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Identification of key genes by integrating DNA methylation and next-generation transcriptome sequencing for esophageal squamous cell carcinoma

机译:整合DNA甲基化和下一代转录组测序技术鉴定食管鳞癌关键基因

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摘要

Aberrant DNA methylation leads to abnormal gene expression, making it a significant regulator in the progression of cancer and leading to the requirement for integration of gene expression with DNA methylation. Here, we identified 120 genes demonstrating an inverse correlation between DNA methylation and mRNA expression in esophageal squamous cell carcinoma (ESCC). Sixteen key genes, such as SIX4, CRABP2, and EHD3, were obtained by filtering 10 datasets and verified in paired ESCC samples by qRT-PCR. 5-Aza-dC as a DNA methyltransferase (DNMT) inhibitor could recover their expression and inhibit clonal growth of cancer cells in seven ESCC cell lines. Furthermore, 11 of the 16 genes were correlated with OS (overall survival) and DFS (disease-free survival) in 125 ESCC patients. ChIP-Seq data and WGBS data showed that DNA methylation and H3K27ac histone modification of these key genes displayed inverse trends, suggesting that there was collaboration between DNA methylation and histone modification in ESCC. Our findings illustrate that the integrated multi-omics data (transcriptome and epigenomics) can accurately obtain potential prognostic biomarkers, which may provide important insight for the effective treatment of cancers.
机译:异常的DNA甲基化会导致异常的基因表达,使其成为癌症进程中的重要调节剂,并导致需要将基因表达与DNA甲基化整合在一起。在这里,我们确定了120个基因,这些基因在食管鳞状细胞癌(ESCC)中的DNA甲基化与mRNA表达之间呈负相关。通过过滤10个数据集获得了16个关键基因,例如SIX4,CRABP2和EHD3,并通过qRT-PCR在成对的ESCC样品中进行了验证。 5-Aza-dC作为DNA甲基转移酶(DNMT)抑制剂可以恢复其表达并抑制7种ESCC细胞系中癌细胞的克隆生长。此外,在125名ESCC患者中,这16个基因中的11个与OS(总生存)和DFS(无疾病生存)相关。 ChIP-Seq数据和WGBS数据显示,这些关键基因的DNA甲基化和H3K27ac组蛋白修饰呈相反趋势,表明ESCC中DNA甲基化和组蛋白修饰之间存在协同作用。我们的发现表明,综合的多组学数据(转录组和表观基因组学)可以准确获得潜在的预后生物标志物,这可能为有效治疗癌症提供重要的见识。

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