GPR92 activation in islet macrophages controls β cell function in a diet-induced obesity model

The molecular mechanisms underlying obesity-induced increases in β cell mass and the resulting β cell dysfunction need to be elucidated further. Our study revealed that GPR92, expressed in islet macrophages, is modulated by dietary interventions in metabolic tissues. Therefore, we aimed to define th...

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Autores principales: de Souza, Camila O., Paschoal, Vivian A., Sun, Xuenan, Vishvanath, Lavanya, Zhang, Qianbin, Shao, Mengle, Onodera, Toshiharu, Chen, Shiuhwei, Joffin, Nolwenn, Bueno, Lorena M.A., Gupta, Rana K., Oh, Da Young
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Clinical Investigation 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9621135/
https://www.ncbi.nlm.nih.gov/pubmed/36066975
http://dx.doi.org/10.1172/JCI160097
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author de Souza, Camila O.
Paschoal, Vivian A.
Sun, Xuenan
Vishvanath, Lavanya
Zhang, Qianbin
Shao, Mengle
Onodera, Toshiharu
Chen, Shiuhwei
Joffin, Nolwenn
Bueno, Lorena M.A.
Gupta, Rana K.
Oh, Da Young
author_facet de Souza, Camila O.
Paschoal, Vivian A.
Sun, Xuenan
Vishvanath, Lavanya
Zhang, Qianbin
Shao, Mengle
Onodera, Toshiharu
Chen, Shiuhwei
Joffin, Nolwenn
Bueno, Lorena M.A.
Gupta, Rana K.
Oh, Da Young
author_sort de Souza, Camila O.
collection PubMed
description The molecular mechanisms underlying obesity-induced increases in β cell mass and the resulting β cell dysfunction need to be elucidated further. Our study revealed that GPR92, expressed in islet macrophages, is modulated by dietary interventions in metabolic tissues. Therefore, we aimed to define the role of GPR92 in islet inflammation by using a high-fat diet–induced (HFD-induced) obese mouse model. GPR92-KO mice exhibited glucose intolerance and reduced insulin levels — despite the enlarged pancreatic islets — as well as increased islet macrophage content and inflammation level compared with WT mice. These results indicate that the lack of GPR92 in islet macrophages can cause β cell dysfunction, leading to disrupted glucose homeostasis. Alternatively, stimulation with the GPR92 agonist farnesyl pyrophosphate results in the inhibition of HFD-induced islet inflammation and increased insulin secretion in WT mice, but not in GPR92-KO mice. Thus, our study suggests that GPR92 can be a potential target to alleviate β cell dysfunction via the inhibition of islet inflammation associated with the progression of diabetes.
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spelling pubmed-96211352022-11-03 GPR92 activation in islet macrophages controls β cell function in a diet-induced obesity model de Souza, Camila O. Paschoal, Vivian A. Sun, Xuenan Vishvanath, Lavanya Zhang, Qianbin Shao, Mengle Onodera, Toshiharu Chen, Shiuhwei Joffin, Nolwenn Bueno, Lorena M.A. Gupta, Rana K. Oh, Da Young J Clin Invest Research Article The molecular mechanisms underlying obesity-induced increases in β cell mass and the resulting β cell dysfunction need to be elucidated further. Our study revealed that GPR92, expressed in islet macrophages, is modulated by dietary interventions in metabolic tissues. Therefore, we aimed to define the role of GPR92 in islet inflammation by using a high-fat diet–induced (HFD-induced) obese mouse model. GPR92-KO mice exhibited glucose intolerance and reduced insulin levels — despite the enlarged pancreatic islets — as well as increased islet macrophage content and inflammation level compared with WT mice. These results indicate that the lack of GPR92 in islet macrophages can cause β cell dysfunction, leading to disrupted glucose homeostasis. Alternatively, stimulation with the GPR92 agonist farnesyl pyrophosphate results in the inhibition of HFD-induced islet inflammation and increased insulin secretion in WT mice, but not in GPR92-KO mice. Thus, our study suggests that GPR92 can be a potential target to alleviate β cell dysfunction via the inhibition of islet inflammation associated with the progression of diabetes. American Society for Clinical Investigation 2022-11-01 /pmc/articles/PMC9621135/ /pubmed/36066975 http://dx.doi.org/10.1172/JCI160097 Text en © 2022 de Souza et al. https://creativecommons.org/licenses/by/4.0/This work is licensed under the Creative Commons Attribution 4.0 International License. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
de Souza, Camila O.
Paschoal, Vivian A.
Sun, Xuenan
Vishvanath, Lavanya
Zhang, Qianbin
Shao, Mengle
Onodera, Toshiharu
Chen, Shiuhwei
Joffin, Nolwenn
Bueno, Lorena M.A.
Gupta, Rana K.
Oh, Da Young
GPR92 activation in islet macrophages controls β cell function in a diet-induced obesity model
title GPR92 activation in islet macrophages controls β cell function in a diet-induced obesity model
title_full GPR92 activation in islet macrophages controls β cell function in a diet-induced obesity model
title_fullStr GPR92 activation in islet macrophages controls β cell function in a diet-induced obesity model
title_full_unstemmed GPR92 activation in islet macrophages controls β cell function in a diet-induced obesity model
title_short GPR92 activation in islet macrophages controls β cell function in a diet-induced obesity model
title_sort gpr92 activation in islet macrophages controls β cell function in a diet-induced obesity model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9621135/
https://www.ncbi.nlm.nih.gov/pubmed/36066975
http://dx.doi.org/10.1172/JCI160097
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