Lineage-specific distribution of high levels of genomic5-hydroxymethylcytosine in mammalian development

被引:0
|
作者
Alexey Ruzov
Yanina Tsenkina
Andrea Serio
Tatiana Dudnakova
Judy Fletcher
Yu Bai
Tatiana Chebotareva
Steve Pells
Zara Hannoun
Gareth Sullivan
Siddharthan Chandran
David C Hay
Mark Bradley
Ian Wilmut
Paul De Sousa
机构
[1] Wolfson Centre for Stem Cells,
[2] Tissue Engineering and Modelling,undefined
[3] Centre for Biomolecular Sciences,undefined
[4] University of Nottingham,undefined
[5] MRC Centre for Regenerative Medicine,undefined
[6] University of Edinburgh,undefined
[7] Euan MacDonald Centre for Motor Neurone Disease Research,undefined
[8] University of Edinburgh,undefined
[9] MRC Human Genetics Unit,undefined
[10] Western General Hospital,undefined
[11] School of Chemistry,undefined
[12] University of Edinburgh,undefined
[13] Roslin Cells,undefined
[14] Roslin Biocentre,undefined
[15] Roslin,undefined
[16] Midlothian,undefined
来源
Cell Research | 2011年 / 21卷
关键词
epigenetics; 5-hydroxymethylcytosine; 5-methylcytosine; CpG-methylation; stem cells; mammalian development; pluripotency;
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摘要
Methylation of cytosine is a DNA modification associated with gene repression. Recently, a novel cytosine modification, 5-hydroxymethylcytosine (5-hmC) has been discovered. Here we examine 5-hmC distribution during mammalian development and in cellular systems, and show that the developmental dynamics of 5-hmC are different from those of 5-methylcytosine (5-mC); in particular 5-hmC is enriched in embryonic contexts compared to adult tissues. A detectable 5-hmC signal appears in pre-implantation development starting at the zygote stage, where the paternal genome is subjected to a genome-wide hydroxylation of 5-mC, which precisely coincides with the loss of the 5-mC signal in the paternal pronucleus. Levels of 5-hmC are high in cells of the inner cell mass in blastocysts, and the modification colocalises with nestin-expressing cell populations in mouse post-implantation embryos. Compared to other adult mammalian organs, 5-hmC is strongly enriched in bone marrow and brain, wherein high 5-hmC content is a feature of both neuronal progenitors and post-mitotic neurons. We show that high levels of 5-hmC are not only present in mouse and human embryonic stem cells (ESCs) and lost during differentiation, as has been reported previously, but also reappear during the generation of induced pluripotent stem cells; thus 5-hmC enrichment correlates with a pluripotent cell state. Our findings suggest that apart from the cells of neuronal lineages, high levels of genomic 5-hmC are an epigenetic feature of embryonic cell populations and cellular pluri- and multi-lineage potency. To our knowledge, 5-hmC represents the first epigenetic modification of DNA discovered whose enrichment is so cell-type specific.
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页码:1332 / 1342
页数:10
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