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宫颈癌前病变患者尿液中肿瘤抑制基因的启动子高甲基化

Promoter hypermethylation of tumor suppressor genes in urine from patients with cervical neoplasia.

作者信息

Feng Qinghua, Hawes Stephen E, Stern Joshua E, Dem Amadou, Sow Papa Salif, Dembele Birama, Toure Papa, Sova Pavel, Laird Peter W, Kiviat Nancy B

机构信息

Department of Pathology, School of Medicine, University of Washington, Seattle, WA 98109, USA.

出版信息

Cancer Epidemiol Biomarkers Prev. 2007 Jun;16(6):1178-84. doi: 10.1158/1055-9965.EPI-06-0694.

Abstract

We examined the feasibility of using detection of high-risk human papillomavirus (HPV) DNA in combination with the presence of aberrantly methylated genes (DAPK1, RARB, TWIST1, and CDH13) for urine-based cervical cancer screening. Urine samples from 129 Senegalese women, aged 35 years or older, 110 with (same day) biopsy-proven cervical neoplasia [cervical intraepithelial neoplasia grade 1 (CIN-1): n = 9; CIN-2-3/carcinoma in situ (CIS): n = 29; invasive cervical cancer (ICC): n = 72], and 19 without cervical neoplasia on biopsy were examined. Hypermethylation of at least one of the four genes identified 62% of ICC and 28% of CIN-2-3/CIS and was present in only 4% of CIN-1 or normal urines. High-risk HPV DNA was detected in urine in 70% of those with biopsy-proven ICC, 59% of those with CIN-2-3/CIS on biopsy, 44% of those with CIN-1 on biopsy, and only 11% of women negative for cervical neoplasia on biopsy. Urine-based detection of either high-risk HPV or hypermethylation of any of the four genes identified 84% of ICC, 64% of CIN-2-3/CIS, 44% of CIN-1, but only 19% of women negative for cervical neoplasia. The sensitivity for detection of CIN-2-3/CIS/ICC by high-risk HPV DNA or aberrant DNA methylation of four genes seems to be comparable to that of an exfoliated cervical cytology. This study shows the potential feasibility of using molecular markers detected in urine for cervical cancer screening.

摘要

我们研究了联合检测高危型人乳头瘤病毒(HPV)DNA与异常甲基化基因(DAPK1、RARB、TWIST1和CDH13)用于基于尿液的宫颈癌筛查的可行性。收集了129名35岁及以上塞内加尔女性的尿液样本,其中110名经活检证实患有宫颈肿瘤[宫颈上皮内瘤变1级(CIN-1):n = 9;CIN-2-3/原位癌(CIS):n = 29;浸润性宫颈癌(ICC):n = 72],另外19名活检未发现宫颈肿瘤。四种基因中至少一种基因的高甲基化可识别出62%的ICC和28%的CIN-2-3/CIS,仅4%的CIN-1或正常尿液样本中存在该情况。活检证实为ICC的患者中,70%尿液检测出高危型HPV DNA;活检为CIN-2-3/CIS的患者中,59%尿液检测出高危型HPV DNA;活检为CIN-1的患者中,44%尿液检测出高危型HPV DNA;活检宫颈肿瘤阴性的女性中,仅11%尿液检测出高危型HPV DNA。基于尿液检测高危型HPV或四种基因中任何一种基因的高甲基化,可识别出84%的ICC、64%的CIN-2-3/CIS、44%的CIN-1,但仅19%活检宫颈肿瘤阴性的女性。通过高危型HPV DNA或四种基因的异常DNA甲基化检测CIN-2-3/CIS/ICC的敏感性似乎与脱落宫颈细胞学检查相当。本研究表明了利用尿液中检测到的分子标志物进行宫颈癌筛查的潜在可行性。

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