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游离血清DNA的高甲基化表明膀胱癌患者的预后较差。

Hypermethylation of cell-free serum DNA indicates worse outcome in patients with bladder cancer.

作者信息

Ellinger Jörg, El Kassem Nadja, Heukamp Lukas C, Matthews Swapna, Cubukluoz Figen, Kahl Philip, Perabo Frank G, Müller Stefan C, von Ruecker Alexander, Bastian Patrick J

机构信息

Klinik und Poliklinik für Urologie, Universitätsklinikum Bonn, Rheinische-Friedrich-Wilhelms-Universität Bonn, Germany.

出版信息

J Urol. 2008 Jan;179(1):346-52. doi: 10.1016/j.juro.2007.08.091. Epub 2007 Nov 19.

Abstract

PURPOSE

CpG island hypermethylation is a frequent event in bladder carcinogenesis and progression. We investigated the diagnostic and prognostic value of hypermethylation in cell-free serum DNA of patients with bladder cancer.

MATERIALS AND METHODS

The study cohort consisted of 45 patients with bladder cancer undergoing cystectomy and 45 with histologically confirmed benign prostatic hyperplasia serving as controls. Hypermethylation at APC, DAPK, GSTP1, PTGS2, TIG1 and Reprimo was analyzed using real-time polymerase chain reaction following methylation sensitive restriction endonuclease treatment.

RESULTS

Hypermethylation at the APC and GSTP1 promoter was detected in 59% of cases, whereas TIG1 (32%), PTGS2 (24%) and DAPK (2%) were less frequently hypermethylated. In the benign prostatic hyperplasia group 3 patients also harbored methylated GSTP1 DNA, whereas none of the other gene sites was methylated. Hypermethylation at APC, GSTP1 or TIG1 distinguished patients with bladder cancer and controls most accurately with 80% sensitivity and 93% specificity. Hypermethylation significantly correlated with prognostic unfavorable clinicopathological parameters, including APC with pT stage, GSTP1, or GSTP1 or TIG1 with multifocal bladder cancer and APC, or APC or TIG1 with surgical margin positivity. Bladder cancer specific mortality was significantly increased in patients with APC hypermethylation.

CONCLUSIONS

The detection of hypermethylation in cell-free serum DNA provides valuable diagnostic and prognostic information that can still be improved by combining the results of 3 gene sites (APC, GSTP1 and TIG1). The presence of hypermethylated DNA in the serum of patients with bladder cancer is associated with a worse outcome. Our results suggest that measuring hypermethylation in the serum of patients with bladder cancer is a useful biomarker.

摘要

目的

CpG岛高甲基化是膀胱癌发生和进展过程中的常见事件。我们研究了膀胱癌患者游离血清DNA中高甲基化的诊断和预后价值。

材料与方法

研究队列包括45例行膀胱切除术的膀胱癌患者和45例经组织学证实为良性前列腺增生的患者作为对照。在甲基化敏感限制性内切酶处理后,使用实时聚合酶链反应分析APC、DAPK、GSTP1、PTGS2、TIG1和Reprimo的高甲基化情况。

结果

59%的病例检测到APC和GSTP1启动子高甲基化,而TIG1(32%)、PTGS2(24%)和DAPK(2%)高甲基化频率较低。在良性前列腺增生组中,3例患者也存在甲基化的GSTP1 DNA,而其他基因位点均未甲基化。APC、GSTP1或TIG1高甲基化对膀胱癌患者和对照的区分最为准确,敏感性为80%,特异性为93%。高甲基化与预后不良的临床病理参数显著相关,包括APC与pT分期、GSTP1或GSTP1或TIG1与多灶性膀胱癌以及APC或APC或TIG1与手术切缘阳性。APC高甲基化患者的膀胱癌特异性死亡率显著增加。

结论

游离血清DNA中高甲基化的检测提供了有价值的诊断和预后信息,通过结合3个基因位点(APC、GSTP1和TIG1)的结果仍可进一步改善。膀胱癌患者血清中高甲基化DNA的存在与较差的预后相关。我们的结果表明,检测膀胱癌患者血清中的高甲基化是一种有用的生物标志物。

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