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PPAR?/? recruits NCOR and regulates transcription reinitiation of ANGPTL4.


ABSTRACT: In the absence of ligands, the nuclear receptor PPAR?/? recruits the NCOR and SMRT corepressors, which form complexes with HDAC3, to canonical target genes. Agonistic ligands cause dissociation of corepressors and enable enhanced transcription. Vice versa, synthetic inverse agonists augment corepressor recruitment and repression. Both basal repression of the target gene ANGPTL4 and reinforced repression elicited by inverse agonists are partially insensitive to HDAC inhibition. This raises the question how PPAR?/? represses transcription mechanistically. We show that the PPAR?/? inverse agonist PT-S264 impairs transcription initiation by decreasing recruitment of activating Mediator subunits, RNA polymerase II, and TFIIB, but not of TFIIA, to the ANGPTL4 promoter. Mass spectrometry identifies NCOR as the main PT-S264-dependent interactor of PPAR?/?. Reconstitution of knockout cells with PPAR?/? mutants deficient in basal repression results in diminished recruitment of NCOR, SMRT, and HDAC3 to PPAR target genes, while occupancy by RNA polymerase II is increased. PT-S264 restores binding of NCOR, SMRT, and HDAC3 to the mutants, resulting in reduced polymerase II occupancy. Our findings corroborate deacetylase-dependent and -independent repressive functions of HDAC3-containing complexes, which act in parallel to downregulate transcription.

SUBMITTER: Legrand N 

PROVIDER: S-EPMC6765110 | biostudies-literature | 2019 Oct

REPOSITORIES: biostudies-literature

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PPARβ/δ recruits NCOR and regulates transcription reinitiation of ANGPTL4.

Legrand Nathalie N   Bretscher Clemens L CL   Zielke Svenja S   Wilke Bernhard B   Daude Michael M   Fritz Barbara B   Diederich Wibke E WE   Adhikary Till T  

Nucleic acids research 20191001 18


In the absence of ligands, the nuclear receptor PPARβ/δ recruits the NCOR and SMRT corepressors, which form complexes with HDAC3, to canonical target genes. Agonistic ligands cause dissociation of corepressors and enable enhanced transcription. Vice versa, synthetic inverse agonists augment corepressor recruitment and repression. Both basal repression of the target gene ANGPTL4 and reinforced repression elicited by inverse agonists are partially insensitive to HDAC inhibition. This raises the qu  ...[more]

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