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肿瘤抑制基因ITIH5、DKK3和RASSF1A的启动子高甲基化作为基于血液的乳腺癌筛查的新型生物标志物。

Promoter hypermethylation of the tumor-suppressor genes ITIH5, DKK3, and RASSF1A as novel biomarkers for blood-based breast cancer screening.

作者信息

Kloten Vera, Becker Birte, Winner Kirsten, Schrauder Michael G, Fasching Peter A, Anzeneder Tobias, Veeck Jürgen, Hartmann Arndt, Knüchel Ruth, Dahl Edgar

出版信息

Breast Cancer Res. 2013 Jan 15;15(1):R4. doi: 10.1186/bcr3375.

Abstract

INTRODUCTION

For early detection of breast cancer, the development of robust blood-based biomarkers that accurately reflect the host tumor is mandatory. We investigated DNA methylation in circulating free DNA (cfDNA) from blood of breast cancer patients and matched controls to establish a biomarker panel potentially useful for early detection of breast cancer.

METHODS

We examined promoter methylation of seven putative tumor-suppressor genes (SFRP1, SFRP2, SFRP5, ITIH5, WIF1, DKK3, and RASSF1A) in cfDNA extracted from serum. Clinical performance was first determined in a test set (n = 261 sera). In an independent validation set (n = 343 sera), we validated the most promising genes for further use in early breast cancer detection. Sera from 59 benign breast disease and 58 colon cancer patients were included for additional specificity testing.

RESULTS

Based on the test set, we determined ITIH5 and DKK3 promoter methylation as candidate biomarkers with the best sensitivity and specificity. In both the test and validation set combined, ITIH5 and DKK3 methylation achieved 41% sensitivity with a specificity of 93% and 100% in healthy and benign disease controls, respectively. Combination of these genes with RASSF1A methylation increased the sensitivity to 67% with a specificity of 69% and 82% in healthy controls and benign disease controls, respectively.

CONCLUSIONS

Tumor-specific methylation of the three-gene panel (ITIH5, DKK3, and RASSF1A) might be a valuable biomarker for the early detection of breast cancer.

摘要

引言

为了早期检测乳腺癌,开发能够准确反映宿主肿瘤情况的、强大的血液生物标志物是必不可少的。我们研究了乳腺癌患者和配对对照者血液中循环游离DNA(cfDNA)的DNA甲基化情况,以建立一个可能有助于早期检测乳腺癌的生物标志物组合。

方法

我们检测了从血清中提取的cfDNA中7个假定的肿瘤抑制基因(SFRP1、SFRP2、SFRP5、ITIH5、WIF1、DKK3和RASSF1A)的启动子甲基化情况。首先在一个测试集(n = 261份血清)中确定临床性能。在一个独立的验证集(n = 343份血清)中,我们验证了最有前景的基因,以便进一步用于早期乳腺癌检测。纳入了59例良性乳腺疾病患者和58例结肠癌患者的血清进行额外的特异性测试。

结果

基于测试集,我们确定ITIH5和DKK3启动子甲基化是具有最佳敏感性和特异性的候选生物标志物。在测试集和验证集合并的情况下,ITIH5和DKK3甲基化分别在健康对照和良性疾病对照中实现了41%的敏感性,特异性分别为93%和100%。这些基因与RASSF1A甲基化相结合,在健康对照和良性疾病对照中的敏感性分别提高到67%,特异性分别为69%和82%。

结论

三基因组合(ITIH5、DKK3和RASSF1A)的肿瘤特异性甲基化可能是早期检测乳腺癌的有价值的生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b705/3672828/c0b1d5de44d1/bcr3375-1.jpg

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