| Literature DB >> 34784250 |
Arturo Mendoza1, Catherine Tang2, Jinyoung Choi1, Mariana Acuña3, Maya Logan1, Adriana G Martin1, Lujain Al-Sowaimel2, Bhavna N Desai2, Danielle E Tenen2, Christopher Jacobs2, Anna Lyubetskaya2, Yulong Fu4, Hong Liu4, Linus Tsai2, David E Cohen3, Douglas Forrest4, Andrew A Wilson5, Anthony N Hollenberg1.
Abstract
Thyroid hormone (TH) action is essential for hepatic lipid synthesis and oxidation. Analysis of hepatocyte-specific thyroid receptor β1 (TRβ1) knockout mice confirmed a role for TH in stimulating de novo lipogenesis and fatty acid oxidation through its nuclear receptor. Specifically, TRβ1 and its principal corepressor NCoR1 in hepatocytes repressed de novo lipogenesis, whereas the TH-mediated induction of lipogenic genes depended on the transcription factor ChREBP. Mice with a hepatocyte-specific deficiency in ChREBP lost TH-mediated stimulation of the lipogenic program, which, in turn, impaired the regulation of fatty acid oxidation. TH regulated ChREBP activation and recruitment to DNA, revealing a mechanism by which TH regulates specific signaling pathways. Regulation of the lipogenic pathway by TH through ChREBP was conserved in hepatocytes derived from human induced pluripotent stem cells. These results demonstrate that TH signaling in the liver acts simultaneously to enhance both lipogenesis and fatty acid oxidation.Entities:
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Year: 2021 PMID: 34784250 PMCID: PMC8853622 DOI: 10.1126/scisignal.abh3839
Source DB: PubMed Journal: Sci Signal ISSN: 1945-0877 Impact factor: 8.192