Literature DB >> 31527837

DNA repair complex licenses acetylation of H2A.Z.1 by KAT2A during transcription.

M Semer1,2,3,4, B Bidon1,2,3,4, A Larnicol1,2,3,4, G Caliskan1,2,3,4,5, P Catez1,2,3,4, J M Egly1,2,3,4, F Coin6,7,8,9, N Le May10,11,12,13.   

Abstract

Post-translational modifications of histone variant H2A.Z accompany gene transactivation, but its modifying enzymes still remain elusive. Here, we reveal a hitherto unknown function of human KAT2A (GCN5) as a histone acetyltransferase (HAT) of H2A.Z at the promoters of a set of transactivated genes. Expression of these genes also depends on the DNA repair complex XPC-RAD23-CEN2. We established that XPC-RAD23-CEN2 interacts both with H2A.Z and KAT2A to drive the recruitment of the HAT at promoters and license H2A.Z acetylation. KAT2A selectively acetylates H2A.Z.1 versus H2A.Z.2 in vitro on several well-defined lysines and we unveiled that alanine-14 in H2A.Z.2 is responsible for inhibiting the activity of KAT2A. Notably, the use of a nonacetylable H2A.Z.1 mutant shows that H2A.Z.1ac recruits the epigenetic reader BRD2 to promote RNA polymerase II recruitment. Our studies identify KAT2A as an H2A.Z.1 HAT in mammals and implicate XPC-RAD23-CEN2 as a transcriptional co-activator licensing the reshaping of the promoter epigenetic landscape.

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Year:  2019        PMID: 31527837     DOI: 10.1038/s41589-019-0354-y

Source DB:  PubMed          Journal:  Nat Chem Biol        ISSN: 1552-4450            Impact factor:   15.040


  9 in total

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Journal:  Nat Chem Biol       Date:  2021-12-13       Impact factor: 15.040

3.  A Read/Write Mechanism Connects p300 Bromodomain Function to H2A.Z Acetylation.

Authors:  Yolanda Colino-Sanguino; Evan M Cornett; David Moulder; Grady C Smith; Joel Hrit; Eric Cordeiro-Spinetti; Robert M Vaughan; Krzysztof Krajewski; Scott B Rothbart; Susan J Clark; Fátima Valdés-Mora
Journal:  iScience       Date:  2019-10-31

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5.  DNA Damage Repair-Related Genes Signature for Immune Infiltration and Outcome in Cervical Cancer.

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6.  GCN5-mediated regulation of pathological cardiac hypertrophy via activation of the TAK1-JNK/p38 signaling pathway.

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7.  Schizosaccharomyces pombe KAT5 contributes to resection and repair of a DNA double-strand break.

Authors:  Tingting Li; Ruben C Petreaca; Susan L Forsburg
Journal:  Genetics       Date:  2021-05-17       Impact factor: 4.562

8.  The bromodomains of BET family proteins can recognize diacetylated histone H2A.Z.

Authors:  Karishma Patel; Paul D Solomon; James L Walshe; Jason K K Low; Joel P Mackay
Journal:  Protein Sci       Date:  2020-12-08       Impact factor: 6.993

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  9 in total

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