Binding of PHF1 Tudor to H3K36me3 enhances nucleosome accessibility

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作者
Catherine A. Musselman
Matthew D. Gibson
Erik W. Hartwick
Justin A. North
Jovylyn Gatchalian
Michael G. Poirier
Tatiana G. Kutateladze
机构
[1] University of Colorado School of Medicine,Department of Pharmacology
[2] Ohio State University,Department of Physics
[3] Program in Structural Biology and Biochemistry,undefined
[4] University of Colorado School of Medicine,undefined
[5] Present address: Department of Biochemistry,undefined
[6] University of Iowa,undefined
[7] Iowa City,undefined
[8] Iowa 52242,undefined
[9] USA,undefined
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The Tudor domain of human PHF1 recognizes trimethylated lysine 36 of histone H3 (H3K36me3). This interaction modulates the methyltransferase activity of the PRC2 complex and has a role in retention of PHF1 at DNA damage sites. We have previously determined the structural basis for the association of Tudor with a methylated histone peptide. Here we detail the molecular mechanism of binding of the Tudor domain to the H3KC36me3-nucleosome core particle (H3KC36me3-NCP). Using a combination of TROSY NMR and FRET, we show that Tudor concomitantly interacts with H3K36me3 and DNA. Binding of the PHF1 Tudor domain to the H3KC36me3-NCP stabilizes the nucleosome in a conformation in which the nucleosomal DNA is more accessible to DNA-binding regulatory proteins. Our data provide a mechanistic explanation for the consequence of reading of the active mark H3K36me3 by the PHF1 Tudor domain.
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