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Structural and Functional Impacts of ER Coactivator Sequential Recruitment.

Molecular cell | 2017

Nuclear receptors recruit multiple coactivators sequentially to activate transcription. This "ordered" recruitment allows different coactivator activities to engage the nuclear receptor complex at different steps of transcription. Estrogen receptor (ER) recruits steroid receptor coactivator-3 (SRC-3) primary coactivator and secondary coactivators, p300/CBP and CARM1. CARM1 recruitment lags behind the binding of SRC-3 and p300 to ER. Combining cryo-electron microscopy (cryo-EM) structure analysis and biochemical approaches, we demonstrate that there is a close crosstalk between early- and late-recruited coactivators. The sequential recruitment of CARM1 not only adds a protein arginine methyltransferase activity to the ER-coactivator complex, it also alters the structural organization of the pre-existing ERE/ERα/SRC-3/p300 complex. It induces a p300 conformational change and significantly increases p300 HAT activity on histone H3K18 residues, which, in turn, promotes CARM1 methylation activity on H3R17 residues to enhance transcriptional activity. This study reveals a structural role for a coactivator sequential recruitment and biochemical process in ER-mediated transcription.

Pubmed ID: 28844863 RIS Download

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Associated grants

  • Agency: NIGMS NIH HHS, United States
    Id: P41 GM103832
  • Agency: NIGMS NIH HHS, United States
    Id: R01 GM079429
  • Agency: NIGMS NIH HHS, United States
    Id: R01 GM072804
  • Agency: NIDDK NIH HHS, United States
    Id: P01 DK059820
  • Agency: NICHD NIH HHS, United States
    Id: R01 HD008188
  • Agency: NCI NIH HHS, United States
    Id: P30 CA125123
  • Agency: NIAID NIH HHS, United States
    Id: R21 AI122418

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