4.7 Article

The USR domain of USF1 mediates NF-Y interactions and cooperative DNA binding

Journal

INTERNATIONAL JOURNAL OF BIOLOGICAL MACROMOLECULES
Volume 193, Issue -, Pages 401-413

Publisher

ELSEVIER
DOI: 10.1016/j.ijbiomac.2021.10.056

Keywords

Trans-activation domain; SAXS; Intrinsically disordered region; Protein-DNA interactions; DNA-binding domain

Funding

  1. Fondazione AIRC per la Ricerca sul Cancro grants [IG-19050, IG-15267]
  2. Ministry of Science and Higher Education of the Russian Federation within the State assignment FSRC 'Crystallography and Photonics' of the Russian Academy of Sciences

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NF-Y cooperates with USF1 in DNA binding and jointly activates target promoters. Certain unstructured domains adapt to small variations in stereo-alignments of TF sites.
The trimeric CCAAT-binding NF-Y is a pioneer Transcription Factor -TF-known to cooperate with neighboring TFs to regulate gene expression. Genome-wide analyses detected a precise stereo-alignment-10/12 bp-of CCAAT with E-box elements and corresponding colocalization of NF-Y with basic-Helix-Loop-Helix (bHLH) TFs. We dissected here NF-Y interactions with USF1 and MAX. USF1, but not MAX, cooperates in DNA binding with NF-Y. NF-Y and USF1 synergize to activate target promoters. Reconstruction of complexes by structural means shows independent DNA binding of MAX, whereas USF1 has extended contacts with NF-Y, involving the USR, a USFspecific amino acid sequence stretch required for trans-activation. The USR is an intrinsically disordered domain and adopts different conformations based on E-box-CCAAT distances. Deletion of the USR abolishes cooperative DNA binding with NF-Y. Our data indicate that the functionality of certain unstructured domains involves adapting to small variation in stereo-alignments of the multimeric TFs sites.

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