Poljak Mario, Oštrbenk Anja, Seme Katja, Šterbenc Anja, Jančar Nina, Vrtačnik Bokal Eda
Institute of Microbiology and Immunology, Faculty of Medicine, University of Ljubljana, Ljubljana, Slovenia.
Institute of Microbiology and Immunology, Faculty of Medicine, University of Ljubljana, Ljubljana, Slovenia.
J Clin Virol. 2016 Mar;76 Suppl 1:S29-S39. doi: 10.1016/j.jcv.2015.11.021. Epub 2015 Nov 19.
Testing cervical smears for the presence of high-risk human papillomaviruses (hrHPV) increases the sensitivity for detecting women with underlying high-grade cervical intraepithelial neoplasia (CIN) and provides better and longer protection against invasive cervical cancer compared to cytology testing alone. The Abbott RealTime High Risk HPV test (RealTime) is a hrHPV DNA test with concurrent partial genotyping for HPV16 and HPV18 and aggregate detection of 12 other hrHPV types that have been extensively analytically and clinically evaluated over the last 6 years.
To provide the first 3-year longitudinal data regarding the clinical performance of RealTime, the risk of CIN2+ according to various negative baseline characteristics, and baseline and future risk for CIN2+ at 3 years for women with baseline infection with various hrHPV types were assessed in a cohort of 3,920 Slovenian women that had hrHPV DNA and/or cytology in 36- to 48-month follow-up results after a baseline screening round in 2009/2010.
A total of 36 CIN2+ cases were identified in the second screening round. Of these, 17 CIN2+ cases were identified passively through questionnaires/data registries and 19 cases actively as the result of actions triggered by second-round cytology and/or HPV test results. Accumulation of CIN2+ cases during follow-up occurred predominantly in woman with normal cytology at baseline. Among women >30 years old, significantly better protection against CIN2+ at 3 years was associated with a negative hrHPV DNA result at baseline (risk for CIN2+ 0.04% [95 CI, 0.00-0.22%]) than by normal cytology at baseline (risk for CIN2+ 0.68% [95 CI, 0.40-1.08%]). Women with baseline HPV16 infection had a significantly higher risk of CIN2+ at baseline (21.9% [95 CI, 15.2-30.4%]) and baseline plus future risk at 3 years for CIN2+ (33.3% [95 CI, 24.7-44.0%]) in comparison to women with baseline non-HPV16/18 hrHPV infection (7.0% [95 CI, 4.6-10.2%]) or those that were hrHPV-positive (11.7% [95 CI, 9.1-14.9%]).
3-year longitudinal data reinforce evidence from previous studies that RealTime can be safely used in primary HPV-based cervical cancer screening. Concurrent partial genotyping for HPV16/18 should be strongly considered as a triage method for HPV screen-positive women.
检测宫颈涂片是否存在高危型人乳头瘤病毒(hrHPV)可提高检测出患有潜在高级别宫颈上皮内瘤变(CIN)女性的敏感性,与单独进行细胞学检测相比,能提供更好且更持久的预防浸润性宫颈癌的保护。雅培实时高危型HPV检测(实时检测)是一种hrHPV DNA检测,可同时对HPV16和HPV18进行部分基因分型,并对其他12种hrHPV类型进行综合检测,在过去6年中已进行了广泛的分析和临床评估。
为了提供关于实时检测临床性能的首份3年纵向数据,在一组3920名斯洛文尼亚女性队列中,评估了根据各种阴性基线特征得出的CIN2+风险,以及基线感染各种hrHPV类型的女性在3年时CIN2+的基线和未来风险,这些女性在2009/2010年进行基线筛查后,在36至4个月的随访结果中进行了hrHPV DNA和/或细胞学检测。
在第二轮筛查中总共确定了36例CIN2+病例。其中,17例CIN2+病例通过问卷/数据登记被动确定,19例通过第二轮细胞学和/或HPV检测结果触发的行动主动确定。随访期间CIN2+病例的累积主要发生在基线细胞学正常的女性中。在30岁以上的女性中,与基线时hrHPV DNA检测结果为阴性(CIN2+风险为0.04%[95%CI,0.00 - 0.22%])相比,基线时细胞学正常(CIN2+风险为0.68%[95%CI,0.40 - 1.08%])在3年时对CIN2+的保护效果明显更好。与基线时非HPV16/18 hrHPV感染的女性(7.0%[95%CI,4.6 - 10.2%])或hrHPV阳性的女性(11.7%[95%CI,9.1 - 14.9%])相比,基线时HPV16感染的女性在基线时CIN2+的风险显著更高(21.9%[95%CI,15.2 - 30.4%]),在3年时基线加未来CIN2+的风险也更高(33.3%[95%CI,24.7 - 44.0%])。
3年纵向数据强化了先前研究的证据,即实时检测可安全用于基于HPV的原发性宫颈癌筛查。对于HPV筛查阳性的女性,应强烈考虑将HPV16/18的同时部分基因分型作为一种分流方法。
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