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首页> 外文期刊>Genome research >Cell type-specific DNA methylation at intragenic CpG islands in the immune system.
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Cell type-specific DNA methylation at intragenic CpG islands in the immune system.

机译:免疫系统中基因内CpG岛的细胞类型特异性DNA甲基化。

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摘要

Human and mouse genomes contain a similar number of CpG islands (CGIs), which are discrete CpG-rich DNA sequences associated with transcription start sites. In both species, approximately 50% of all CGIs are remote from annotated promoters but, nevertheless, often have promoter-like features. To determine the role of CGI methylation in cell differentiation, we analyzed DNA methylation at a comprehensive CGI set in cells of the mouse hematopoietic lineage. Using a method that potentially detects approximately 33% of genomic CpGs in the methylated state, we found that large differences in gene expression were accompanied by surprisingly few DNA methylation changes. There were, however, many DNA methylation differences between hematopoietic cells and a distantly related tissue, brain. Altered DNA methylation in the immune system occurred predominantly at CGIs within gene bodies, which have the properties of cell type-restricted promoters, but infrequently at annotated gene promoters or CGI flanking sequences (CGI "shores"). Unexpectedly, elevated intragenic CGI methylation correlated with silencing of the associated gene. Differentially methylated intragenic CGIs tended to lack H3K4me3 and associate with a transcriptionally repressive environment regardless of methylation state. Our results indicate that DNA methylation changes play a relatively minor role in the late stages of differentiation and suggest that intragenic CGIs represent regulatory sites of differential gene expression during the early stages of lineage specification.
机译:人和小鼠基因组包含相似数量的CpG岛(CGI),它们是与转录起始位点相关的离散的富含CpG的DNA序列。在这两个物种中,大约所有CGI的50%都远离带注释的启动子,但是,通常具有类似启动子的特征。为了确定CGI甲基化在细胞分化中的作用,我们在小鼠造血谱系细胞中的综合CGI集上分析了DNA甲基化。使用一种可能检测到约33%处于甲基化状态的基因组CpG的方法,我们发现基因表达的巨大差异伴随着令人惊讶的少量DNA甲基化变化。但是,造血细胞与远距离相关的组织大脑之间存在许多DNA甲基化差异。免疫系统中DNA甲基化的改变主要发生在基因体内的CGI,其具有细胞类型限制的启动子的特性,但很少出现在带注释的基因启动子或CGI侧翼序列(CGI“岸边”)上。出乎意料的是,升高的基因内CGI甲基化与相关基因的沉默相关。差异甲基化的基因内CGI倾向于缺乏H3K4me3,并且与转录抑制环境相关,而与甲基化状态无关。我们的结果表明,DNA甲基化变化在分化的晚期阶段起着相对较小的作用,并暗示基因内CGI代表了谱系规范早期的差异基因表达的调控位点。

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