Transcription coactivator mediator subunit MED1 is required for the development of fatty liver in the mouse

Liang Bai; Yuzhi Jia; Navin Viswakarma; Jiansheng Huang; Aurore Vluggens; Nathan E Wolins; Nadereh Jafari; M Sambasiva Rao; Jayme Borensztajn; Gongshe Yang; Janardan K Reddy

doi:10.1002/hep.24155

Transcription coactivator mediator subunit MED1 is required for the development of fatty liver in the mouse

Hepatology. 2011 Apr;53(4):1164-74. doi: 10.1002/hep.24155.

Authors

Liang Bai¹, Yuzhi Jia, Navin Viswakarma, Jiansheng Huang, Aurore Vluggens, Nathan E Wolins, Nadereh Jafari, M Sambasiva Rao, Jayme Borensztajn, Gongshe Yang, Janardan K Reddy

Affiliation

¹ Department of Pathology, Feinberg School of Medicine, Northwestern University, Chicago, IL; Laboratory of Animal Fat Deposition and Muscle Development, College of Animal Science and Technology, Northwest A&F University, Shaanxi, China.

Abstract

Peroxisome proliferator-activated receptor-γ (PPARγ), a nuclear receptor, when overexpressed in liver stimulates the induction of adipocyte-specific and lipogenesis-related genes and causes hepatic steatosis. We report here that Mediator 1 (MED1; also known as PBP or TRAP220), a key subunit of the Mediator complex, is required for high-fat diet-induced hepatic steatosis as well as PPARγ-stimulated adipogenic hepatic steatosis. Mediator forms the bridge between transcriptional activators and RNA polymerase II. MED1 interacts with nuclear receptors such as PPARγ and other transcriptional activators. Liver-specific MED1 knockout (MED1(ΔLiv) ) mice, when fed a high-fat (60% kcal fat) diet for up to 4 months failed to develop fatty liver. Similarly, MED1(ΔLiv) mice injected with adenovirus-PPARγ (Ad/PPARγ) by tail vein also did not develop fatty liver, whereas mice with MED1 (MED1(fl/fl) ) fed a high-fat diet or injected with Ad/PPARγ developed severe hepatic steatosis. Gene expression profiling and northern blot analyses of Ad/PPARγ-injected mouse livers showed impaired induction in MED1(ΔLiv) mouse liver of adipogenic markers, such as aP2, adipsin, adiponectin, and lipid droplet-associated genes, including caveolin-1, CideA, S3-12, and others. These adipocyte-specific and lipogenesis-related genes are strongly induced in MED1(fl/fl) mouse liver in response to Ad/PPARγ. Re-expression of MED1 using adenovirally-driven MED1 (Ad/MED1) in MED1(ΔLiv) mouse liver restored PPARγ-stimulated hepatic adipogenic response. These studies also demonstrate that disruption of genes encoding other coactivators such as SRC-1, PRIC285, PRIP, and PIMT had no effect on hepatic adipogenesis induced by PPARγ overexpression.

Conclusion: We conclude that transcription coactivator MED1 is required for high-fat diet-induced and PPARγ-stimulated fatty liver development, which suggests that MED1 may be considered a potential therapeutic target for hepatic steatosis. (HEPATOLOGY 2011;).

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Dietary Fats / administration & dosage
Fatty Liver / etiology*
Gene Expression Profiling
Genes, Regulator
Mediator Complex Subunit 1 / deficiency
Mediator Complex Subunit 1 / physiology*
Mice
PPAR gamma / biosynthesis
PPAR gamma / pharmacology

Substances

Dietary Fats
Mediator Complex Subunit 1
PPAR gamma

Abstract

Publication types

MeSH terms

Substances

Grants and funding