Gliadin Fragments and a Specific Gliadin 33-mer Peptide Close K(ATP) Channels and Induce Insulin Secretion in INS-1E Cells and Rat Islets of Langerhans

In non-obese diabetic (NOD) mice, diabetes incidence is reduced by a gluten-free diet. Gluten peptides, such as the compound gliadin, can cross the intestinal barrier and may directly affect pancreatic beta cells. We investigated the effects of enzymatically-digested gliadin in NOD mice, INS-1E cell...

Descripción completa

Detalles Bibliográficos
Autores principales: Dall, Morten, Calloe, Kirstine, Haupt-Jorgensen, Martin, Larsen, Jesper, Schmitt, Nicole, Josefsen, Knud, Buschard, Karsten
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3681969/
https://www.ncbi.nlm.nih.gov/pubmed/23785500
http://dx.doi.org/10.1371/journal.pone.0066474
_version_ 1782273341625729024
author Dall, Morten
Calloe, Kirstine
Haupt-Jorgensen, Martin
Larsen, Jesper
Schmitt, Nicole
Josefsen, Knud
Buschard, Karsten
author_facet Dall, Morten
Calloe, Kirstine
Haupt-Jorgensen, Martin
Larsen, Jesper
Schmitt, Nicole
Josefsen, Knud
Buschard, Karsten
author_sort Dall, Morten
collection PubMed
description In non-obese diabetic (NOD) mice, diabetes incidence is reduced by a gluten-free diet. Gluten peptides, such as the compound gliadin, can cross the intestinal barrier and may directly affect pancreatic beta cells. We investigated the effects of enzymatically-digested gliadin in NOD mice, INS-1E cells and rat islets. Six injections of gliadin digest in 6-week-old NOD mice did not affect diabetes development, but increased weight gain (20% increase by day 100). In INS-1E cells, incubation with gliadin digest induced a dose-dependent increase in insulin secretion, up to 2.5-fold after 24 hours. A similar effect was observed in isolated rat islets (1.6-fold increase). In INS-1E cells, diazoxide reduced the stimulatory effect of gliadin digest. Additionally, gliadin digest was shown to decrease current through K(ATP)-channels. A specific gliadin 33-mer had a similar effect, both on current and insulin secretion. Finally, INS-1E incubation with gliadin digest potentiated palmitate-induced insulin secretion by 13% compared to controls. Our data suggest that gliadin fragments may contribute to the beta-cell hyperactivity observed prior to the development of type 1 diabetes.
format Online
Article
Text
id pubmed-3681969
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-36819692013-06-19 Gliadin Fragments and a Specific Gliadin 33-mer Peptide Close K(ATP) Channels and Induce Insulin Secretion in INS-1E Cells and Rat Islets of Langerhans Dall, Morten Calloe, Kirstine Haupt-Jorgensen, Martin Larsen, Jesper Schmitt, Nicole Josefsen, Knud Buschard, Karsten PLoS One Research Article In non-obese diabetic (NOD) mice, diabetes incidence is reduced by a gluten-free diet. Gluten peptides, such as the compound gliadin, can cross the intestinal barrier and may directly affect pancreatic beta cells. We investigated the effects of enzymatically-digested gliadin in NOD mice, INS-1E cells and rat islets. Six injections of gliadin digest in 6-week-old NOD mice did not affect diabetes development, but increased weight gain (20% increase by day 100). In INS-1E cells, incubation with gliadin digest induced a dose-dependent increase in insulin secretion, up to 2.5-fold after 24 hours. A similar effect was observed in isolated rat islets (1.6-fold increase). In INS-1E cells, diazoxide reduced the stimulatory effect of gliadin digest. Additionally, gliadin digest was shown to decrease current through K(ATP)-channels. A specific gliadin 33-mer had a similar effect, both on current and insulin secretion. Finally, INS-1E incubation with gliadin digest potentiated palmitate-induced insulin secretion by 13% compared to controls. Our data suggest that gliadin fragments may contribute to the beta-cell hyperactivity observed prior to the development of type 1 diabetes. Public Library of Science 2013-06-13 /pmc/articles/PMC3681969/ /pubmed/23785500 http://dx.doi.org/10.1371/journal.pone.0066474 Text en © 2013 Dall et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Dall, Morten
Calloe, Kirstine
Haupt-Jorgensen, Martin
Larsen, Jesper
Schmitt, Nicole
Josefsen, Knud
Buschard, Karsten
Gliadin Fragments and a Specific Gliadin 33-mer Peptide Close K(ATP) Channels and Induce Insulin Secretion in INS-1E Cells and Rat Islets of Langerhans
title Gliadin Fragments and a Specific Gliadin 33-mer Peptide Close K(ATP) Channels and Induce Insulin Secretion in INS-1E Cells and Rat Islets of Langerhans
title_full Gliadin Fragments and a Specific Gliadin 33-mer Peptide Close K(ATP) Channels and Induce Insulin Secretion in INS-1E Cells and Rat Islets of Langerhans
title_fullStr Gliadin Fragments and a Specific Gliadin 33-mer Peptide Close K(ATP) Channels and Induce Insulin Secretion in INS-1E Cells and Rat Islets of Langerhans
title_full_unstemmed Gliadin Fragments and a Specific Gliadin 33-mer Peptide Close K(ATP) Channels and Induce Insulin Secretion in INS-1E Cells and Rat Islets of Langerhans
title_short Gliadin Fragments and a Specific Gliadin 33-mer Peptide Close K(ATP) Channels and Induce Insulin Secretion in INS-1E Cells and Rat Islets of Langerhans
title_sort gliadin fragments and a specific gliadin 33-mer peptide close k(atp) channels and induce insulin secretion in ins-1e cells and rat islets of langerhans
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3681969/
https://www.ncbi.nlm.nih.gov/pubmed/23785500
http://dx.doi.org/10.1371/journal.pone.0066474
work_keys_str_mv AT dallmorten gliadinfragmentsandaspecificgliadin33merpeptideclosekatpchannelsandinduceinsulinsecretioninins1ecellsandratisletsoflangerhans
AT calloekirstine gliadinfragmentsandaspecificgliadin33merpeptideclosekatpchannelsandinduceinsulinsecretioninins1ecellsandratisletsoflangerhans
AT hauptjorgensenmartin gliadinfragmentsandaspecificgliadin33merpeptideclosekatpchannelsandinduceinsulinsecretioninins1ecellsandratisletsoflangerhans
AT larsenjesper gliadinfragmentsandaspecificgliadin33merpeptideclosekatpchannelsandinduceinsulinsecretioninins1ecellsandratisletsoflangerhans
AT schmittnicole gliadinfragmentsandaspecificgliadin33merpeptideclosekatpchannelsandinduceinsulinsecretioninins1ecellsandratisletsoflangerhans
AT josefsenknud gliadinfragmentsandaspecificgliadin33merpeptideclosekatpchannelsandinduceinsulinsecretioninins1ecellsandratisletsoflangerhans
AT buschardkarsten gliadinfragmentsandaspecificgliadin33merpeptideclosekatpchannelsandinduceinsulinsecretioninins1ecellsandratisletsoflangerhans

Ejemplares similares