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Diverse nucleosome Site-Selectivity among histone deacetylase complexes

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posted on 2021-03-18, 13:02 authored by Zhipeng A Wang, Christopher J Millard, Chia-Liang Lin, Jennifer E Gurnett, Mingxuan Wu, Kwangwoon Lee, Louise Fairall, John WR Schwabe, Philip A Cole
Histone acetylation regulates chromatin structure and gene expression and is removed by histone deacetylases (HDACs). HDACs are commonly found in various protein complexes to confer distinct cellular functions, but how the multi-subunit complexes influence deacetylase activities and site-selectivities in chromatin is poorly understood. Previously we reported the results of studies on the HDAC1 containing CoREST complex and acetylated nucleosome substrates which revealed a notable preference for deacetylation of histone H3 acetyl-Lys9 vs. acetyl-Lys14 (Wu et al, 2018). Here we analyze the enzymatic properties of five class I HDAC complexes: CoREST, NuRD, Sin3B, MiDAC and SMRT with site-specific acetylated nucleosome substrates. Our results demonstrate that these HDAC complexes show a wide variety of deacetylase rates in a site-selective manner. A Gly13 in the histone H3 tail is responsible for a sharp reduction in deacetylase activity of the CoREST complex for H3K14ac. These studies provide a framework for connecting enzymatic and biological functions of specific HDAC complexes.

Funding

NIH (GM62437)

Leukemia and Lymphoma Society (SCOR)

Wellcome Trust (100237/Z/12/Z)

History

Citation

eLife 2020;9:e57663 DOI: 10.7554/eLife.57663

Author affiliation

Department of Molecular and Cell Biology

Version

  • VoR (Version of Record)

Published in

eLife

Volume

9

Publisher

eLife Sciences Publications Ltd

issn

2050-084X

eissn

2050-084X

Acceptance date

2020-06-04

Copyright date

2020

Available date

2021-03-18

Spatial coverage

England

Language

English

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