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Methylation of the candidate biomarker TCF21 is very frequent across a spectrum of early-stage nonsmall cell lung cancers

机译:候选生物标志物TCF21的甲基化在一系列早期非小细胞肺癌中非常频繁

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摘要

Background: The transcription factor TCF21 is involved in mesenchymal-to-epithelial differentiation and was shown to be aberrantly hypermethylated in lung and head and neck cancers. Because of its reported high frequency of hypermethylation in lung cancer, further characterization of the stages and types of nonsmall cell lung cancer (NSCLC) that are hypermethylated and the frequency of hypermethylation and associated "second hits" were assessed. Methods: TCF21 promoter hypermethylation in 105 NSCLC including various stages and histologies in smokers and nonsmokers was determined. In addition, TCF21 loss of heterozygosity and mutational status were examined. Twenty-two cancer cell lines from varied tissue origins were also assayed. The NSCLC results were validated and expanded by examining TCF21 immunohistochemical expression on a tissue microarray containing 300 NSCLC cases. Results: Overall, 81% of NSCLC samples showed TCF21 promoter hypermethylation, and 84% showed decreased TCF21 protein expression. Multivariate analysis showed that TCF21 expression, although below normal in both histologies, was lower in adenocarcinoma than in squamous cell carcinoma and was not independently correlated with sex, smoking, and EGFR mutation status or with clinical outcome. Cell lines from other cancer types also showed frequent TCF21 promoter hypermethylation. Conclusions: Hypermethylation and decreased expression of TCF21 were tumor specific and very frequent in all NSCLCs, even early-stage disease, thus making TCF21 a potential candidate methylation biomarker for early-stage NSCLC screening. TCF21 hypermethylation in a variety of tumor cell lines suggests it may also be a valuable methylation biomarker in other tumor types. © 2010 American Cancer Society.
机译:背景:转录因子TCF21参与间充质到上皮的分化,并被证明在肺癌,头颈癌中异常甲基化。由于据报道其在肺癌中高甲基化的频率很高,因此对高甲基化的非小细胞肺癌(NSCLC)的阶段和类型以及其高甲基化的频率和相关的“第二击”进行了进一步的表征。方法:确定105例NSCLC中TCF21启动子的甲基化水平,包括吸烟者和非吸烟者的不同阶段和组织学。另外,检查了TCF21杂合性丧失和突变状态。还检测了来自不同组织来源的22个癌细胞系。通过在包含300例NSCLC病例的组织微阵列上检查TCF21免疫组织化学表达,验证并扩展了NSCLC结果。结果:总的来说,81%的NSCLC样品显示TCF21启动子高度甲基化,84%的TCF21蛋白表达降低。多变量分析表明,尽管TCF21的表达在两种组织学中均低于正常水平,但在腺癌中却低于鳞状细胞癌,并且与性别,吸烟,EGFR突变状态或临床结局无关。来自其他癌症类型的细胞系也显示出频繁的TCF21启动子高甲基化。结论:TCF21的高甲基化和表达降低是肿瘤特异性的,并且在所有NSCLC中甚至是早期疾病中都非常频繁,因此TCF21可能成为早期NSCLC筛查的潜在候选甲基化生物标志物。 TCF21在多种肿瘤细胞系中的甲基化过度表明,它在其他肿瘤类型中也可能是有价值的甲基化生物标志物。 ©2010美国癌症协会。

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