Xenin-25 Amplifies GIP-Mediated Insulin Secretion in Humans With Normal and Impaired Glucose Tolerance but Not Type 2 Diabetes

Glucose-dependent insulinotropic polypeptide (GIP) potentiates glucose-stimulated insulin secretion (GSIS). This response is blunted in type 2 diabetes (T2DM). Xenin-25 is a 25–amino acid neurotensin-related peptide that amplifies GIP-mediated GSIS in hyperglycemic mice. This study determines if xen...

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Autores principales: Wice, Burton M., Reeds, Dominic N., Tran, Hung D., Crimmins, Dan L., Patterson, Bruce W., Dunai, Judit, Wallendorf, Michael J., Ladenson, Jack H., Villareal, Dennis T., Polonsky, Kenneth S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Diabetes Association 2012
Materias:
Pathophysiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3379667/
https://www.ncbi.nlm.nih.gov/pubmed/22522617
http://dx.doi.org/10.2337/db11-1451
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author Wice, Burton M.
Reeds, Dominic N.
Tran, Hung D.
Crimmins, Dan L.
Patterson, Bruce W.
Dunai, Judit
Wallendorf, Michael J.
Ladenson, Jack H.
Villareal, Dennis T.
Polonsky, Kenneth S.
author_facet Wice, Burton M.
Reeds, Dominic N.
Tran, Hung D.
Crimmins, Dan L.
Patterson, Bruce W.
Dunai, Judit
Wallendorf, Michael J.
Ladenson, Jack H.
Villareal, Dennis T.
Polonsky, Kenneth S.
author_sort Wice, Burton M.
collection PubMed
description Glucose-dependent insulinotropic polypeptide (GIP) potentiates glucose-stimulated insulin secretion (GSIS). This response is blunted in type 2 diabetes (T2DM). Xenin-25 is a 25–amino acid neurotensin-related peptide that amplifies GIP-mediated GSIS in hyperglycemic mice. This study determines if xenin-25 amplifies GIP-mediated GSIS in humans with normal glucose tolerance (NGT), impaired glucose tolerance (IGT), or T2DM. Each fasting subject received graded glucose infusions to progressively raise plasma glucose concentrations, along with vehicle alone, GIP, xenin-25, or GIP plus xenin-25. Plasma glucose, insulin, C-peptide, and glucagon levels and insulin secretion rates (ISRs) were determined. GIP amplified GSIS in all groups. Initially, this response was rapid, profound, transient, and essentially glucose independent. Thereafter, ISRs increased as a function of plasma glucose. Although magnitudes of insulin secretory responses to GIP were similar in all groups, ISRs were not restored to normal in subjects with IGT and T2DM. Xenin-25 alone had no effect on ISRs or plasma glucagon levels, but the combination of GIP plus xenin-25 transiently increased ISR and plasma glucagon levels in subjects with NGT and IGT but not T2DM. Since xenin-25 signaling to islets is mediated by a cholinergic relay, impaired islet responses in T2DM may reflect defective neuronal, rather than GIP, signaling.
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spelling pubmed-33796672013-07-01 Xenin-25 Amplifies GIP-Mediated Insulin Secretion in Humans With Normal and Impaired Glucose Tolerance but Not Type 2 Diabetes Wice, Burton M. Reeds, Dominic N. Tran, Hung D. Crimmins, Dan L. Patterson, Bruce W. Dunai, Judit Wallendorf, Michael J. Ladenson, Jack H. Villareal, Dennis T. Polonsky, Kenneth S. Diabetes Pathophysiology Glucose-dependent insulinotropic polypeptide (GIP) potentiates glucose-stimulated insulin secretion (GSIS). This response is blunted in type 2 diabetes (T2DM). Xenin-25 is a 25–amino acid neurotensin-related peptide that amplifies GIP-mediated GSIS in hyperglycemic mice. This study determines if xenin-25 amplifies GIP-mediated GSIS in humans with normal glucose tolerance (NGT), impaired glucose tolerance (IGT), or T2DM. Each fasting subject received graded glucose infusions to progressively raise plasma glucose concentrations, along with vehicle alone, GIP, xenin-25, or GIP plus xenin-25. Plasma glucose, insulin, C-peptide, and glucagon levels and insulin secretion rates (ISRs) were determined. GIP amplified GSIS in all groups. Initially, this response was rapid, profound, transient, and essentially glucose independent. Thereafter, ISRs increased as a function of plasma glucose. Although magnitudes of insulin secretory responses to GIP were similar in all groups, ISRs were not restored to normal in subjects with IGT and T2DM. Xenin-25 alone had no effect on ISRs or plasma glucagon levels, but the combination of GIP plus xenin-25 transiently increased ISR and plasma glucagon levels in subjects with NGT and IGT but not T2DM. Since xenin-25 signaling to islets is mediated by a cholinergic relay, impaired islet responses in T2DM may reflect defective neuronal, rather than GIP, signaling. American Diabetes Association 2012-07 2012-06-15 /pmc/articles/PMC3379667/ /pubmed/22522617 http://dx.doi.org/10.2337/db11-1451 Text en © 2012 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered. See http://creativecommons.org/licenses/by-nc-nd/3.0/ for details.
spellingShingle Pathophysiology
Wice, Burton M.
Reeds, Dominic N.
Tran, Hung D.
Crimmins, Dan L.
Patterson, Bruce W.
Dunai, Judit
Wallendorf, Michael J.
Ladenson, Jack H.
Villareal, Dennis T.
Polonsky, Kenneth S.
Xenin-25 Amplifies GIP-Mediated Insulin Secretion in Humans With Normal and Impaired Glucose Tolerance but Not Type 2 Diabetes
title Xenin-25 Amplifies GIP-Mediated Insulin Secretion in Humans With Normal and Impaired Glucose Tolerance but Not Type 2 Diabetes
title_full Xenin-25 Amplifies GIP-Mediated Insulin Secretion in Humans With Normal and Impaired Glucose Tolerance but Not Type 2 Diabetes
title_fullStr Xenin-25 Amplifies GIP-Mediated Insulin Secretion in Humans With Normal and Impaired Glucose Tolerance but Not Type 2 Diabetes
title_full_unstemmed Xenin-25 Amplifies GIP-Mediated Insulin Secretion in Humans With Normal and Impaired Glucose Tolerance but Not Type 2 Diabetes
title_short Xenin-25 Amplifies GIP-Mediated Insulin Secretion in Humans With Normal and Impaired Glucose Tolerance but Not Type 2 Diabetes
title_sort xenin-25 amplifies gip-mediated insulin secretion in humans with normal and impaired glucose tolerance but not type 2 diabetes
topic Pathophysiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3379667/
https://www.ncbi.nlm.nih.gov/pubmed/22522617
http://dx.doi.org/10.2337/db11-1451
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