Absence of cannabinoid 1 receptor in beta cells protects against high-fat/high-sugar diet-induced beta cell dysfunction and inflammation in murine islets

AIMS/HYPOTHESIS: The cannabinoid 1 receptor (CB1R) regulates insulin sensitivity and glucose metabolism in peripheral tissues. CB1R is expressed on pancreatic beta cells and is coupled to the G protein Gαi, suggesting a negative regulation of endogenous signalling in the beta cell. Deciphering the e...

Descripción completa

Detalles Bibliográficos
Autores principales: González-Mariscal, Isabel, Montoro, Rodrigo A., Doyle, Máire E., Liu, Qing-Rong, Rouse, Michael, O’Connell, Jennifer F., Santa-Cruz Calvo, Sara, Krzysik-Walker, Susan M., Ghosh, Soumita, Carlson, Olga D., Lehrmann, Elin, Zhang, Yongqing, Becker, Kevin G., Chia, Chee W., Ghosh, Paritosh, Egan, Josephine M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Berlin Heidelberg 2018
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6201315/
https://www.ncbi.nlm.nih.gov/pubmed/29497784
http://dx.doi.org/10.1007/s00125-018-4576-4
_version_ 1783365471970525184
author González-Mariscal, Isabel
Montoro, Rodrigo A.
Doyle, Máire E.
Liu, Qing-Rong
Rouse, Michael
O’Connell, Jennifer F.
Santa-Cruz Calvo, Sara
Krzysik-Walker, Susan M.
Ghosh, Soumita
Carlson, Olga D.
Lehrmann, Elin
Zhang, Yongqing
Becker, Kevin G.
Chia, Chee W.
Ghosh, Paritosh
Egan, Josephine M.
author_facet González-Mariscal, Isabel
Montoro, Rodrigo A.
Doyle, Máire E.
Liu, Qing-Rong
Rouse, Michael
O’Connell, Jennifer F.
Santa-Cruz Calvo, Sara
Krzysik-Walker, Susan M.
Ghosh, Soumita
Carlson, Olga D.
Lehrmann, Elin
Zhang, Yongqing
Becker, Kevin G.
Chia, Chee W.
Ghosh, Paritosh
Egan, Josephine M.
author_sort González-Mariscal, Isabel
collection PubMed
description AIMS/HYPOTHESIS: The cannabinoid 1 receptor (CB1R) regulates insulin sensitivity and glucose metabolism in peripheral tissues. CB1R is expressed on pancreatic beta cells and is coupled to the G protein Gαi, suggesting a negative regulation of endogenous signalling in the beta cell. Deciphering the exact function of CB1R in beta cells has been confounded by the expression of this receptor on multiple tissues involved in regulating metabolism. Thus, in models of global genetic or pharmacological CB1R blockade, it is difficult to distinguish the indirect effects of improved insulin sensitivity in peripheral tissues from the direct effects of inhibiting CB1R in beta cells per se. To assess the direct contribution of beta cell CB1R to metabolism, we designed a mouse model that allows us to determine the role of CB1R specifically in beta cells in the context of whole-body metabolism. METHODS: We generated a beta cell specific Cnr1 (CB1R) knockout mouse (β-CB1R(−/−)) to study the long-term consequences of CB1R ablation on beta cell function in adult mice. We measured beta cell function, proliferation and viability in these mice in response to a high-fat/high-sugar diet and induction of acute insulin resistance with the insulin receptor antagonist S961. RESULTS: β-CB1R(−/−) mice had increased fasting (153 ± 23% increase at 10 weeks of age) and stimulated insulin secretion and increased intra-islet cAMP levels (217 ± 33% increase at 10 weeks of age), resulting in primary hyperinsulinaemia, as well as increased beta cell viability, proliferation and islet area (1.9-fold increase at 10 weeks of age). Hyperinsulinaemia led to insulin resistance, which was aggravated by a high-fat/high-sugar diet and weight gain, although beta cells maintained their insulin secretory capacity in response to glucose. Strikingly, islets from β-CB1R(−/−) mice were protected from diet-induced inflammation. Mechanistically, we show that this is a consequence of curtailment of oxidative stress and reduced activation of the NLRP3 inflammasome in beta cells. CONCLUSIONS/INTERPRETATION: Our data demonstrate CB1R to be a negative regulator of beta cell function and a mediator of islet inflammation under conditions of metabolic stress. Our findings point to beta cell CB1R as a therapeutic target, and broaden its potential to include anti-inflammatory effects in both major forms of diabetes. DATA AVAILABILITY: Microarray data have been deposited at GEO (GSE102027). ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s00125-018-4576-4) contains peer-reviewed but unedited supplementary material, which is available to authorised users.
format Online
Article
Text
id pubmed-6201315
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher Springer Berlin Heidelberg
record_format MEDLINE/PubMed
spelling pubmed-62013152018-12-01 Absence of cannabinoid 1 receptor in beta cells protects against high-fat/high-sugar diet-induced beta cell dysfunction and inflammation in murine islets González-Mariscal, Isabel Montoro, Rodrigo A. Doyle, Máire E. Liu, Qing-Rong Rouse, Michael O’Connell, Jennifer F. Santa-Cruz Calvo, Sara Krzysik-Walker, Susan M. Ghosh, Soumita Carlson, Olga D. Lehrmann, Elin Zhang, Yongqing Becker, Kevin G. Chia, Chee W. Ghosh, Paritosh Egan, Josephine M. Diabetologia Article AIMS/HYPOTHESIS: The cannabinoid 1 receptor (CB1R) regulates insulin sensitivity and glucose metabolism in peripheral tissues. CB1R is expressed on pancreatic beta cells and is coupled to the G protein Gαi, suggesting a negative regulation of endogenous signalling in the beta cell. Deciphering the exact function of CB1R in beta cells has been confounded by the expression of this receptor on multiple tissues involved in regulating metabolism. Thus, in models of global genetic or pharmacological CB1R blockade, it is difficult to distinguish the indirect effects of improved insulin sensitivity in peripheral tissues from the direct effects of inhibiting CB1R in beta cells per se. To assess the direct contribution of beta cell CB1R to metabolism, we designed a mouse model that allows us to determine the role of CB1R specifically in beta cells in the context of whole-body metabolism. METHODS: We generated a beta cell specific Cnr1 (CB1R) knockout mouse (β-CB1R(−/−)) to study the long-term consequences of CB1R ablation on beta cell function in adult mice. We measured beta cell function, proliferation and viability in these mice in response to a high-fat/high-sugar diet and induction of acute insulin resistance with the insulin receptor antagonist S961. RESULTS: β-CB1R(−/−) mice had increased fasting (153 ± 23% increase at 10 weeks of age) and stimulated insulin secretion and increased intra-islet cAMP levels (217 ± 33% increase at 10 weeks of age), resulting in primary hyperinsulinaemia, as well as increased beta cell viability, proliferation and islet area (1.9-fold increase at 10 weeks of age). Hyperinsulinaemia led to insulin resistance, which was aggravated by a high-fat/high-sugar diet and weight gain, although beta cells maintained their insulin secretory capacity in response to glucose. Strikingly, islets from β-CB1R(−/−) mice were protected from diet-induced inflammation. Mechanistically, we show that this is a consequence of curtailment of oxidative stress and reduced activation of the NLRP3 inflammasome in beta cells. CONCLUSIONS/INTERPRETATION: Our data demonstrate CB1R to be a negative regulator of beta cell function and a mediator of islet inflammation under conditions of metabolic stress. Our findings point to beta cell CB1R as a therapeutic target, and broaden its potential to include anti-inflammatory effects in both major forms of diabetes. DATA AVAILABILITY: Microarray data have been deposited at GEO (GSE102027). ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s00125-018-4576-4) contains peer-reviewed but unedited supplementary material, which is available to authorised users. Springer Berlin Heidelberg 2018-03-01 2018 /pmc/articles/PMC6201315/ /pubmed/29497784 http://dx.doi.org/10.1007/s00125-018-4576-4 Text en © The Author(s) 2018 Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.
spellingShingle Article
González-Mariscal, Isabel
Montoro, Rodrigo A.
Doyle, Máire E.
Liu, Qing-Rong
Rouse, Michael
O’Connell, Jennifer F.
Santa-Cruz Calvo, Sara
Krzysik-Walker, Susan M.
Ghosh, Soumita
Carlson, Olga D.
Lehrmann, Elin
Zhang, Yongqing
Becker, Kevin G.
Chia, Chee W.
Ghosh, Paritosh
Egan, Josephine M.
Absence of cannabinoid 1 receptor in beta cells protects against high-fat/high-sugar diet-induced beta cell dysfunction and inflammation in murine islets
title Absence of cannabinoid 1 receptor in beta cells protects against high-fat/high-sugar diet-induced beta cell dysfunction and inflammation in murine islets
title_full Absence of cannabinoid 1 receptor in beta cells protects against high-fat/high-sugar diet-induced beta cell dysfunction and inflammation in murine islets
title_fullStr Absence of cannabinoid 1 receptor in beta cells protects against high-fat/high-sugar diet-induced beta cell dysfunction and inflammation in murine islets
title_full_unstemmed Absence of cannabinoid 1 receptor in beta cells protects against high-fat/high-sugar diet-induced beta cell dysfunction and inflammation in murine islets
title_short Absence of cannabinoid 1 receptor in beta cells protects against high-fat/high-sugar diet-induced beta cell dysfunction and inflammation in murine islets
title_sort absence of cannabinoid 1 receptor in beta cells protects against high-fat/high-sugar diet-induced beta cell dysfunction and inflammation in murine islets
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6201315/
https://www.ncbi.nlm.nih.gov/pubmed/29497784
http://dx.doi.org/10.1007/s00125-018-4576-4
work_keys_str_mv AT gonzalezmariscalisabel absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT montororodrigoa absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT doylemairee absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT liuqingrong absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT rousemichael absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT oconnelljenniferf absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT santacruzcalvosara absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT krzysikwalkersusanm absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT ghoshsoumita absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT carlsonolgad absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT lehrmannelin absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT zhangyongqing absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT beckerkeving absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT chiacheew absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT ghoshparitosh absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets
AT eganjosephinem absenceofcannabinoid1receptorinbetacellsprotectsagainsthighfathighsugardietinducedbetacelldysfunctionandinflammationinmurineislets

Ejemplares similares