Bloom, Stephen R.
Genetic and biased agonist-mediated reductions in β-arrestin recruitment prolong cAMP signaling at glucagon family receptors
title Genetic and biased agonist-mediated reductions in β-arrestin recruitment prolong cAMP signaling at glucagon family receptors
title_full Genetic and biased agonist-mediated reductions in β-arrestin recruitment prolong cAMP signaling at glucagon family receptors
title_fullStr Genetic and biased agonist-mediated reductions in β-arrestin recruitment prolong cAMP signaling at glucagon family receptors
title_full_unstemmed Genetic and biased agonist-mediated reductions in β-arrestin recruitment prolong cAMP signaling at glucagon family receptors
title_short Genetic and biased agonist-mediated reductions in β-arrestin recruitment prolong cAMP signaling at glucagon family receptors
title_sort genetic and biased agonist-mediated reductions in β-arrestin recruitment prolong camp signaling at glucagon family receptors
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7948418/
https://www.ncbi.nlm.nih.gov/pubmed/33268378
http://dx.doi.org/10.1074/jbc.RA120.016334
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