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Publication : Changes in nucleosome occupancy associated with metabolic alterations in aged mammalian liver.

First Author  Bochkis IM Year  2014
Journal  Cell Rep Volume  9
Issue  3 Pages  996-1006
PubMed ID  25437555 Mgi Jnum  J:218603
Mgi Id  MGI:5618035 Doi  10.1016/j.celrep.2014.09.048
Citation  Bochkis IM, et al. (2014) Changes in nucleosome occupancy associated with metabolic alterations in aged mammalian liver. Cell Rep 9(3):996-1006
abstractText  Aging is accompanied by physiological impairments, which, in insulin-responsive tissues, including the liver, predispose individuals to metabolic disease. However, the molecular mechanisms underlying these changes remain largely unknown. Here, we analyze genome-wide profiles of RNA and chromatin organization in the liver of young (3 months) and old (21 months) mice. Transcriptional changes suggest that derepression of the nuclear receptors PPARalpha, PPARgamma, and LXRalpha in aged mouse liver leads to activation of targets regulating lipid synthesis and storage, whereas age-dependent changes in nucleosome occupancy are associated with binding sites for both known regulators (forkhead factors and nuclear receptors) and candidates associated with nuclear lamina (Hdac3 and Srf) implicated to govern metabolic function of aging liver. Winged-helix transcription factor Foxa2 and nuclear receptor corepressor Hdac3 exhibit a reciprocal binding pattern at PPARalpha targets contributing to gene expression changes that lead to steatosis in aged liver.
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