Extended HPV genotyping by the BD Onclarity assay: concordance with screening HPV-DNA assays, triage biomarkers, and histopathology in women from the NTCC2 study.

IF 3.7 2区 生物学 Q2 MICROBIOLOGY
Laura De Marco, Simonetta Bisanzi, Guglielmo Ronco, Pamela Mancuso, Francesca Carozzi, Elena Allia, Raffaella Rizzolo, Daniela Gustinucci, Helena Frayle, Jessica Viti, Anna Iossa, Elena Cesarini, Simonetta Bulletti, Basilio Passamonti, Silvia Gori, Laura Toniolo, Francesco Venturelli, Annarosa Del Mistro, Paolo Giorgi Rossi, Maria Benevolo
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引用次数: 0

Abstract

The use of clinically validated human papillomavirus (HPV) assays is recommended in cervical cancer screening, and extended genotyping is getting attention as a triage biomarker because of the different oncogenic risk of the high-risk HPV genotypes. We compared the results of the Becton & Dickinson (BD) Onclarity HPV assay, on the residual baseline cervico-vaginal specimens of the NTCC2 trial, to those of the screening HPV-DNA assay (Cobas 4800 or HC2) and to cytology, p16/ki67 and E6/E7 mRNA triage results. We genotyped virtually all HPV-positive women and a consecutive sample of HPV-negatives. Among the 3,129 baseline-positives, 75.5% (k = 0.368) were BD-positive, as were 5 of the 333 baseline-negatives (1.5%). The concordance between BD and HPV-DNA screening test was 87% for Cobas (1,250/1,436) and 65.9% for HC2 (1,115/1,693). A higher than the recommended positivity threshold for Onclarity would increase the agreement but would not improve concordance in the overall screening population. Among the baseline-positive cases, we observed an increasing trend of BD positivity with cytology severity (from 71.6% in negative for intraepithelial lesion of malignancy to 95.1% in ASC-H+ samples), with histologically confirmed CIN3 (96.9%), with p16/ki67 dual staining positivity (90.9% among the positive and 69.6% among the negative specimens), and with E6/E7 mRNA positivity (93.4% in the mRNA-positive cases vs 39.7% among the mRNA-negatives). Our findings confirm some disagreement among different HPV assays used for screening. Nevertheless, the agreement is substantial for women with high-grade cytology, histologically confirmed CIN3, and p16/ki67 or mRNA positivity at triage, thus confirming a good clinical performance of all the tests used.The NTCC2 trial is registered as Clinicaltrials.gov identifier NCT01837693.

Importance: Large randomized clinical trials have demonstrated that human papillomavirus (HPV) testing for high-risk types is more effective than cytology in detecting pre-cancerous lesions and preventing cervical cancer. Its use is being implemented in cervical cancer screening in several countries. The most recent guidelines recommend a risk-based management. It is therefore important to assess the individual risk of having/developing high-grade lesions of women testing high-risk HPV-positive. A crucial viral factor influencing the risk is the HPV genotype since different types are associated to different carcinogenetic risks. Understanding the degree of concordance among different assays targeting either HPV presence/type(s) or cellular morphology and proteins' expression provides knowledge useful to better define how these tests can be used in screening protocols for an effective triage and to anticipate the possible implementation issues. Our study shows that the concordance between tests is higher when the infections have a higher probability of producing a clinically relevant lesion.

通过 BD Onclarity 检测法进行扩展 HPV 基因分型:与 NTCC2 研究中妇女的 HPV-DNA 检测法、分流生物标志物和组织病理学相一致。
在宫颈癌筛查中建议使用经过临床验证的人乳头瘤病毒(HPV)检测方法,由于高危 HPV 基因型的致癌风险不同,扩展基因分型作为一种分诊生物标志物受到了关注。我们比较了 Becton & Dickinson (BD) Onclarity HPV 检测法对 NTCC2 试验中残留的基线宫颈阴道标本的检测结果、筛查 HPV-DNA 检测法(Cobas 4800 或 HC2)的检测结果以及细胞学、p16/ki67 和 E6/E7 mRNA 分流结果。我们对几乎所有 HPV 阳性的妇女和 HPV 阴性的连续样本进行了基因分型。在 3129 位基线阳性者中,75.5%(k = 0.368)为 BD 阳性,333 位基线阴性者中有 5 位(1.5%)为 BD 阳性。Cobas 的 BD 与 HPV-DNA 筛查测试的一致性为 87%(1,250/1,436),HC2 为 65.9%(1,115/1,693)。高于建议的 Onclarity 阳性阈值会增加一致性,但不会提高整体筛查人群的一致性。在基线阳性病例中,我们观察到随着细胞学严重程度的增加,BD 阳性率呈上升趋势(从恶性上皮内病变阴性的 71.6% 到 ASC-H+ 样本的 95.1%)。9%)、p16/ki67 双染色阳性(阳性标本占 90.9%,阴性标本占 69.6%)和 E6/E7 mRNA 阳性(mRNA 阳性病例占 93.4%,mRNA 阴性病例占 39.7%)。我们的研究结果证实,用于筛查的不同 HPV 检测方法之间存在一些分歧。尽管如此,对于细胞学分级较高、组织学确诊为 CIN3、p16/ki67 或 mRNA 阳性的妇女,筛查结果的一致性还是很高的,从而证实了所有检测方法都具有良好的临床表现。NTCC2 试验的注册号为 Clinicaltrials.gov identifier NCT01837693:大型随机临床试验表明,在检测宫颈癌前病变和预防宫颈癌方面,高危型人类乳头瘤病毒(HPV)检测比细胞学检查更有效。一些国家已开始在宫颈癌筛查中使用这种方法。最新的指南建议采用基于风险的管理方法。因此,评估高危型 HPV 阳性妇女发生/发展高级别病变的个体风险非常重要。影响风险的一个关键病毒因素是 HPV 基因型,因为不同类型的 HPV 有不同的致癌风险。了解针对 HPV 存在/类型或细胞形态和蛋白表达的不同检测方法之间的一致性程度,有助于更好地确定如何在筛查方案中使用这些检测方法进行有效分流,并预测可能出现的实施问题。我们的研究表明,当感染产生临床相关病变的概率较高时,检测之间的一致性较高。
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来源期刊
Microbiology spectrum
Microbiology spectrum Biochemistry, Genetics and Molecular Biology-Genetics
CiteScore
3.20
自引率
5.40%
发文量
1800
期刊介绍: Microbiology Spectrum publishes commissioned review articles on topics in microbiology representing ten content areas: Archaea; Food Microbiology; Bacterial Genetics, Cell Biology, and Physiology; Clinical Microbiology; Environmental Microbiology and Ecology; Eukaryotic Microbes; Genomics, Computational, and Synthetic Microbiology; Immunology; Pathogenesis; and Virology. Reviews are interrelated, with each review linking to other related content. A large board of Microbiology Spectrum editors aids in the development of topics for potential reviews and in the identification of an editor, or editors, who shepherd each collection.
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