Mapping H4K20me3 onto the chromatin landscape of senescent cells indicates a function in control of cell senescence and tumor suppression through preservation of genetic and epigenetic stability

David M. Nelson,Farah Jaber-Hijazi,John J. Cole,Neil A. Robertson,Jeff S. Pawlikowski,Kevin Norris,Steven W. Criscione,Nikolay A. Pchelintsev,Desiree Piscitello,Nicholas Stong,Taranjit Singh Rai,Tony McBryan,Gabriel L. Otte,Colin Nixon,William Clark,Harold Riethman,Hong Wu,Gunnar Schotta,Benjamin A. Garcia,Nicola Neretti,Duncan Martin Baird,Shelley L. Berger,Peter D. Adams

Mapping H4K20me3 onto the chromatin landscape of senescent cells indicates a function in control of cell senescence and tumor suppression through preservation of genetic and epigenetic stability

2016

Background Histone modification H4K20me3 and its methyltransferase SUV420H2 have been implicated in suppression of tumorigenesis. The underlying mechanism is unclear, although H4K20me3 abundance increases during cellular senescence, a stable proliferation arrest and tumor suppressor process, triggered by diverse molecular cues, including activated oncogenes. Here, we investigate the function of H4K20me3 in senescence and tumor suppression.

Keywords:

Genetics
Senescence
DNA methylation
Chromatin
Biology
Histone
Carcinogenesis
Epigenetics
Cell growth
Cell biology
Methyltransferase
Epigenome
Heterochromatin

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