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异常的波形蛋白甲基化是上消化道病变的特征。

Aberrant vimentin methylation is characteristic of upper gastrointestinal pathologies.

机构信息

Case Western Reserve University, 10900 Euclid Avenue, Cleveland, OH 44106, USA.

出版信息

Cancer Epidemiol Biomarkers Prev. 2012 Apr;21(4):594-600. doi: 10.1158/1055-9965.EPI-11-1060. Epub 2012 Feb 7.

Abstract

BACKGROUND

We have previously established aberrant DNA methylation of vimentin exon-1 (VIM methylation) as a common epigenetic event in colon cancer and as a biomarker for detecting colon neoplasia. We now examine vimentin methylation in neoplasia of the upper gastrointestinal tract.

METHODS

Using a quantitative real-time methylation-specific PCR assay, we tested for vimentin methylation in archival specimens of esophageal and gastric neoplasia.

RESULTS

We find that acquisition of aberrant vimentin methylation is highly common in these neoplasms, but largely absent in controls. The highest frequency of vimentin methylation was detected in lesions of the distal esophagus, including 91% of Barrett's esophagus (n = 11), 100% of high-grade dysplasia (HGD, n = 5), and 81% of esophageal adenocarcinoma (EAC, n = 26) but absent in controls (n = 9). Vimentin methylation similarly was detected in 87% of signet ring (n = 15) and 53% of intestinal type gastric cancers (n = 17). Moreover, in tests of cytology brushings vimentin methylation proved detectable in 100% of Barrett's esophagus cases (n = 7), 100% of HGD cases (n = 4), and 83% of EAC cases (n = 18) but was absent in all controls (n = 5).

CONCLUSIONS

These findings establish aberrant vimentin methylation as a highly common epigenetic alteration in neoplasia of the upper gastrointestinal tract and show that Barrett's esophagus, even without dysplasia, already contains epigenetic alterations characteristic of adenocarcinoma.

IMPACT

These findings suggest vimentin methylation as a biomarker of upper gastrointestinal neoplasia with potential for development as molecular cytology in esophageal screening.

摘要

背景

我们之前已经确定,波形蛋白外显子 1 的异常甲基化(VIM 甲基化)是结肠癌中常见的表观遗传事件,也是检测结肠肿瘤的生物标志物。现在,我们研究了上消化道肿瘤中的波形蛋白甲基化。

方法

我们使用定量实时甲基化特异性 PCR 检测方法,检测了食管和胃肿瘤存档标本中的波形蛋白甲基化。

结果

我们发现,这些肿瘤中异常波形蛋白甲基化的获得非常普遍,但在对照中基本不存在。在远端食管病变中检测到最高频率的波形蛋白甲基化,包括 Barrett 食管(n = 11)的 91%、高级别异型增生(HGD,n = 5)的 100%和食管腺癌(EAC,n = 26)的 81%,而对照(n = 9)中则不存在。波形蛋白甲基化在 87%的印戒细胞(n = 15)和 53%的肠型胃癌(n = 17)中也被检测到。此外,细胞学刷检的检测中,波形蛋白甲基化在 100%的 Barrett 食管病例(n = 7)、100%的 HGD 病例(n = 4)和 83%的 EAC 病例(n = 18)中均可检测到,但在所有对照(n = 5)中均不存在。

结论

这些发现确立了异常波形蛋白甲基化为上消化道肿瘤中一种非常普遍的表观遗传改变,并表明 Barrett 食管,即使没有异型增生,也已经包含了腺癌的特征性表观遗传改变。

影响

这些发现提示波形蛋白甲基化作为上消化道肿瘤的生物标志物具有发展为食管筛查分子细胞学的潜力。

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