Author:
Zhang Yuxiang,Fang Bin,Damle Manashree,Guan Dongyin,Li Zhenghui,Kim Yong Hoon,Gannon Maureen,Lazar Mitchell A.
Abstract
Hepatocyte nuclear factor 6 (HNF6) is required for liver development, but its role in adult liver metabolism is not known. Here we show that deletion of HNF6 in livers of adult C57Bl/6 mice leads to hepatic steatosis in mice fed normal laboratory chow. Although HNF6 is known mainly as a transcriptional activator, hepatic loss of HNF6 up-regulated many lipogenic genes bound directly by HNF6. Many of these genes are targets of the circadian nuclear receptor Rev-erbα, and binding of Rev-erbα at these sites was lost when HNF6 was ablated in the liver. While HNF6 and Rev-erbα coordinately regulate hepatic lipid metabolism, each factor also affects additional gene sets independently. These findings highlight a novel mechanism of transcriptional repression by HNF6 and demonstrate how overlapping and distinct mechanisms of transcription factor function contribute to the integrated physiology of the liver.
Funder
National Institutes of Health
Cox Medical Research Institute
Publisher
Cold Spring Harbor Laboratory
Subject
Developmental Biology,Genetics
Cited by
53 articles.
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