DNA Methylation–Dependent Restriction of Tyrosine Hydroxylase Contributes to Pancreatic β-Cell Heterogeneity

The molecular and functional heterogeneity of pancreatic β-cells is well recognized, but the underlying mechanisms remain unclear. Pancreatic islets harbor a subset of β-cells that co-express tyrosine hydroxylase (TH), an enzyme involved in synthesis of catecholamines that repress insulin secretion....

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Autores principales: Parveen, Nazia, Wang, Jean Kimi, Bhattacharya, Supriyo, Cuala, Janielle, Rajkumar, Mohan Singh, Butler, Alexandra E., Wu, Xiwei, Shih, Hung-Ping, Georgia, Senta K., Dhawan, Sangeeta
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Diabetes Association 2023
Materias:
Islet Studies
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10130487/
https://www.ncbi.nlm.nih.gov/pubmed/36607262
http://dx.doi.org/10.2337/db22-0506
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author Parveen, Nazia
Wang, Jean Kimi
Bhattacharya, Supriyo
Cuala, Janielle
Rajkumar, Mohan Singh
Butler, Alexandra E.
Wu, Xiwei
Shih, Hung-Ping
Georgia, Senta K.
Dhawan, Sangeeta
author_facet Parveen, Nazia
Wang, Jean Kimi
Bhattacharya, Supriyo
Cuala, Janielle
Rajkumar, Mohan Singh
Butler, Alexandra E.
Wu, Xiwei
Shih, Hung-Ping
Georgia, Senta K.
Dhawan, Sangeeta
author_sort Parveen, Nazia
collection PubMed
description The molecular and functional heterogeneity of pancreatic β-cells is well recognized, but the underlying mechanisms remain unclear. Pancreatic islets harbor a subset of β-cells that co-express tyrosine hydroxylase (TH), an enzyme involved in synthesis of catecholamines that repress insulin secretion. Restriction of the TH(+) β-cells within islets is essential for appropriate function in mice, such that a higher proportion of these cells corresponds to reduced insulin secretion. Here, we use these cells as a model to dissect the developmental control of β-cell heterogeneity. We define the specific molecular and metabolic characteristics of TH(+) β-cells and show differences in their developmental restriction in mice and humans. We show that TH expression in β-cells is restricted by DNA methylation during β-cell differentiation. Ablation of de novo DNA methyltransferase Dnmt3a in the embryonic progenitors results in a dramatic increase in the proportion of TH(+) β-cells, whereas β-cell–specific ablation of Dnmt3a does not. We demonstrate that maintenance of Th promoter methylation is essential for its continued restriction in postnatal β-cells. Loss of Th promoter methylation in response to chronic overnutrition increases the number of TH(+) β-cells, corresponding to impaired β-cell function. These results reveal a regulatory role of DNA methylation in determining β-cell heterogeneity.
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spelling pubmed-101304872023-04-27 DNA Methylation–Dependent Restriction of Tyrosine Hydroxylase Contributes to Pancreatic β-Cell Heterogeneity Parveen, Nazia Wang, Jean Kimi Bhattacharya, Supriyo Cuala, Janielle Rajkumar, Mohan Singh Butler, Alexandra E. Wu, Xiwei Shih, Hung-Ping Georgia, Senta K. Dhawan, Sangeeta Diabetes Islet Studies The molecular and functional heterogeneity of pancreatic β-cells is well recognized, but the underlying mechanisms remain unclear. Pancreatic islets harbor a subset of β-cells that co-express tyrosine hydroxylase (TH), an enzyme involved in synthesis of catecholamines that repress insulin secretion. Restriction of the TH(+) β-cells within islets is essential for appropriate function in mice, such that a higher proportion of these cells corresponds to reduced insulin secretion. Here, we use these cells as a model to dissect the developmental control of β-cell heterogeneity. We define the specific molecular and metabolic characteristics of TH(+) β-cells and show differences in their developmental restriction in mice and humans. We show that TH expression in β-cells is restricted by DNA methylation during β-cell differentiation. Ablation of de novo DNA methyltransferase Dnmt3a in the embryonic progenitors results in a dramatic increase in the proportion of TH(+) β-cells, whereas β-cell–specific ablation of Dnmt3a does not. We demonstrate that maintenance of Th promoter methylation is essential for its continued restriction in postnatal β-cells. Loss of Th promoter methylation in response to chronic overnutrition increases the number of TH(+) β-cells, corresponding to impaired β-cell function. These results reveal a regulatory role of DNA methylation in determining β-cell heterogeneity. American Diabetes Association 2023-05 2023-01-06 /pmc/articles/PMC10130487/ /pubmed/36607262 http://dx.doi.org/10.2337/db22-0506 Text en © 2023 by the American Diabetes Association https://www.diabetesjournals.org/journals/pages/licenseReaders may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered. More information is available at https://www.diabetesjournals.org/journals/pages/license.
spellingShingle Islet Studies
Parveen, Nazia
Wang, Jean Kimi
Bhattacharya, Supriyo
Cuala, Janielle
Rajkumar, Mohan Singh
Butler, Alexandra E.
Wu, Xiwei
Shih, Hung-Ping
Georgia, Senta K.
Dhawan, Sangeeta
DNA Methylation–Dependent Restriction of Tyrosine Hydroxylase Contributes to Pancreatic β-Cell Heterogeneity
title DNA Methylation–Dependent Restriction of Tyrosine Hydroxylase Contributes to Pancreatic β-Cell Heterogeneity
title_full DNA Methylation–Dependent Restriction of Tyrosine Hydroxylase Contributes to Pancreatic β-Cell Heterogeneity
title_fullStr DNA Methylation–Dependent Restriction of Tyrosine Hydroxylase Contributes to Pancreatic β-Cell Heterogeneity
title_full_unstemmed DNA Methylation–Dependent Restriction of Tyrosine Hydroxylase Contributes to Pancreatic β-Cell Heterogeneity
title_short DNA Methylation–Dependent Restriction of Tyrosine Hydroxylase Contributes to Pancreatic β-Cell Heterogeneity
title_sort dna methylation–dependent restriction of tyrosine hydroxylase contributes to pancreatic β-cell heterogeneity
topic Islet Studies
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10130487/
https://www.ncbi.nlm.nih.gov/pubmed/36607262
http://dx.doi.org/10.2337/db22-0506
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