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Beyond SAHF: An integrative view of chromatin compartmentalization during senescence.

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Peer-reviewed

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Abstract

Cellular senescence, a persistent form of cell cycle arrest, has been linked to the formation of heterochromatic foci, accompanied by additional concentric epigenetic layers. However, senescence is a highly heterogeneous phenotype, and the formation of these structures is context dependent. Recent developments in the understanding of the high-order chromatin organization have opened new avenues for contextualizing the nuclear and chromatin phenotypes of senescence. Oncogene-induced senescence displays prominent foci and typically exhibits increased chromatin compartmentalization, based on the chromosome conformation assays, as marked by increased transcompaction and segregation of the heterochromatin and euchromatin. However, other types of senescence (e.g., replicative senescence) exhibit comparatively lower levels of compartmentalization. Thus, a more integrative view of the global rearrangement of the chromatin architecture that occurs during senescence is emerging, with potential functional implications for the heterogeneity of the senescence phenotype.

Description

Journal Title

Curr Opin Cell Biol

Conference Name

Journal ISSN

0955-0674
1879-0410

Volume Title

Publisher

Elsevier

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Except where otherwised noted, this item's license is described as Attribution 4.0 International
Sponsorship
Cancer Research UK (C63389/A30462)
Biotechnology and Biological Sciences Research Council (BB/S013466/1)
BBSRC (BB/T013486/1)
Cancer Research UK (24453)
This work is supported by a Cancer Research UK Cambridge Institute core grant (no. C9545/A29580) to MN laboratory. MN is also supported by BBSRC (BB/S013466/1 and BB/T013486/1) and Diabetes UK via BIRAX and the British Council (65BX18MNIB). IO is also supported by a Cancer Research UK Pioneer Award (C63389/A30462).