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首页> 外文期刊>Scientific reports. >Genome-wide DNA methylome analysis reveals epigenetically dysregulated non-coding RNAs in human breast cancer
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Genome-wide DNA methylome analysis reveals epigenetically dysregulated non-coding RNAs in human breast cancer

机译:全基因组DNA甲基化组分析揭示了人类乳腺癌的表观遗传失调的非编码RNA

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Despite growing appreciation of the importance of epigenetics in breast cancer, our understanding of epigenetic alterations of non-coding RNAs (ncRNAs) in breast cancer remains limited. Here, we explored the epigenetic patterns of ncRNAs in breast cancers using published sequencing-based methylome data, primarily focusing on the two most commonly studied ncRNA biotypes, long ncRNAs and miRNAs. We observed widely aberrant methylation in the promoters of ncRNAs, and this abnormal methylation was more frequent than that in protein-coding genes. Specifically, intergenic ncRNAs were observed to comprise a majority (51.45% of the lncRNAs and 51.57% of the miRNAs) of the aberrantly methylated ncRNA promoters. Moreover, we summarized five patterns of aberrant ncRNA promoter methylation in the context of genomic CpG islands (CGIs), in which aberrant methylation occurred not only on CGIs, but also in regions flanking CGI and in CGI-lacking promoters. Integration with transcriptional datasets enabled us to determine that the ncRNA promoter methylation events were associated with transcriptional changes. Furthermore, a panel of ncRNAs were identified as biomarkers that discriminated between disease phenotypes. Finally, the potential functions of aberrantly methylated ncRNAs were predicted, suggestiong that ncRNAs and coding genes cooperatively mediate pathway dysregulation during the development and progression of breast cancer.
机译:尽管越来越认识到表观遗传学在乳腺癌中的重要性,但我们对乳腺癌中非编码RNA(ncRNA)的表观遗传学改变的理解仍然有限。在这里,我们使用已发表的基于测序的甲基化组数据研究了乳腺癌中ncRNA的表观遗传模式,主要侧重于两种最常研究的ncRNA生物型,长ncRNA和miRNA。我们在ncRNA的启动子中观察到广泛的异常甲基化,并且这种异常甲基化比在蛋白质编码基因中更常见。具体地,观察到基因间的ncRNA包含异常甲基化的ncRNA启动子的大部分(lncRNA的51.45%和miRNA的51.57%)。此外,我们总结了基因组CpG岛(CGI)的情况下异常ncRNA启动子甲基化的五种模式,其中异常甲基化不仅发生在CGI上,而且发生在CGI侧翼区域和缺少CGI的启动子中。与转录数据集的整合使我们能够确定ncRNA启动子甲基化事件与转录变化有关。此外,一组ncRNA被鉴定为可区分疾病表型的生物标志物。最后,预测了异常甲基化的ncRNA的潜在功能,提示ncRNA和编码基因在乳腺癌的发生和发展过程中协同介导通路失调。

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