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Date publication

avril 2018

Journal

FEBS letters

Auteurs

Membres identifiés du Cancéropôle Est :
Dr ROCHETTE-EGLY Cécile


Tous les auteurs :
Carrier M, Lutzing R, Gaouar S, Rochette-Egly C

Résumé

The nuclear retinoic acid (RA) receptors (RARα, β and γ) are ligand-dependent regulators of transcription. Upon activation by RA, they are recruited at the promoters of target genes together with several coregulators. Then, they are degraded by the ubiquitin proteasome system. Here, we report that the degradation of the RARα subtype involves ubiquitination and the tripartite motif protein TRIM24, which was originally identified as a ligand-dependent corepressor of RARα. We show that in response to RA, TRIM24 serves as an adapter linking RARα to the proteasome for its degradation. In addition, TRIM24 and the proteasome are recruited with RARα to the promoters of target genes and thus are inherently linked to RARα transcriptional activity.

Mots clés

TRIM24, degradation, proteasome, retinoic acid receptor, transcription, ubiquitin

Référence

FEBS Lett.. 2018 Apr;592(8):1426-1433

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