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VGLL4 and MENIN function as TEAD1 corepressors to block pancreatic β cell proliferation.


ABSTRACT: TEAD1 and the mammalian Hippo pathway regulate cellular proliferation and function, though their regulatory function in β cells remains poorly characterized. In this study, we demonstrate that while β cell-specific TEAD1 deletion results in a cell-autonomous increase of β cell proliferation, β cell-specific deletion of its canonical coactivators, YAP and TAZ, does not affect proliferation, suggesting the involvement of other cofactors. Using an improved split-GFP system and yeast two-hybrid platform, we identify VGLL4 and MENIN as TEAD1 corepressors in β cells. We show that VGLL4 and MENIN bind to TEAD1 and repress the expression of target genes, including FZD7 and CCN2, which leads to an inhibition of β cell proliferation. In conclusion, we demonstrate that TEAD1 plays a critical role in β cell proliferation and identify VGLL4 and MENIN as TEAD1 corepressors in β cells. We propose that these could be targeted to augment proliferation in β cells for reversing diabetes.

SUBMITTER: Li F 

PROVIDER: S-EPMC9970006 | biostudies-literature | 2023 Jan

REPOSITORIES: biostudies-literature

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VGLL4 and MENIN function as TEAD1 corepressors to block pancreatic β cell proliferation.

Li Feng F   Liu Ruya R   Negi Vinny V   Yang Ping P   Lee Jeongkyung J   Jagannathan Rajaganapathi R   Moulik Mousumi M   Yechoor Vijay K VK  

Cell reports 20230119 1


TEAD1 and the mammalian Hippo pathway regulate cellular proliferation and function, though their regulatory function in β cells remains poorly characterized. In this study, we demonstrate that while β cell-specific TEAD1 deletion results in a cell-autonomous increase of β cell proliferation, β cell-specific deletion of its canonical coactivators, YAP and TAZ, does not affect proliferation, suggesting the involvement of other cofactors. Using an improved split-GFP system and yeast two-hybrid plat  ...[more]

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