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全基因组鉴定 OTP 基因为乳腺癌的新型甲基化标记物。

Genome-wide identification of OTP gene as a novel methylation marker of breast cancer.

机构信息

Genomictree Inc., Daejeon 301-721, Republic of Korea.

出版信息

Oncol Rep. 2012 May;27(5):1681-8. doi: 10.3892/or.2012.1691. Epub 2012 Feb 17.

DOI:10.3892/or.2012.1691
PMID:22366991
Abstract

Aberrant DNA methylation occurs early and frequently in tumorigenesis. Identification of DNA methylation biomarkers is a field that provides potential for improving the clinical process of breast cancer diagnosis. We utilized a genome-wide technique, methylated DNA isolation assay (MeDIA), in combination with high-resolution CpG microarray analysis to identify hypermethylated genes in breast cancer. Among differentially methylated genes between tumor and adjacent normal tissues, 3 candidate genes (LHX2, WT1 and OTP) were finally selected through a step-wise filtering process and examined for methylation status in normal tissues, primary tumor, and paired adjacent normal-appearing tissues from 39 breast cancer patients. Based on the calculated cut-off values, all genes showed significantly higher frequencies of aberrant hypermethylation in primary tumors (43.6% for LHX2, 89.7% for WT1 and 100% for OTP, p<0.05) while frequencies were intermediate in paired adjacent normal tissues and absent in normal tissues. On further analysis, the methylation level in primary tumors was not significantly correlated with clinicopathological features. Interestingly, DNA methylation of a novel gene OTP was detected in adjacent normal tissues even 6 cm away from primary tumors, suggesting that OTP methylation may qualify as a biomarker for the early detection of breast cancer. In conclusion, we successfully identified a novel gene OTP frequently methylated in breast cancer by genome-wide screening. Our results suggest that the OTP gene may play a crucial role in breast carcinogenesis, although further clinical validation will be needed to evaluate the potential application of OTP in the early detection of breast cancer.

摘要

异常的 DNA 甲基化在肿瘤发生的早期就经常发生。鉴定 DNA 甲基化生物标志物是一个提供潜在改善乳腺癌诊断临床过程的领域。我们利用全基因组技术,即甲基化 DNA 分离测定法(MeDIA),结合高分辨率 CpG 微阵列分析,鉴定乳腺癌中的高甲基化基因。在肿瘤和相邻正常组织之间差异甲基化的基因中,通过逐步过滤过程最终选择了 3 个候选基因(LHX2、WT1 和 OTP),并在 39 名乳腺癌患者的正常组织、原发肿瘤和配对的相邻正常组织中检测了这些基因的甲基化状态。根据计算出的截止值,所有基因在原发肿瘤中均表现出明显更高频率的异常高甲基化(LHX2 为 43.6%,WT1 为 89.7%,OTP 为 100%,p<0.05),而在配对的相邻正常组织中的频率中等,在正常组织中不存在。进一步分析表明,原发肿瘤中的甲基化水平与临床病理特征无显著相关性。有趣的是,即使在距离原发肿瘤 6 厘米的相邻正常组织中也检测到了新基因 OTP 的 DNA 甲基化,这表明 OTP 甲基化可能有资格成为乳腺癌早期检测的生物标志物。总之,我们通过全基因组筛选成功鉴定了一种在乳腺癌中经常甲基化的新基因 OTP。我们的结果表明,OTP 基因可能在乳腺癌发生中发挥关键作用,尽管需要进一步的临床验证来评估 OTP 在乳腺癌早期检测中的潜在应用。

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