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High-resolution visualization of H3 variants during replication reveals their controlled recycling

1 déc. 2018Nature Communications

DOI : 10.1038/s41467-018-05697-1

Auteurs

Camille Clément, Guillermo A. Orsi, Alberto Gatto, Ekaterina Boyarchuk, Audrey Forest, Bassam Hajj, Judith Miné-Hattab, Mickaël Garnier, Zachary A. Gurard-Levin, Jean-Pierre Quivy, Geneviève Almouzni

Résumé

Abstract

DNA replication is a challenge for the faithful transmission of parental information to daughter cells, as both DNA and chromatin organization must be duplicated. Replication stress further complicates the safeguard of epigenome integrity. Here, we investigate the transmission of the histone variants H3.3 and H3.1 during replication. We follow their distribution relative to replication timing, first in the genome and, second, in 3D using super-resolution microscopy. We find that H3.3 and H3.1 mark early- and late-replicating chromatin, respectively. In the nucleus, H3.3 forms domains, which decrease in density throughout replication, while H3.1 domains increase in density. Hydroxyurea impairs local recycling of parental histones at replication sites. Similarly, depleting the histone chaperone ASF1 affects recycling, leading to an impaired histone variant landscape. We discuss how faithful transmission of histone variants involves ASF1 and can be impacted by replication stress, with ensuing consequences for cell fate and tumorigenesis.

Equipes

Équipe

Dynamique de la chromatine

GENEVIEVE ALMOUZNI

Membres

GENEVIEVE ALMOUZNI

Directeur de recherche CNRS

JEAN-PIERRE QUIVY

Directeur de recherche CNRS

BASSAM HAJJ

Chargé de recherche CNRS

MICKAEL GARNIER

Ingénieur de recherche