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乳腺癌患者血清中的DNA甲基化:一种独立的预后标志物。

DNA methylation in serum of breast cancer patients: an independent prognostic marker.

作者信息

Müller Hannes M, Widschwendter Andreas, Fiegl Heidi, Ivarsson Lennart, Goebel Georg, Perkmann Elisabeth, Marth Christian, Widschwendter Martin

机构信息

Department of Obstetrics and Gynecology, Innsbruck University Hospital, University of Innsbruck, Anichstrasse 35, A-6020 Innsbruck, Austria.

出版信息

Cancer Res. 2003 Nov 15;63(22):7641-5.

Abstract

Changes in the status of DNA methylation are one of the most common molecular alterations in human neoplasia. Because it is possible to detect these epigenetic alterations in the bloodstream of patients, we investigated whether aberrant DNA methylation in patient pretherapeutic sera is of prognostic significance in breast cancer. Using MethyLight, a high-throughput DNA methylation assay, we analyzed 39 genes in a gene evaluation set, consisting of 10 sera from metastasized patients, 26 patients with primary breast cancer, and 10 control patients. To determine the prognostic value of genes identified within the gene evaluation set, we finally analyzed pretreatment sera of 24 patients having had no adjuvant treatment (training set) to determine their prognostic value. An independent test set consisting of 62 patients was then used to test the validity of genes and combinations of genes, which in the training set were found to be good prognostic markers. In the gene evaluation set we identified five genes (ESR1, APC, HSD17B4, HIC1, and RASSF1A). In the training set, patients with methylated serum DNA for RASSF1A and/or APC had the worst prognosis (P < 0.001). This finding was confirmed by analyzing serum samples from the independent test set (P = 0.007). When analyzing all 86 of the investigated patients, multivariate analysis showed methylated RASSF1A and/or APC serum DNA to be independently associated with poor outcome, with a relative risk for death of 5.7. DNA methylation of particular genes in pretherapeutic sera of breast cancer patients, especially of RASSF1A/APC, is more powerful than standard prognostic parameters.

摘要

DNA甲基化状态的改变是人类肿瘤中最常见的分子改变之一。由于有可能在患者血液中检测到这些表观遗传改变,我们研究了患者治疗前血清中异常DNA甲基化在乳腺癌中是否具有预后意义。我们使用一种高通量DNA甲基化检测方法MethyLight,分析了一个基因评估集中的39个基因,该评估集包括10份来自转移性患者的血清、26份原发性乳腺癌患者的血清以及10份对照患者的血清。为了确定基因评估集中所鉴定基因的预后价值,我们最终分析了24例未接受辅助治疗患者(训练集)的治疗前血清,以确定其预后价值。然后使用一个由62例患者组成的独立测试集来检验在训练集中被发现是良好预后标志物的基因及基因组合的有效性。在基因评估集中,我们鉴定出五个基因(ESR1、APC、HSD17B4、HIC1和RASSF1A)。在训练集中,RASSF1A和/或APC血清DNA甲基化的患者预后最差(P < 0.001)。通过分析独立测试集的血清样本证实了这一发现(P = 0.007)。在分析所有86例被调查患者时,多变量分析显示RASSF1A和/或APC血清DNA甲基化与不良预后独立相关,死亡相对风险为5.7。乳腺癌患者治疗前血清中特定基因的DNA甲基化,尤其是RASSF1A/APC的DNA甲基化,比标准预后参数更具预测力。

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