Dynamic changes in β-cell [Ca(2+)] regulate NFAT activation, gene transcription, and islet gap junction communication

OBJECTIVE: Diabetes occurs because of insufficient insulin secretion due to β-cell dysfunction within the islet of Langerhans. Elevated glucose levels trigger β-cell membrane depolarization, action potential generation, and slow sustained free-Ca(2+) ([Ca(2+)]) oscillations, which trigger insulin re...

Descripción completa

Detalles Bibliográficos
Autores principales: Miranda, Jose G., Schleicher, Wolfgang E., Wells, Kristen L., Ramirez, David G., Landgrave, Samantha P., Benninger, Richard K.P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8804269/
https://www.ncbi.nlm.nih.gov/pubmed/34979329
http://dx.doi.org/10.1016/j.molmet.2021.101430
_version_ 1784643038961729536
author Miranda, Jose G.
Schleicher, Wolfgang E.
Wells, Kristen L.
Ramirez, David G.
Landgrave, Samantha P.
Benninger, Richard K.P.
author_facet Miranda, Jose G.
Schleicher, Wolfgang E.
Wells, Kristen L.
Ramirez, David G.
Landgrave, Samantha P.
Benninger, Richard K.P.
author_sort Miranda, Jose G.
collection PubMed
description OBJECTIVE: Diabetes occurs because of insufficient insulin secretion due to β-cell dysfunction within the islet of Langerhans. Elevated glucose levels trigger β-cell membrane depolarization, action potential generation, and slow sustained free-Ca(2+) ([Ca(2+)]) oscillations, which trigger insulin release. Nuclear factor of activated T-cell (NFAT) is a transcription factor, which is regulated by the increases in [Ca(2+)] and calceineurin (CaN) activation. NFAT regulation links cell activity with gene transcription in many systems and regulates proliferation and insulin granule biogenesis within the β-cell. However, the link between the regulation of β-cell electrical activity and oscillatory [Ca(2+)] dynamics with NFAT activation and downstream transcription is poorly understood. Here, we tested whether dynamic changes to β-cell electrical activity and [Ca(2+)] regulate NFAT activation and downstream transcription. METHODS: In cell lines, mouse islets, and human islets, including those from donors with type 2 diabetes, we applied both agonists/antagonists of ion channels together with optogenetics to modulate β-cell electrical activity. We measured the dynamics of [Ca(2+)] and NFAT activation as well as performed whole transcriptome and functional analyses. RESULTS: Both glucose-induced membrane depolarization and optogenetic stimulation triggered NFAT activation as well as increased the transcription of NFAT targets and intermediate early genes (IEGs). Importantly, slow, sustained [Ca(2+)] oscillation conditions led to NFAT activation and downstream transcription. In contrast, in human islets from donors with type2 diabetes, NFAT activation by glucose was diminished, but rescued upon pharmacological stimulation of electrical activity. NFAT activation regulated GJD2 expression and increased Cx36 gap junction permeability upon elevated oscillatory [Ca(2+)] dynamics. However, it is unclear if NFAT directly binds the GJD2 gene to regulate expression. CONCLUSIONS: This study provides an insight into the specific patterns of electrical activity that regulate NFAT activation, gene transcription, and islet function. In addition, it provides information on how these factors are disrupted in diabetes.
format Online
Article
Text
id pubmed-8804269
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-88042692022-02-04 Dynamic changes in β-cell [Ca(2+)] regulate NFAT activation, gene transcription, and islet gap junction communication Miranda, Jose G. Schleicher, Wolfgang E. Wells, Kristen L. Ramirez, David G. Landgrave, Samantha P. Benninger, Richard K.P. Mol Metab Original Article OBJECTIVE: Diabetes occurs because of insufficient insulin secretion due to β-cell dysfunction within the islet of Langerhans. Elevated glucose levels trigger β-cell membrane depolarization, action potential generation, and slow sustained free-Ca(2+) ([Ca(2+)]) oscillations, which trigger insulin release. Nuclear factor of activated T-cell (NFAT) is a transcription factor, which is regulated by the increases in [Ca(2+)] and calceineurin (CaN) activation. NFAT regulation links cell activity with gene transcription in many systems and regulates proliferation and insulin granule biogenesis within the β-cell. However, the link between the regulation of β-cell electrical activity and oscillatory [Ca(2+)] dynamics with NFAT activation and downstream transcription is poorly understood. Here, we tested whether dynamic changes to β-cell electrical activity and [Ca(2+)] regulate NFAT activation and downstream transcription. METHODS: In cell lines, mouse islets, and human islets, including those from donors with type 2 diabetes, we applied both agonists/antagonists of ion channels together with optogenetics to modulate β-cell electrical activity. We measured the dynamics of [Ca(2+)] and NFAT activation as well as performed whole transcriptome and functional analyses. RESULTS: Both glucose-induced membrane depolarization and optogenetic stimulation triggered NFAT activation as well as increased the transcription of NFAT targets and intermediate early genes (IEGs). Importantly, slow, sustained [Ca(2+)] oscillation conditions led to NFAT activation and downstream transcription. In contrast, in human islets from donors with type2 diabetes, NFAT activation by glucose was diminished, but rescued upon pharmacological stimulation of electrical activity. NFAT activation regulated GJD2 expression and increased Cx36 gap junction permeability upon elevated oscillatory [Ca(2+)] dynamics. However, it is unclear if NFAT directly binds the GJD2 gene to regulate expression. CONCLUSIONS: This study provides an insight into the specific patterns of electrical activity that regulate NFAT activation, gene transcription, and islet function. In addition, it provides information on how these factors are disrupted in diabetes. Elsevier 2021-12-31 /pmc/articles/PMC8804269/ /pubmed/34979329 http://dx.doi.org/10.1016/j.molmet.2021.101430 Text en © 2022 The Authors https://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
Miranda, Jose G.
Schleicher, Wolfgang E.
Wells, Kristen L.
Ramirez, David G.
Landgrave, Samantha P.
Benninger, Richard K.P.
Dynamic changes in β-cell [Ca(2+)] regulate NFAT activation, gene transcription, and islet gap junction communication
title Dynamic changes in β-cell [Ca(2+)] regulate NFAT activation, gene transcription, and islet gap junction communication
title_full Dynamic changes in β-cell [Ca(2+)] regulate NFAT activation, gene transcription, and islet gap junction communication
title_fullStr Dynamic changes in β-cell [Ca(2+)] regulate NFAT activation, gene transcription, and islet gap junction communication
title_full_unstemmed Dynamic changes in β-cell [Ca(2+)] regulate NFAT activation, gene transcription, and islet gap junction communication
title_short Dynamic changes in β-cell [Ca(2+)] regulate NFAT activation, gene transcription, and islet gap junction communication
title_sort dynamic changes in β-cell [ca(2+)] regulate nfat activation, gene transcription, and islet gap junction communication
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8804269/
https://www.ncbi.nlm.nih.gov/pubmed/34979329
http://dx.doi.org/10.1016/j.molmet.2021.101430
work_keys_str_mv AT mirandajoseg dynamicchangesinbcellca2regulatenfatactivationgenetranscriptionandisletgapjunctioncommunication
AT schleicherwolfgange dynamicchangesinbcellca2regulatenfatactivationgenetranscriptionandisletgapjunctioncommunication
AT wellskristenl dynamicchangesinbcellca2regulatenfatactivationgenetranscriptionandisletgapjunctioncommunication
AT ramirezdavidg dynamicchangesinbcellca2regulatenfatactivationgenetranscriptionandisletgapjunctioncommunication
AT landgravesamanthap dynamicchangesinbcellca2regulatenfatactivationgenetranscriptionandisletgapjunctioncommunication
AT benningerrichardkp dynamicchangesinbcellca2regulatenfatactivationgenetranscriptionandisletgapjunctioncommunication

Ejemplares similares