Stability and flexibility of epigenetic gene regulation in mammalian development

被引:0
|
作者
Wolf Reik
机构
[1] Laboratory of Developmental Genetics and Imprinting,
[2] The Babraham Institute,undefined
来源
Nature | 2007年 / 447卷
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摘要
During development, cells start in a pluripotent state, from which they can differentiate into many cell types, and progressively develop a narrower potential. Their gene-expression programmes become more defined, restricted and, potentially, 'locked in'. Pluripotent stem cells express genes that encode a set of core transcription factors, while genes that are required later in development are repressed by histone marks, which confer short-term, and therefore flexible, epigenetic silencing. By contrast, the methylation of DNA confers long-term epigenetic silencing of particular sequences — transposons, imprinted genes and pluripotency-associated genes — in somatic cells. Long-term silencing can be reprogrammed by demethylation of DNA, and this process might involve DNA repair. It is not known whether any of the epigenetic marks has a primary role in determining cell and lineage commitment during development.
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页码:425 / 432
页数:7
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