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Cancer Biology & Therapy Volume 13, 2012 - Issue 11
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Regulation of oncogene-induced cell cycle exit and senescence by chromatin modifiers

Gregory David 1Department of Pharmacology and NYU Cancer Institute; NYU Langone Medical Center; New York, NY USA.
Pages 992-1000 | Received 11 May 2012, Accepted 12 Jun 2012, Published online: 24 Jul 2012
 
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Abstract

Oncogene activation leads to dramatic changes in numerous biological pathways controlling cellular division, and results in the initiation of a transcriptional program that promotes transformation. Conversely, it also triggers an irreversible cell cycle exit called cellular senescence, which allows the organism to counteract the potentially detrimental uncontrolled proliferation of damaged cells. Therefore, a tight transcriptional control is required at the onset of oncogenic signal, coordinating both positive and negative regulation of gene expression. Not surprisingly, numerous chromatin modifiers contribute to the cellular response to oncogenic stress. While these chromatin modifiers were initially thought of as mere mediators of the cellular response to oncogenic stress, recent studies have uncovered a direct and specific regulation of chromatin modifiers by oncogenic signals. We review here the diverse functions of chromatin modifiers in the cellular response to oncogenic stress, and discuss the implications of these findings on the regulation of cell cycle progression and proliferation by activated oncogenes.

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