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Pharmacological Unmasking Microarray Approach-Based Discovery of Novel DNA Methylation Markers for Hepatocellular Carcinoma

机译:基于药理学揭示基因芯片方法的肝细胞癌新型DNA甲基化标记物的发现

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摘要

DNA methylation is one of the main epigenetic mechanisms and hypermethylation of CpG islands at tumor suppressor genes switches off these genes. To find novel DNA methylation markers in hepatocellular carcinoma (HCC), we performed pharmacological unmasking (treatment with 5-aza-2'-deoxycytidine or trichostatin A) followed by microarray analysis in HCC cell lines. Of the 239 promoter CpG island loci hypermethylated in HCC cell lines (as revealed by methylation-specific PCR), 221 loci were found to be hypermethylated in HCC or nonneoplastic liver tissues. Thirty-three loci showed a 20% higher methylation frequency in tumors than in adjacent nonneoplastic tissues. Correlation of individual cancer-related methylation markers with clinicopathological features of HCC patients (n = 95) revealed that the number of hypermethylated genes in HCC tumors was higher in older than in younger patients. Univariate and multivariate survival analysis revealed that the HIST1H2AE methylation status is closely correlated with the patient's overall survival (P = 0.022 and P = 0.010, respectively). In conclusion, we identified 221 novel DNA methylation markers for HCC. One promising prognostic marker, HIST1H2AE, should be further validated in the prognostication of HCC patients.
机译:DNA甲基化是主要的表观遗传机制之一,在肿瘤抑制基因上CpG岛的超甲基化会关闭这些基因。为了在肝细胞癌(HCC)中发现新的DNA甲基化标记,我们进行了药理学研究(用5-氮杂2'-脱氧胞苷或曲古抑菌素A处理),然后在HCC细胞系中进行了微阵列分析。在HCC细胞系中高甲基化的239个启动子CpG岛基因座(通过甲基化特异性PCR揭示)中,发现221个基因座在HCC或非肿瘤肝组织中是高甲基化的。 33个基因座在肿瘤中的甲基化频率比相邻的非肿瘤组织高20%。肝癌患者个别癌症相关甲基化标志物与临床病理特征的相关性(n = 95)显示,老年患者HCC肿瘤中高甲基化基因的数量高于年轻患者。单因素和多因素生存分析表明,HIST1H2AE甲基化状态与患者的整体生存密切相关(分别为P = 0.022和P = 0.010)。总之,我们确定了221种新的HCC DNA甲基化标记。一种有前途的预后标志物HIST1H2AE,应在HCC患者的预后中进一步验证。

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