Biparental Contributions of the H2A.B Histone Variant Control Embryonic Development in Mice

Overview

Journal PLoS Biol

Specialty Biology

Date 2020 Dec 28

PMID 33362208

Citations 9

Authors

Antoine Molaro

Anna J Wood

Derek Janssens

Selina M Kindelay

Michael T Eickbush

Steven Wu

Priti Singh

Charles H Muller

Steven Henikoff

Harmit S Malik

Affiliations

Soon will be listed here.

Abstract

Histone variants expand chromatin functions in eukaryote genomes. H2A.B genes are testis-expressed short histone H2A variants that arose in placental mammals. Their biological functions remain largely unknown. To investigate their function, we generated a knockout (KO) model that disrupts all 3 H2A.B genes in mice. We show that H2A.B KO males have globally altered chromatin structure in postmeiotic germ cells. Yet, they do not show impaired spermatogenesis or testis function. Instead, we find that H2A.B plays a crucial role postfertilization. Crosses between H2A.B KO males and females yield embryos with lower viability and reduced size. Using a series of genetic crosses that separate parental and zygotic contributions, we show that the H2A.B status of both the father and mother, but not of the zygote, affects embryonic viability and growth during gestation. We conclude that H2A.B is a novel parental-effect gene, establishing a role for short H2A histone variants in mammalian development. We posit that parental antagonism over embryonic growth drove the origin and ongoing diversification of short histone H2A variants in placental mammals.

Citing Articles

The Function of H2A Histone Variants and Their Roles in Diseases.

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Multifunctional histone variants in genome function.

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Roles of Histone H2A Variants in Cancer Development, Prognosis, and Treatment.

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Casting histone variants during mammalian reproduction.

Karam G, Molaro A Chromosoma. 2023; 132(3):153-165.

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Expansion and loss of sperm nuclear basic protein genes in correspond with genetic conflicts between sex chromosomes.

Chang C, Mejia Natividad I, Malik H Elife. 2023; 12.

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