What Makes a Histone Variant a Variant: Changing H2A to Become H2A.Z

Overview

Journal PLoS Genet

Specialty Genetics

Date 2021 Dec 6

PMID 34871303

Citations 8

Authors

Hilary T Brewis

Alice Y Wang

Aline Gaub

Justine J Lau

Peter C Stirling

Michael S Kobor

Affiliations

Soon will be listed here.

Abstract

Chromatin structure and underlying DNA accessibility is modulated by the incorporation of histone variants. H2A.Z, a variant of the H2A core histone family, plays a distinct and essential role in a diverse set of biological functions including gene regulation and maintenance of heterochromatin-euchromatin boundaries. Although it is currently unclear how the replacement of H2A with H2A.Z can regulate gene expression, the variance in their amino acid sequence likely contributes to their functional differences. To tease apart regions of H2A.Z that confer its unique identity, a set of plasmids expressing H2A-H2A.Z hybrids from the native H2A.Z promoter were examined for their ability to recapitulate H2A.Z function. First, we found that the H2A.Z M6 region was necessary and sufficient for interaction with the SWR1-C chromatin remodeler. Remarkably, the combination of only 9 amino acid changes, the H2A.Z M6 region, K79 and L81 (two amino acids in the α2-helix), were sufficient to fully rescue growth phenotypes of the htz1Δ mutant. Furthermore, combining three unique H2A.Z regions (K79 and L81, M6, C-terminal tail) was sufficient for expression of H2A.Z-dependent heterochromatin-proximal genes and GAL1 derepression. Surprisingly, hybrid constructs that restored the transcription of H2A.Z-dependent genes, did not fully recapitulate patterns of H2A.Z-specific enrichment at the tested loci. This suggested that H2A.Z function in transcription regulation may be at least partially independent of its specific localization in chromatin. Together, this work has identified three regions that can confer specific H2A.Z-identity to replicative H2A, furthering our understanding of what makes a histone variant a variant.

Citing Articles

Characterizing the regulatory effects of H2A.Z and SWR1-C on gene expression during hydroxyurea exposure in Saccharomyces cerevisiae.

Brewis H, Stirling P, Kobor M PLoS Genet. 2025; 21(1):e1011566.

PMID: 39836664 PMC: 11761084. DOI: 10.1371/journal.pgen.1011566.

Beyond the Usual Suspects: Examining the Role of Understudied Histone Variants in Breast Cancer.

Dhahri H, Saintilnord W, Chandler D, Fondufe-Mittendorf Y Int J Mol Sci. 2024; 25(12).

PMID: 38928493 PMC: 11203562. DOI: 10.3390/ijms25126788.

Truncating the spliceosomal 'rope protein' Prp45 results in Htz1 dependent phenotypes.

Abrhamova K, Grouslova M, Valentova A, Hao X, Liu B, Prevorovsky M RNA Biol. 2024; 21(1):1-17.

PMID: 38711165 PMC: 11085953. DOI: 10.1080/15476286.2024.2348896.

Replacement of Arabidopsis H2A.Z with human H2A.Z orthologs reveals extensive functional conservation and limited importance of the N-terminal tail sequence for Arabidopsis development.

Sijacic P, Holder D, Krall E, Willett C, Foroozani M, Deal R bioRxiv. 2023; .

PMID: 37961174 PMC: 10635141. DOI: 10.1101/2023.11.03.565555.

Competitive Chemical Reaction Kinetic Model of Nucleosome Assembly Using the Histone Variant H2A.Z and H2A In Vitro.

Zhao H, Shao X, Guo M, Xing Y, Wang J, Luo L Int J Mol Sci. 2023; 24(21).

PMID: 37958827 PMC: 10647764. DOI: 10.3390/ijms242115846.

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