Molecular determinants of MED1 interaction with the DNA bound VDR–RXR heterodimer

辅活化剂 视黄醇X受体 核受体 骨化三醇受体 生物 调解人 核受体辅活化子2 核受体辅活化子3 核受体辅活化子1 细胞生物学 遗传学 生物化学 转录因子 受体 基因
作者
Anna Y. Belorusova,Maxime Bourguet,Steve Hessmann,Sandra Chalhoub,Bruno Kieffer,Sarah Cianférani,Natacha Rochel
出处
期刊:Nucleic Acids Research [Oxford University Press]
卷期号:48 (19): 11199-11213 被引量:13
标识
DOI:10.1093/nar/gkaa775
摘要

Abstract The MED1 subunit of the Mediator complex is an essential coactivator of nuclear receptor-mediated transcriptional activation. While structural requirements for ligand-dependent binding of classical coactivator motifs of MED1 to numerous nuclear receptor ligand-binding domains have been fully elucidated, the recognition of the full-length or truncated coactivator by full nuclear receptor complexes remain unknown. Here we present structural details of the interaction between a large part of MED1 comprising its structured N-terminal and the flexible receptor-interacting domains and the mutual heterodimer of the vitamin D receptor (VDR) and the retinoid X receptor (RXR) bound to their cognate DNA response element. Using a combination of structural and biophysical methods we show that the ligand-dependent interaction between VDR and the second coactivator motif of MED1 is crucial for complex formation and we identify additional, previously unseen, interaction details. In particular, we identified RXR regions involved in the interaction with the structured N-terminal domain of MED1, as well as VDR regions outside the classical coactivator binding cleft affected by coactivator recruitment. These findings highlight important roles of each receptor within the heterodimer in selective recognition of MED1 and contribute to our understanding of the nuclear receptor-coregulator complexes.

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