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结直肠癌患者血浆中游离循环肿瘤相关DNA的检测及其与预后的关系。

Detection of free-circulating tumor-associated DNA in plasma of colorectal cancer patients and its association with prognosis.

作者信息

Lecomte Thierry, Berger Anne, Zinzindohoué Franck, Micard Stéphanie, Landi Bruno, Blons Hélène, Beaune Philippe, Cugnenc Paul-Henri, Laurent-Puig Pierre

机构信息

Laboratoire de Toxicologie Moléculaire INSERM, Paris, France.

出版信息

Int J Cancer. 2002 Aug 10;100(5):542-8. doi: 10.1002/ijc.10526.

Abstract

Tumor cells are characterized by specific genetic alterations. When such genetic alterations are identified in body fluid including plasma, regardless of the presence of detectable tumor cells, it shows the existence of free-circulating tumor-associated DNA. The objective of our study was to assess the prognostic value of free-circulating tumor-associated DNA in colorectal cancer patients' plasma. The first step of our work was to find common genetic alterations in tumors that would subsequently be used for plasma DNA screening. We focused on KRAS2 mutations in codons 12 and 13 by the mutant allele-specific amplification (MASA) method and p16 hypermethylation by the methylation-specific polymerase chain reaction (MSP) method. Patients with a tumor presenting either alteration were selected for plasma screening; 58 tumors were analyzed for KRAS2 mutations and tested for p16 gene promoter methylation. Survival and recurrence rates were assessed in patients with and without free-circulating tumor-associated DNA alterations in plasma. Of the 58 tumors analyzed, 39 (67%) demonstrated either one or both of the studied genetic alterations. Twenty-two (38%) were mutated at KRAS2, and an identical alteration was detected in 10 (45%) of the 22 corresponding plasma samples. Thirty-one (53%) had p16 gene promoter hypermethylation that could also be detected in the plasma in 21 cases (68%). Among the 39 patients who had one or the other alteration in tumor DNA, 37 had at least one reliable plasma test. In 26 (70%) of the 37 patients, free-circulating tumor-associated DNA was detected in plasma. The 2-year overall survival rate was 48% in the group where free-circulating tumor-associated DNA was detected in plasma and 100% in the one where free-circulating tumor-associated DNA was not detected in plasma (p < 0.03). Among these 37 patients, 25 patients had a stage I, II or III disease. In this subgroup of patients, the 2-year recurrence-free survival rate for the 17 patients with free-circulating tumor-associated DNA detected in plasma was 66%, compared to 100% for the 8 patients without free-circulating tumor-associated DNA detected in plasma (p = 0.044). The presence of free-circulating tumor-associated DNA in plasma seems to be a relevant prognostic marker for patients with colorectal cancer and may be used to identify patients with a high risk of recurrence.

摘要

肿瘤细胞具有特定的基因改变特征。当在包括血浆在内的体液中鉴定出此类基因改变时,无论是否存在可检测到的肿瘤细胞,都表明存在游离循环肿瘤相关DNA。我们研究的目的是评估游离循环肿瘤相关DNA在结直肠癌患者血浆中的预后价值。我们工作的第一步是在肿瘤中寻找常见的基因改变,随后将其用于血浆DNA筛查。我们通过突变等位基因特异性扩增(MASA)方法关注KRAS2基因第12和13密码子的突变,以及通过甲基化特异性聚合酶链反应(MSP)方法关注p16基因的高甲基化。选择存在上述任何一种改变的肿瘤患者进行血浆筛查;对58个肿瘤进行KRAS2突变分析并检测p16基因启动子甲基化情况。对血浆中存在或不存在游离循环肿瘤相关DNA改变的患者评估生存率和复发率。在分析的58个肿瘤中,39个(67%)显示出一种或两种所研究的基因改变。22个(38%)在KRAS2基因发生突变,在22个相应血浆样本中的10个(45%)检测到相同改变。31个(53%)存在p16基因启动子高甲基化,其中21例(68%)在血浆中也能检测到。在肿瘤DNA存在一种或另一种改变的39例患者中,37例进行了至少一次可靠的血浆检测。在这37例患者中的26例(70%)血浆中检测到游离循环肿瘤相关DNA。血浆中检测到游离循环肿瘤相关DNA的组2年总生存率为48%,血浆中未检测到游离循环肿瘤相关DNA的组为100%(p<0.03)。在这37例患者中,25例患者疾病分期为I、II或III期。在该亚组患者中,血浆中检测到游离循环肿瘤相关DNA的17例患者2年无复发生存率为66%,而血浆中未检测到游离循环肿瘤相关DNA的8例患者为100%(p = 0.044)。血浆中游离循环肿瘤相关DNA的存在似乎是结直肠癌患者的一个相关预后标志物,可用于识别复发风险高的患者。

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