δ‐cells and β‐cells are electrically coupled and regulate α‐cell activity via somatostatin

KEY POINTS: We used a mouse expressing a light‐sensitive ion channel in β‐cells to understand how α‐cell activity is regulated by β‐cells. Light activation of β‐cells triggered a suppression of α‐cell activity via gap junction‐dependent activation of δ‐cells. Mathematical modelling of human islets s...

Descripción completa

Detalles Bibliográficos
Autores principales: Briant, L. J. B., Reinbothe, T. M., Spiliotis, I., Miranda, C., Rodriguez, B., Rorsman, P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2017
Materias:
Endocrine, Nutrition and Metabolism
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5767697/
https://www.ncbi.nlm.nih.gov/pubmed/28975620
http://dx.doi.org/10.1113/JP274581
_version_ 1783292576163430400
author Briant, L. J. B.
Reinbothe, T. M.
Spiliotis, I.
Miranda, C.
Rodriguez, B.
Rorsman, P.
author_facet Briant, L. J. B.
Reinbothe, T. M.
Spiliotis, I.
Miranda, C.
Rodriguez, B.
Rorsman, P.
author_sort Briant, L. J. B.
collection PubMed
description KEY POINTS: We used a mouse expressing a light‐sensitive ion channel in β‐cells to understand how α‐cell activity is regulated by β‐cells. Light activation of β‐cells triggered a suppression of α‐cell activity via gap junction‐dependent activation of δ‐cells. Mathematical modelling of human islets suggests that 23% of the inhibitory effect of glucose on glucagon secretion is mediated by β‐cells via gap junction‐dependent activation of δ‐cells/somatostatin secretion. ABSTRACT: Glucagon, the body's principal hyperglycaemic hormone, is released from α‐cells of the pancreatic islet. Secretion of this hormone is dysregulated in type 2 diabetes mellitus but the mechanisms controlling secretion are not well understood. Regulation of glucagon secretion by factors secreted by neighbouring β‐ and δ‐cells (paracrine regulation) have been proposed to be important. In this study, we explored the importance of paracrine regulation by using an optogenetic strategy. Specific light‐induced activation of β‐cells in mouse islets expressing the light‐gated channelrhodopsin‐2 resulted in stimulation of electrical activity in δ‐cells but suppression of α‐cell activity. Activation of the δ‐cells was rapid and sensitive to the gap junction inhibitor carbenoxolone, whereas the effect on electrical activity in α‐cells was blocked by CYN 154806, an antagonist of the somatostatin‐2 receptor. These observations indicate that optogenetic activation of the β‐cells propagates to the δ‐cells via gap junctions, and the consequential stimulation of somatostatin secretion inhibits α‐cell electrical activity by a paracrine mechanism. To explore whether this pathway is important for regulating α‐cell activity and glucagon secretion in human islets, we constructed computational models of human islets. These models had detailed architectures based on human islets and consisted of a collection of >500 α‐, β‐ and δ‐cells. Simulations of these models revealed that this gap junctional/paracrine mechanism accounts for up to 23% of the suppression of glucagon secretion by high glucose.
format Online
Article
Text
id pubmed-5767697
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher John Wiley and Sons Inc.
record_format MEDLINE/PubMed
spelling pubmed-57676972018-01-17 δ‐cells and β‐cells are electrically coupled and regulate α‐cell activity via somatostatin Briant, L. J. B. Reinbothe, T. M. Spiliotis, I. Miranda, C. Rodriguez, B. Rorsman, P. J Physiol Endocrine, Nutrition and Metabolism KEY POINTS: We used a mouse expressing a light‐sensitive ion channel in β‐cells to understand how α‐cell activity is regulated by β‐cells. Light activation of β‐cells triggered a suppression of α‐cell activity via gap junction‐dependent activation of δ‐cells. Mathematical modelling of human islets suggests that 23% of the inhibitory effect of glucose on glucagon secretion is mediated by β‐cells via gap junction‐dependent activation of δ‐cells/somatostatin secretion. ABSTRACT: Glucagon, the body's principal hyperglycaemic hormone, is released from α‐cells of the pancreatic islet. Secretion of this hormone is dysregulated in type 2 diabetes mellitus but the mechanisms controlling secretion are not well understood. Regulation of glucagon secretion by factors secreted by neighbouring β‐ and δ‐cells (paracrine regulation) have been proposed to be important. In this study, we explored the importance of paracrine regulation by using an optogenetic strategy. Specific light‐induced activation of β‐cells in mouse islets expressing the light‐gated channelrhodopsin‐2 resulted in stimulation of electrical activity in δ‐cells but suppression of α‐cell activity. Activation of the δ‐cells was rapid and sensitive to the gap junction inhibitor carbenoxolone, whereas the effect on electrical activity in α‐cells was blocked by CYN 154806, an antagonist of the somatostatin‐2 receptor. These observations indicate that optogenetic activation of the β‐cells propagates to the δ‐cells via gap junctions, and the consequential stimulation of somatostatin secretion inhibits α‐cell electrical activity by a paracrine mechanism. To explore whether this pathway is important for regulating α‐cell activity and glucagon secretion in human islets, we constructed computational models of human islets. These models had detailed architectures based on human islets and consisted of a collection of >500 α‐, β‐ and δ‐cells. Simulations of these models revealed that this gap junctional/paracrine mechanism accounts for up to 23% of the suppression of glucagon secretion by high glucose. John Wiley and Sons Inc. 2017-11-02 2018-01-15 /pmc/articles/PMC5767697/ /pubmed/28975620 http://dx.doi.org/10.1113/JP274581 Text en © 2017 University of Oxford. The Journal of Physiology published by John Wiley & Sons Ltd on behalf of The Physiological Society This is an open access article under the terms of the Creative Commons Attribution (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Endocrine, Nutrition and Metabolism
Briant, L. J. B.
Reinbothe, T. M.
Spiliotis, I.
Miranda, C.
Rodriguez, B.
Rorsman, P.
δ‐cells and β‐cells are electrically coupled and regulate α‐cell activity via somatostatin
title δ‐cells and β‐cells are electrically coupled and regulate α‐cell activity via somatostatin
title_full δ‐cells and β‐cells are electrically coupled and regulate α‐cell activity via somatostatin
title_fullStr δ‐cells and β‐cells are electrically coupled and regulate α‐cell activity via somatostatin
title_full_unstemmed δ‐cells and β‐cells are electrically coupled and regulate α‐cell activity via somatostatin
title_short δ‐cells and β‐cells are electrically coupled and regulate α‐cell activity via somatostatin
title_sort δ‐cells and β‐cells are electrically coupled and regulate α‐cell activity via somatostatin
topic Endocrine, Nutrition and Metabolism
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5767697/
https://www.ncbi.nlm.nih.gov/pubmed/28975620
http://dx.doi.org/10.1113/JP274581
work_keys_str_mv AT briantljb dcellsandbcellsareelectricallycoupledandregulateacellactivityviasomatostatin
AT reinbothetm dcellsandbcellsareelectricallycoupledandregulateacellactivityviasomatostatin
AT spiliotisi dcellsandbcellsareelectricallycoupledandregulateacellactivityviasomatostatin
AT mirandac dcellsandbcellsareelectricallycoupledandregulateacellactivityviasomatostatin
AT rodriguezb dcellsandbcellsareelectricallycoupledandregulateacellactivityviasomatostatin
AT rorsmanp dcellsandbcellsareelectricallycoupledandregulateacellactivityviasomatostatin

Ejemplares similares