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Integrating Multi-omics Data to Dissect Mechanisms of DNA repair Dysregulation in Breast Cancer

机译:集成多OMICS数据以对乳腺癌DNA修复失调机制的描述

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DNA repair genes and pathways that are transcriptionally dysregulated in cancer provide the first line of evidence for the altered DNA repair status in tumours, and hence have been explored intensively as a source for biomarker discovery. The molecular mechanisms underlying DNA repair dysregulation, however, have not been systematically investigated in any cancer type. In this study, we performed a statistical analysis to dissect the roles of DNA copy number alteration (CNA), DNA methylation (DM) at gene promoter regions and the expression changes of transcription factors (TFs) in the differential expression of individual DNA repair genes in normal versus tumour breast samples. These gene-level results were summarised at pathway level to assess whether different DNA repair pathways are affected in distinct manners. Our results suggest that CNA and expression changes of TFs are major causes of DNA repair dysregulation in breast cancer, and that a subset of the identified TFs may exert global impacts on the dysregulation of multiple repair pathways. Our work hence provides novel insights into DNA repair dysregulation in breast cancer. These insights improve our understanding of the molecular basis of the DNA repair biomarkers identified thus far, and have potential to inform future biomarker discovery.
机译:DNA修复基因和在癌症中转录的途径提供了第一线证据,用于肿瘤中的改变的DNA修复状态,因此已被广泛探讨作为生物标志物发现的来源。然而,DNA修复失调的分子机制尚未在任何癌症类型中系统地研究。在这项研究中,我们进行了统计分析,解剖了DNA拷贝数改变(CNA),DNA甲基化(DM)在基因启动子区的作用以及单个DNA修复基因的差异表达中转录因子(TFS)的表达变化在正常与肿瘤乳房样品中。这些基因级结果总结了途径水平,以评估不同的DNA修复途径是否受到不同的方式影响。我们的研究结果表明,TFS的CNA和表达变化是DNA修复乳腺癌中DNA修复失调的主要原因,并且所识别的TFS的子集可能对多种修复途径的失调施加全局影响。因此,我们的工作为DNA修复乳腺癌的DNA修复失调提供了新的见解。这些见解改善了我们对迄今确定的DNA修复生物标志物的分子基础的理解,并且有可能通知未来的生物标志物发现。

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