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DNA 共甲基化分析提示乳腺癌样本中基因对之间存在新的功能关联。

DNA co-methylation analysis suggests novel functional associations between gene pairs in breast cancer samples.

机构信息

Center for Bioinformatics, Saarland University, Saarbrücken D-66041, Germany.

出版信息

Hum Mol Genet. 2013 Aug 1;22(15):3016-22. doi: 10.1093/hmg/ddt158. Epub 2013 Apr 9.

Abstract

Localized promoter hypermethylation and overall DNA hypomethylation have been associated with the presence of tumor in humans. Yet, despite the large amount of recently produced epigenetic data, there is still a lack of understanding on how several genes behave in tumor cells with respect to their epigenetic alterations such as DNA methylation. Here we performed a novel type of analysis that measures the correlation of DNA methylation levels between two genes across many samples. We linked this so-called co-methylation to the genomic distance of these genes, their functional similarity and their expression levels. Co-methylation analysis of more than 300 breast cancer samples from the TCGA portal yielded 187 pairs of genes showing Pearson correlation coefficients |r| ≥ 0.75. These pairs were formed by 133 genes. Less than half of these pairs are located on the same chromosome. For these, we found that the level of co-methylation is weakly anti-correlated with genomic distance (r = -0.29). Linking co-methylation with the functional similarity of genes showed that genes with r ≥ 0.8 tend to have similar molecular function and to be involved in the same biological process as described in the Gene Ontology project. Clustering of highly co-methylated genes identified four enriched KEGG pathways. Hence we have introduced co-methylation as a new indicator to discover functional associations between gene pairs in breast cancer and furthermore to discover new candidate genes that should be inspected more closely in the context of the studied disease.

摘要

局部启动子超甲基化和总体 DNA 低甲基化与人类肿瘤的存在有关。然而,尽管最近产生了大量的表观遗传数据,但对于几个基因在肿瘤细胞中的表观遗传改变(如 DNA 甲基化)如何表现,仍缺乏理解。在这里,我们进行了一种新的分析,测量了许多样本中两个基因之间的 DNA 甲基化水平的相关性。我们将这种所谓的共甲基化与这些基因的基因组距离、功能相似性和表达水平联系起来。对来自 TCGA 门户的 300 多个乳腺癌样本进行的共甲基化分析产生了 187 对 Pearson 相关系数 |r|≥0.75 的基因。这些对由 133 个基因组成。这些对中不到一半位于同一染色体上。对于这些基因,我们发现共甲基化水平与基因组距离呈弱负相关(r = -0.29)。将共甲基化与基因功能相似性联系起来表明,r≥0.8 的基因往往具有相似的分子功能,并参与基因本体论项目中描述的相同生物学过程。高度共甲基化基因的聚类确定了四个丰富的 KEGG 途径。因此,我们引入了共甲基化作为一种新的指标,以发现乳腺癌中基因对之间的功能关联,并进一步发现新的候选基因,在研究疾病的背景下应更仔细地检查这些候选基因。

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