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CpG Island Methylation in Human Lymphocytes Is Highly Correlated with DNA Sequence, Repeats, and Predicted DNA Structure

机译:人淋巴细胞中的CpG岛甲基化与DNA序列,重复序列和预测的DNA结构高度相关

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摘要

CpG island methylation plays an important role in epigenetic gene control during mammalian development and is frequently altered in disease situations such as cancer. The majority of CpG islands is normally unmethylated, but a sizeable fraction is prone to become methylated in various cell types and pathological situations. The goal of this study is to show that a computational epigenetics approach can discriminate between CpG islands that are prone to methylation from those that remain unmethylated. We develop a bioinformatics scoring and prediction method on the basis of a set of 1,184 DNA attributes, which refer to sequence, repeats, predicted structure, CpG islands, genes, predicted binding sites, conservation, and single nucleotide polymorphisms. These attributes are scored on 132 CpG islands across the entire human Chromosome 21, whose methylation status was previously established for normal human lymphocytes. Our results show that three groups of DNA attributes, namely certain sequence patterns, specific DNA repeats, and a particular DNA structure, are each highly correlated with CpG island methylation (correlation coefficients of 0.64, 0.66, and 0.49, respectively). We predicted, and subsequently experimentally examined 12 CpG islands from human Chromosome 21 with unknown methylation patterns and found more than 90% of our predictions to be correct. In addition, we applied our prediction method to analyzing Human Epigenome Project methylation data on human Chromosome 6 and again observed high prediction accuracy. In summary, our results suggest that DNA composition of CpG islands (sequence, repeats, and structure) plays a significant role in predisposing CpG islands for DNA methylation. This finding may have a strong impact on our understanding of changes in CpG island methylation in development and disease.
机译:CpG岛甲基化在哺乳动物发育过程中的表观遗传基因控制中起着重要作用,并且在诸如癌症等疾病中经常发生变化。大多数CpG岛通常未甲基化,但是相当大的一部分在各种细胞类型和病理情况下都容易甲基化。这项研究的目的是表明,一种计算表观遗传学方法可以区分容易甲基化的CpG岛和未甲基化的CpG岛。我们基于一组1,184个DNA属性,开发了生物信息学评分和预测方法,这些属性涉及序列,重复序列,预测结构,CpG岛,基因,预测结合位点,保守性和单核苷酸多态性。这些属性是在整个人类21号染色体上的132个CpG岛上评分的,该染色体先前已为正常人淋巴细胞建立了甲基化状态。我们的结果表明,三组DNA属性,即某些序列模式,特定的DNA重复序列和特定的DNA结构,均与CpG岛甲基化高度相关(相关系数分别为0.64、0.66和0.49)。我们预测了人类染色体21的12个CpG岛,然后进行了实验检查,这些岛的甲基化模式未知,发现我们90%以上的预测都是正确的。此外,我们将预测方法用于分析人类染色体6的人类表观基因组计划甲基化数据,并再次观察到较高的预测准确性。总之,我们的结果表明CpG岛的DNA组成(序列,重复序列和结构)在CpG岛的DNA甲基化易感性中起着重要作用。这一发现可能会对我们对CpG岛甲基化在发育和疾病中的变化的理解产生重大影响。

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