A Functional Interaction between RIP140 and PGC-1α Regulates the Expression of the Lipid Droplet Protein CIDEA

Author:

Hallberg Magnus1,Morganstein Daniel L.1,Kiskinis Evangelos1,Shah Kunal1,Kralli Anastasia2,Dilworth Stephen M.1,White Roger1,Parker Malcolm G.1,Christian Mark1

Affiliation:

1. Institute of Reproductive and Developmental Biology, Faculty of Medicine, Imperial College London, Du Cane Road, London, United Kingdom W12 0NN

2. Department of Cell Biology, The Scripps Research Institute, La Jolla, California 92037

Abstract

ABSTRACT Nuclear receptors activate or repress target genes depending on the recruitment of coactivators or corepressors. The corepressor RIP140 and the PPAR coactivator 1α (PGC-1α) both play key roles in the regulated transcription of genes involved in energy homeostasis. We investigated the roles of RIP140 and PGC-1α in controlling the expression of CIDEA, an important regulatory factor in adipose cell function and obesity. Ectopically expressed CIDEA surrounded lipid droplets in brown adipocytes and induced the formation of lipid droplets in nonadipogenic cell lines. The expression and promoter activity of CIDEA was repressed by RIP140 and induced by PGC-1α, mediated through the binding of estrogen-related receptor α and NRF-1 to their cognate binding sites. Importantly, we demonstrate that RIP140 interacts directly with PGC-1α and suppresses its activity. The direct antagonism of PGC-1α by RIP140 provides a mechanism for regulating target gene transcription via nuclear receptor-dependent and -independent pathways.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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