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Analysis of Matched Tumor and Normal Profiles Reveals Common Transcriptional and Epigenetic Signals Shared across Cancer Types

机译:匹配的肿瘤和正常形态的分析揭示了跨癌症类型共享的常见转录和表观遗传信号

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摘要

To identify the transcriptional regulatory changes that are most widespread in solid tumors, we performed a pan-cancer analysis using over 600 pairs of tumors and adjacent normal tissues profiled in The Cancer Genome Atlas (TCGA). Frequency of upregulation was calculated across mRNA expression levels, microRNA expression levels and CpG methylation sites and is provided here as a resource. Frequent tumor-associated alterations were identified using a simple statistical approach. Many of the identified changes were consistent with the increased rate of cell division in cancer, such as the overexpression of cell cycle genes and hypermethylation of PRC2 binding sites. However, we also identified proliferation-independent alterations, which highlight novel pathways essential to tumor formation. Nearly all of the GABA receptors are frequently downregulated, with the gene encoding the delta subunit (GABRD) strongly upregulated as the notable exception. Metabolic genes are also frequently downregulated, particularly alcohol dehydrogenases and others consistent with the decreased role of oxidative phosphorylation in cancerous cells. Alterations in the composition of GABA receptors and metabolism may play a key role in the differentiation of cancer cells, independent of proliferation.
机译:为了鉴定在实体瘤中最普遍的转录调控变化,我们使用了超过600对肿瘤和癌基因组图谱(TCGA)中描述的邻近正常组织进行了全癌分析。在mRNA表达水平,microRNA表达水平和CpG甲基化位点之间计算上调频率,并在此处作为资源提供。使用简单的统计方法可确定与肿瘤相关的频繁改变。许多已确定的变化与癌症中细胞分裂的增加速率一致,例如细胞周期基因的过表达和PRC2结合位点的超甲基化。但是,我们还确定了不依赖增殖的改变,突显了肿瘤形成必不可少的新途径。几乎所有的GABA受体都经常被下调,其中一个明显的例外是编码δ亚基(GABRD)的基因被上调。代谢基因也经常被下调,特别是酒精脱氢酶和其他与癌细胞中氧化磷酸化作用降低有关的基因。 GABA受体组成和代谢的改变可能在癌细胞的分化中起关键作用,而与增殖无关。

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