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Examining How the MAFB Transcription Factor Affects Islet β-Cell Function Postnatally.
Citation | “Examining How The Mafb Transcription Factor Affects Islet Β-Cell Function Postnatally.”. Diabetes, pp. 337-348. . |
Center | Vanderbilt University |
Author | Holly A Cyphert, Emily M Walker, Yan Hang, Sangeeta Dhawan, Rachana Haliyur, Lauren Bonatakis, Dana Avrahami, Marcela Brissova, Klaus H Kaestner, Anil Bhushan, Alvin C Powers, Roland Stein |
Abstract |
The sustained expression of the MAFB transcription factor in human islet β-cells represents a distinct difference in mice. Moreover, mRNA expression of closely related and islet β-cell-enriched MAFA does not peak in humans until after 9 years of age. We show that the MAFA protein also is weakly produced within the juvenile human islet β-cell population and that expression is postnatally restricted in mouse β-cells by de novo DNA methylation. To gain insight into how MAFB affects human β-cells, we developed a mouse model to ectopically express in adult mouse β-cells using transcriptional control sequences. Coexpression of MafB with MafA had no overt impact on mouse β-cells, suggesting that the human adult β-cell MAFA/MAFB heterodimer is functionally equivalent to the mouse MafA homodimer. However, MafB alone was unable to rescue the islet β-cell defects in a mouse mutant lacking MafA in β-cells. Of note, transgenic production of MafB in β-cells elevated tryptophan hydroxylase 1 mRNA production during pregnancy, which drives the serotonin biosynthesis critical for adaptive maternal β-cell responses. Together, these studies provide novel insight into the role of MAFB in human islet β-cells. |
Year of Publication |
2019
|
Journal |
Diabetes
|
Volume |
68
|
Issue |
2
|
Number of Pages |
337-348
|
Date Published |
12/2019
|
ISSN Number |
1939-327X
|
DOI |
10.2337/db18-0903
|
Alternate Journal |
Diabetes
|
PMID |
30425060
|
PMCID |
PMC6341297
|
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