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Human papilloma virus genotyping for the cross‐sectional and longitudinal probability of developing cervical intraepithelial neoplasia grade 2 or more

机译:人类乳头瘤病毒基因分型对发展为2级或以上宫颈上皮内瘤变的横断面和纵向可能性的影响

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摘要

Human papilloma virus (HPV) testing is more sensitive but less specific than cytology. We evaluated stand‐alone genotyping as a possible triage method. During a multicentre randomised controlled trial comparing HPV testing to conventional cytology, HPV‐positive women were referred to colposcopy and followed up if no high‐grade lesion was detected. HPV‐positive samples were genotyped by GP5+/GP6+ primed polymerase chain reaction followed by reverse line blot. Genotypes were hierarchically ordered by positive predictive value (PPV) for CIN grade 2 or more (CIN2+), and grouped by cluster analysis into three groups (A, B and C in decreasing order). Receiver operating characteristic curves were computed. Among 2,255 HPV‐positive women with genotyping, 239 CIN2+ (including 113 CIN3+) were detected at baseline or during a 3‐year follow‐up. HPV33 had the highest PPV with CIN2+ and CIN3+ as the endpoint and when considering lesions detected at baseline or also during follow‐up. HPV16 and HPV35 were the second and third, respectively. Cross‐sectional sensitivity for CIN2+ at baseline was 67.3% (95% CI 59.7–74.2), 91.8% (95% CI 86.6–95.5) and 94.7% (95% CI 90.2–97.6), respectively, when considering as “positive” any of the HPV types in group A (33, 16 and 35), A or B (31, 52, 18, 59 and 58) and A or B or C (39, 51, 56, 45 and 68). The corresponding cross‐sectional PPVs for CIN2+ were 15.8% 95% (CI 13.2–18.7), 12.0% (95% CI 10.3–13.9) and 9.6% (95% CI 8.2–11.1), respectively. HPV33, 16 and 35 confer a high probability of CIN2+ but this rapidly decreases when adding other genotypes.
机译:人乳头瘤病毒(HPV)检测比细胞学检测更为敏感,但特异性较低。我们评估了独立基因分型作为一种可能的分类方法。在一项将HPV检测与常规细胞学比较的多中心随机对照试验中,将HPV阳性妇女转诊为阴道镜检查,如果未检测到高级别病灶,则进行随访。 HPV阳性样品通过GP5 + / GP6 +引发的聚合酶链反应,然后进行反向线印迹进行基因分型。基因型按阳性预测值(PPV)对CIN 2级或更高(CIN2 +)进行分层排序,并通过聚类分析分为三组(降序排列的A,B和C)。计算接收器工作特性曲线。在2255名具有基因分型的HPV阳性女性中,在基线或3年随访期间检测到239个CIN2 +(包括113个CIN3 +)。当考虑基线或随访期间发现的病变时,HPV33的PPV最高,以CIN2 +和CIN3 +为终点。 HPV16和HPV35分别是第二和第三。当被视为“阳性”时,基线时CIN2 +的横断面敏感性分别为67.3%(95%CI 59.7–74.2),91.8%(95%CI 86.6–95.5)和94.7%(95%CI 90.2–97.6)。 A组(33、16和35),A或B(31、52、18、59和58)和A或B或C(39、51、56、45和68)中的任何HPV类型。 CIN2 +的相应横截面PPV分别为15.8%95%(CI 13.2-18.7),12.0%(95%CI 10.3-13.9)和9.6%(95%CI 8.2-11.1)。 HPV33、16和35具有很高的CIN2 +发生率,但是当添加其他基因型时,这种情况会迅速降低。

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