Regulation of chromatin structure via histone post-translational modification and the link to carcinogenesis

被引:0
作者
Laura L. Thompson
Brent J. Guppy
Laryssa Sawchuk
James R. Davie
Kirk J. McManus
机构
[1] University of Manitoba,Department of Biochemistry & Medical Genetics
[2] CancerCare Manitoba,Manitoba Institute of Cell Biology
[3] John Buhler Research Centre,Manitoba Institute of Child Health
来源
Cancer and Metastasis Reviews | 2013年 / 32卷
关键词
Histones; Post-translational modifications; Phosphorylation; Methylation; Ubiquitination; Epigenetics; Genome instability; Cancer;
D O I
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学科分类号
摘要
The loss of genome integrity contributes to the development of tumors. Although genome instability is associated with virtually all tumor types including both solid and liquid tumors, the aberrant molecular origins that drive this instability are poorly understood. It is now becoming clear that epigenetics and specific histone post-translational modifications (PTMs) have essential roles in maintaining genome stability under normal conditions. A strong relationship exists between aberrant histone PTMs, genome instability, and tumorigenesis. Changes in the genomic location of specific histone PTMs or alterations in the steady-state levels of the PTM are the consequence of imbalances in the enzymes and their activities catalyzing the addition of PTMs (“writers”) or removal of PTMs (“erasers”). This review focuses on the misregulation of three specific types of histone PTMs: histone H3 phosphorylation at serines 10 and 28, H4 mono-methylation at lysine 20, and H2B ubiquitination at lysine 120. We discuss the normal regulation of these PTMs by the respective “writers” and “erasers” and the impact of their misregulation on genome stability.
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页码:363 / 376
页数:13
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