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Coregulator Sin3a Promotes Postnatal Murine β-Cell Fitness by Regulating Genes in Ca Homeostasis, Cell Survival, Vesicle Biosynthesis, Glucose Metabolism, and Stress Response.

Citation
Yang, X., et al. “Coregulator Sin3A Promotes Postnatal Murine Β-Cell Fitness By Regulating Genes In Ca Homeostasis, Cell Survival, Vesicle Biosynthesis, Glucose Metabolism, And Stress Response.”. Diabetes, pp. 1219-1231.
Center Vanderbilt University
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Author Xiaodun Yang, Sarah M Graff, Cody N Heiser, Kung-Hsien Ho, Bob Chen, Alan J Simmons, Austin N Southard-Smith, Gregory David, David A Jacobson, Irina Kaverina, Christopher E Wright V, Ken S Lau, Guoqiang Gu
Abstract

Swi-independent 3a and 3b (Sin3a and Sin3b) are paralogous transcriptional coregulators that direct cellular differentiation, survival, and function. Here, we report that mouse Sin3a and Sin3b are coproduced in most pancreatic cells during embryogenesis but become much more enriched in endocrine cells in adults, implying continued essential roles in mature endocrine cell function. Mice with loss of in endocrine progenitors were normal during early postnatal stages but gradually developed diabetes before weaning. These physiological defects were preceded by the compromised survival, insulin-vesicle packaging, insulin secretion, and nutrient-induced Ca influx of -deficient β-cells. RNA sequencing coupled with candidate chromatin immunoprecipitation assays revealed several genes that could be directly regulated by Sin3a in β-cells, which modulate Ca/ion transport, cell survival, vesicle/membrane trafficking, glucose metabolism, and stress responses. Finally, mice with loss of both and in multipotent embryonic pancreatic progenitors had significantly reduced islet cell mass at birth, caused by decreased endocrine progenitor production and increased β-cell death. These findings highlight the stage-specific requirements for the presumed "general" coregulators Sin3a and Sin3b in islet β-cells, with Sin3a being dispensable for differentiation but required for postnatal function and survival.

Year of Publication
2020
Journal
Diabetes
Volume
69
Issue
6
Number of Pages
1219-1231
Date Published
06/2020
ISSN Number
1939-327X
DOI
10.2337/db19-0721
Alternate Journal
Diabetes
PMID
32245798
PMCID
PMC7243292
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