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Publication : MED1 is a lipogenesis coactivator required for postnatal adipose expansion.

First Author  Jang Y Year  2021
Journal  Genes Dev Volume  35
Issue  9-10 Pages  713-728
PubMed ID  33888555 Mgi Jnum  J:314174
Mgi Id  MGI:6814636 Doi  10.1101/gad.347583.120
Citation  Jang Y, et al. (2021) MED1 is a lipogenesis coactivator required for postnatal adipose expansion. Genes Dev 35(9-10):713-728
abstractText  MED1 often serves as a surrogate of the general transcription coactivator complex Mediator for identifying active enhancers. MED1 is required for phenotypic conversion of fibroblasts to adipocytes in vitro, but its role in adipose development and expansion in vivo has not been reported. Here, we show that MED1 is not generally required for transcription during adipogenesis in culture and that MED1 is dispensable for adipose development in mice. Instead, MED1 is required for postnatal adipose expansion and the induction of fatty acid and triglyceride synthesis genes after pups switch diet from high-fat maternal milk to carbohydrate-based chow. During adipogenesis, MED1 is dispensable for induction of lineage-determining transcription factors (TFs) PPARgamma and C/EBPalpha but is required for lipid accumulation in the late phase of differentiation. Mechanistically, MED1 controls the induction of lipogenesis genes by facilitating lipogenic TF ChREBP- and SREBP1a-dependent recruitment of Mediator to active enhancers. Together, our fi ndings identify a cell- and gene-specific regulatory role of MED1 as a lipogenesis coactivator required for postnatal adipose expansion.
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