| Literature DB >> 28283545 |
Julien Douet1,2, David Corujo1,2, Roberto Malinverni1,2, Justine Renauld3, Viola Sansoni4, Melanija Posavec Marjanović1, Neus Cantariño1, Vanesa Valero1,2, Fabien Mongelard5, Philippe Bouvet5, Axel Imhof4, Marc Thiry3, Marcus Buschbeck6,2.
Abstract
Genetic loss-of-function studies on development, cancer and somatic cell reprogramming have suggested that the group of macroH2A histone variants might function through stabilizing the differentiated state by a yet unknown mechanism. Here, we present results demonstrating that macroH2A variants have a major function in maintaining nuclear organization and heterochromatin architecture. Specifically, we find that a substantial amount of macroH2A is associated with heterochromatic repeat sequences. We further identify macroH2A on sites of interstitial heterochromatin decorated by histone H3 trimethylated on K9 (H3K9me3). Loss of macroH2A leads to major defects in nuclear organization, including reduced nuclear circularity, disruption of nucleoli and a global loss of dense heterochromatin. Domains formed by DNA repeat sequences are disorganized, expanded and fragmented, and mildly re-expressed when depleted of macroH2A. At the molecular level, we find that macroH2A is required for the interaction of repeat sequences with the nucleostructural protein lamin B1. Taken together, our results argue that a major function of macroH2A histone variants is to link nucleosome composition to higher-order chromatin architecture.Entities:
Keywords: DNA repeats; Heterochromatin; Histone variant; Nuclear organization
Mesh:
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Year: 2017 PMID: 28283545 DOI: 10.1242/jcs.199216
Source DB: PubMed Journal: J Cell Sci ISSN: 0021-9533 Impact factor: 5.285