4.8 Article

OCT4 interprets and enhances nucleosome flexibility

Journal

NUCLEIC ACIDS RESEARCH
Volume 50, Issue 18, Pages 10311-10327

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/nar/gkac755

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Funding

  1. Max Planck Society
  2. Royal Netherlands Academy of Arts and Sciences
  3. University of Utrecht
  4. Babes-Bolyai University
  5. Gauss Centre for Supercomputing e.V. [12622]

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Through experiments and molecular simulations, this study reveals how the pioneer factor Oct4 interprets and enhances nucleosome structural flexibility. Oct4 uses its DNA binding domains to propagate and stabilize open nucleosome conformations, providing a structural basis for the versatility of transcription factors' interaction with nucleosomes.
Pioneer transcription factors are proteins that induce cellular identity transitions by binding to inaccessible regions of DNA in nuclear chromatin. They contribute to chromatin opening and recruit other factors to regulatory DNA elements. The structural features and dynamics modulating their interaction with nucleosomes are still unresolved. From a combination of experiments and molecular simulations, we reveal here how the pioneer factor and master regulator of pluripotency, Oct4, interprets and enhances nucleosome structural flexibility. The magnitude of Oct4's impact on nucleosome dynamics depends on the binding site position and the mobility of the unstructured tails of nucleosomal histone proteins. Oct4 uses both its DNA binding domains to propagate and stabilize open nucleosome conformations, one for specific sequence recognition and the other for nonspecific interactions with nearby regions of DNA. Our findings provide a structural basis for the versatility of transcription factors in engaging with nucleosomes and have implications for understanding how pioneer factors induce chromatin dynamics.

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