Free fatty acid receptor 4 inhibitory signaling in delta cells regulates islet hormone secretion in mice

OBJECTIVE: Maintenance of glucose homeostasis requires the precise regulation of hormone secretion from the endocrine pancreas. Free fatty acid receptor 4 (FFAR4/GPR120) is a G protein-coupled receptor whose activation in islets of Langerhans promotes insulin and glucagon secretion and inhibits soma...

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Autores principales: Croze, Marine L., Flisher, Marcus F., Guillaume, Arthur, Tremblay, Caroline, Noguchi, Glyn M., Granziera, Sabrina, Vivot, Kevin, Castillo, Vincent C., Campbell, Scott A., Ghislain, Julien, Huising, Mark O., Poitout, Vincent
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
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Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7873385/
https://www.ncbi.nlm.nih.gov/pubmed/33484949
http://dx.doi.org/10.1016/j.molmet.2021.101166
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author Croze, Marine L.
Flisher, Marcus F.
Guillaume, Arthur
Tremblay, Caroline
Noguchi, Glyn M.
Granziera, Sabrina
Vivot, Kevin
Castillo, Vincent C.
Campbell, Scott A.
Ghislain, Julien
Huising, Mark O.
Poitout, Vincent
author_facet Croze, Marine L.
Flisher, Marcus F.
Guillaume, Arthur
Tremblay, Caroline
Noguchi, Glyn M.
Granziera, Sabrina
Vivot, Kevin
Castillo, Vincent C.
Campbell, Scott A.
Ghislain, Julien
Huising, Mark O.
Poitout, Vincent
author_sort Croze, Marine L.
collection PubMed
description OBJECTIVE: Maintenance of glucose homeostasis requires the precise regulation of hormone secretion from the endocrine pancreas. Free fatty acid receptor 4 (FFAR4/GPR120) is a G protein-coupled receptor whose activation in islets of Langerhans promotes insulin and glucagon secretion and inhibits somatostatin secretion. However, the contribution of individual islet cell types (α, β, and δ cells) to the insulinotropic and glucagonotropic effects of GPR120 remains unclear. As gpr120 mRNA is enriched in somatostatin-secreting δ cells, we hypothesized that GPR120 activation stimulates insulin and glucagon secretion via inhibition of somatostatin release. METHODS: Glucose tolerance tests were performed in mice after administration of selective GPR120 agonist Compound A. Insulin, glucagon, and somatostatin secretion were measured in static incubations of isolated mouse islets in response to endogenous (ω-3 polyunsaturated fatty acids) and/or pharmacological (Compound A and AZ-13581837) GPR120 agonists. The effect of Compound A on hormone secretion was tested further in islets isolated from mice with global or somatostatin cell-specific knock-out of gpr120. Gpr120 expression was assessed in pancreatic sections by RNA in situ hybridization. Cyclic AMP (cAMP) and calcium dynamics in response to pharmacological GPR120 agonists were measured specifically in α, β, and δ cells in intact islets using cAMPER and GCaMP6 reporter mice, respectively. RESULTS: Acute exposure to Compound A increased glucose tolerance, circulating insulin, and glucagon levels in vivo. Endogenous and/or pharmacological GPR120 agonists reduced somatostatin secretion in isolated islets and concomitantly demonstrated dose-dependent potentiation of glucose-stimulated insulin secretion and arginine-stimulated glucagon secretion. Gpr120 was enriched in δ cells. Pharmacological GPR120 agonists reduced cAMP and calcium levels in δ cells but increased these signals in α and β cells. Compound A-mediated inhibition of somatostatin secretion was insensitive to pertussis toxin. The effect of Compound A on hormone secretion was completely absent in islets from mice with either global or somatostatin cell-specific deletion of gpr120 and partially reduced upon blockade of somatostatin receptor signaling by cyclosomatostatin. CONCLUSIONS: Inhibitory GPR120 signaling in δ cells contributes to both insulin and glucagon secretion in part by mitigating somatostatin release.
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spelling pubmed-78733852021-02-17 Free fatty acid receptor 4 inhibitory signaling in delta cells regulates islet hormone secretion in mice Croze, Marine L. Flisher, Marcus F. Guillaume, Arthur Tremblay, Caroline Noguchi, Glyn M. Granziera, Sabrina Vivot, Kevin Castillo, Vincent C. Campbell, Scott A. Ghislain, Julien Huising, Mark O. Poitout, Vincent Mol Metab Original Article OBJECTIVE: Maintenance of glucose homeostasis requires the precise regulation of hormone secretion from the endocrine pancreas. Free fatty acid receptor 4 (FFAR4/GPR120) is a G protein-coupled receptor whose activation in islets of Langerhans promotes insulin and glucagon secretion and inhibits somatostatin secretion. However, the contribution of individual islet cell types (α, β, and δ cells) to the insulinotropic and glucagonotropic effects of GPR120 remains unclear. As gpr120 mRNA is enriched in somatostatin-secreting δ cells, we hypothesized that GPR120 activation stimulates insulin and glucagon secretion via inhibition of somatostatin release. METHODS: Glucose tolerance tests were performed in mice after administration of selective GPR120 agonist Compound A. Insulin, glucagon, and somatostatin secretion were measured in static incubations of isolated mouse islets in response to endogenous (ω-3 polyunsaturated fatty acids) and/or pharmacological (Compound A and AZ-13581837) GPR120 agonists. The effect of Compound A on hormone secretion was tested further in islets isolated from mice with global or somatostatin cell-specific knock-out of gpr120. Gpr120 expression was assessed in pancreatic sections by RNA in situ hybridization. Cyclic AMP (cAMP) and calcium dynamics in response to pharmacological GPR120 agonists were measured specifically in α, β, and δ cells in intact islets using cAMPER and GCaMP6 reporter mice, respectively. RESULTS: Acute exposure to Compound A increased glucose tolerance, circulating insulin, and glucagon levels in vivo. Endogenous and/or pharmacological GPR120 agonists reduced somatostatin secretion in isolated islets and concomitantly demonstrated dose-dependent potentiation of glucose-stimulated insulin secretion and arginine-stimulated glucagon secretion. Gpr120 was enriched in δ cells. Pharmacological GPR120 agonists reduced cAMP and calcium levels in δ cells but increased these signals in α and β cells. Compound A-mediated inhibition of somatostatin secretion was insensitive to pertussis toxin. The effect of Compound A on hormone secretion was completely absent in islets from mice with either global or somatostatin cell-specific deletion of gpr120 and partially reduced upon blockade of somatostatin receptor signaling by cyclosomatostatin. CONCLUSIONS: Inhibitory GPR120 signaling in δ cells contributes to both insulin and glucagon secretion in part by mitigating somatostatin release. Elsevier 2021-01-20 /pmc/articles/PMC7873385/ /pubmed/33484949 http://dx.doi.org/10.1016/j.molmet.2021.101166 Text en © 2021 The Author(s) http://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
Croze, Marine L.
Flisher, Marcus F.
Guillaume, Arthur
Tremblay, Caroline
Noguchi, Glyn M.
Granziera, Sabrina
Vivot, Kevin
Castillo, Vincent C.
Campbell, Scott A.
Ghislain, Julien
Huising, Mark O.
Poitout, Vincent
Free fatty acid receptor 4 inhibitory signaling in delta cells regulates islet hormone secretion in mice
title Free fatty acid receptor 4 inhibitory signaling in delta cells regulates islet hormone secretion in mice
title_full Free fatty acid receptor 4 inhibitory signaling in delta cells regulates islet hormone secretion in mice
title_fullStr Free fatty acid receptor 4 inhibitory signaling in delta cells regulates islet hormone secretion in mice
title_full_unstemmed Free fatty acid receptor 4 inhibitory signaling in delta cells regulates islet hormone secretion in mice
title_short Free fatty acid receptor 4 inhibitory signaling in delta cells regulates islet hormone secretion in mice
title_sort free fatty acid receptor 4 inhibitory signaling in delta cells regulates islet hormone secretion in mice
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7873385/
https://www.ncbi.nlm.nih.gov/pubmed/33484949
http://dx.doi.org/10.1016/j.molmet.2021.101166
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