The performance of single and combination test strategies using visual inspection, cytology, high-risk HPV DNA and HPV16/18 to screen South African women with and without HIV-infection.

IF 3.1 2区医学 Q3 IMMUNOLOGY

Infectious Agents and Cancer Pub Date : 2024-05-09 DOI:10.1186/s13027-024-00586-3

Greta Dreyer, Cathy Visser, Gerrit Jan Dreyer, Matthys H Botha, Frederick H van der Merwe, Karin L Richter, Leon C Snyman

{"title":"The performance of single and combination test strategies using visual inspection, cytology, high-risk HPV DNA and HPV16/18 to screen South African women with and without HIV-infection.","authors":"Greta Dreyer, Cathy Visser, Gerrit Jan Dreyer, Matthys H Botha, Frederick H van der Merwe, Karin L Richter, Leon C Snyman","doi":"10.1186/s13027-024-00586-3","DOIUrl":null,"url":null,"abstract":"Background: Cervical cancer screening strategies should ideally be informed by population-specific data. Strategies recommended for secondary prevention, are often inadequately studied in populations with high cervical disease burdens. This report describes the test performance measured against CIN2 + /CIN3 + histology in HIV-positive women (HPW) and HIV-negative women (HNW) with the aim to determine the most effective strategies to identify South African women at risk.Methods: Primary screening using visual inspection, cytology and HPV DNA (cobas®) was performed in two South African provinces on 456 HPW and 639 HNW participating in the multicentric DiaVACCS trial. Histology was obtained for 91.7% screen-positive and 42.7% screen-negative participants, and unavailable histology was determined by multiple imputation to adjust for verification bias. Cross-sectional test performance was calculated for single and combination test strategies with and without intermediate risk categories using different cut-offs. Minimum acceptability for sensitivity and specificity, treatment and follow-up numbers were considered to evaluate strategies.Results: The only single test to reach acceptability in HPW was cytology (LSIL) [sensitivity 71.2%; specificity 90.5%; treatment 33.4%]; in HNW only HPV (hr) qualified [sensitivity 68.2%; specificity 85.2%; treatment 23.5%]. The universally best performing strategy which also resulted in smaller treatment numbers without intermediate risk group was primary HPV(hr), with treatment of both HPV(16/18) and cytology (ASCUS +) [HPW: sensitivity 73.6%; specificity 89.7%; treatment 34.7%. HNW: sensitivity 59.1%; specificity 93.6%; treatment 13.9%]. DNA testing for hrHPV (any) and hrHPV (16/18) was the best universally acceptable strategy with an intermediate risk category (early follow-up) in HPW [sensitivity 82.1%; specificity 96.4%; treatment 17.1%; follow-up 31.4%] and HNW [sensitivity 68.2%; specificity 96.7%; treatment 7.6%; follow-up 15.9%]. In comparison, using both HPV (16/18) and cytology (ASCUS +) as secondary tests in hrHPV positive women, decreased follow-up [HPW 13.8%, HNW 9.6%], but increased treatment [HPW 34.7%, HNW 13.9%].Conclusion: Using hrHPV (any) as primary and both HPV16/18 and cytology as secondary tests, was universally acceptable without an intermediate risk group. Strategies with follow-up groups improved screening performance with smaller treatment numbers, but with effective management of the intermediate risk group as prerequisite.","PeriodicalId":13568,"journal":{"name":"Infectious Agents and Cancer","volume":"19 1","pages":"22"},"PeriodicalIF":3.1000,"publicationDate":"2024-05-09","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11084067/pdf/","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Infectious Agents and Cancer","FirstCategoryId":"3","ListUrlMain":"https://doi.org/10.1186/s13027-024-00586-3","RegionNum":2,"RegionCategory":"医学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q3","JCRName":"IMMUNOLOGY","Score":null,"Total":0}

引用次数: 0

Abstract

Background: Cervical cancer screening strategies should ideally be informed by population-specific data. Strategies recommended for secondary prevention, are often inadequately studied in populations with high cervical disease burdens. This report describes the test performance measured against CIN2 + /CIN3 + histology in HIV-positive women (HPW) and HIV-negative women (HNW) with the aim to determine the most effective strategies to identify South African women at risk.

Methods: Primary screening using visual inspection, cytology and HPV DNA (cobas®) was performed in two South African provinces on 456 HPW and 639 HNW participating in the multicentric DiaVACCS trial. Histology was obtained for 91.7% screen-positive and 42.7% screen-negative participants, and unavailable histology was determined by multiple imputation to adjust for verification bias. Cross-sectional test performance was calculated for single and combination test strategies with and without intermediate risk categories using different cut-offs. Minimum acceptability for sensitivity and specificity, treatment and follow-up numbers were considered to evaluate strategies.

Results: The only single test to reach acceptability in HPW was cytology (LSIL) [sensitivity 71.2%; specificity 90.5%; treatment 33.4%]; in HNW only HPV (hr) qualified [sensitivity 68.2%; specificity 85.2%; treatment 23.5%]. The universally best performing strategy which also resulted in smaller treatment numbers without intermediate risk group was primary HPV(hr), with treatment of both HPV(16/18) and cytology (ASCUS +) [HPW: sensitivity 73.6%; specificity 89.7%; treatment 34.7%. HNW: sensitivity 59.1%; specificity 93.6%; treatment 13.9%]. DNA testing for hrHPV (any) and hrHPV (16/18) was the best universally acceptable strategy with an intermediate risk category (early follow-up) in HPW [sensitivity 82.1%; specificity 96.4%; treatment 17.1%; follow-up 31.4%] and HNW [sensitivity 68.2%; specificity 96.7%; treatment 7.6%; follow-up 15.9%]. In comparison, using both HPV (16/18) and cytology (ASCUS +) as secondary tests in hrHPV positive women, decreased follow-up [HPW 13.8%, HNW 9.6%], but increased treatment [HPW 34.7%, HNW 13.9%].

Conclusion: Using hrHPV (any) as primary and both HPV16/18 and cytology as secondary tests, was universally acceptable without an intermediate risk group. Strategies with follow-up groups improved screening performance with smaller treatment numbers, but with effective management of the intermediate risk group as prerequisite.

查看原文本刊更多论文

使用肉眼检查、细胞学、高危人乳头瘤病毒 DNA 和人乳头瘤病毒 16/18 对感染和未感染艾滋病毒的南非妇女进行筛查的单一和组合检测策略的性能。

背景：宫颈癌筛查策略最好以特定人群的数据为依据。在宫颈疾病负担较重的人群中，建议用于二级预防的策略往往没有得到充分研究。本报告介绍了针对 HIV 阳性妇女（HPW）和 HIV 阴性妇女（HNW）的 CIN2 + /CIN3 + 组织学检测性能，旨在确定识别南非高危妇女的最有效策略：在南非的两个省，对参加 DiaVACCS 多中心试验的 456 名 HPW 和 639 名 HNW 进行了目测、细胞学和 HPV DNA（cobas®）初级筛查。91.7%的筛查阳性参与者和42.7%的筛查阴性参与者获得了组织学结果，无法获得的组织学结果通过多重估算来确定，以调整验证偏差。使用不同的临界值计算了有中间风险类别和无中间风险类别的单一检验策略和组合检验策略的横断面检验性能。评估策略时考虑了灵敏度和特异性的最低可接受性、治疗和随访人数：在高危人群中，唯一达到可接受性的单一检测方法是细胞学检测（LSIL）[灵敏度为 71.2%；特异性为 90.5%；治疗率为 33.4%]；在高净人群中，只有 HPV（hr）符合条件[灵敏度为 68.2%；特异性为 85.2%；治疗率为 23.5%]。在没有中危人群的情况下，效果普遍最佳且治疗人数较少的策略是初级HPV（hr），同时治疗HPV（16/18）和细胞学（ASCUS +）[高危人群：灵敏度73.6%；特异性89.7%；治疗34.7%。HNW：敏感性59.1%；特异性93.6%；治疗率13.9%]。在高危人群[灵敏度 82.1%；特异性 96.4%；治疗 17.1%；随访 31.4%]和高净值人群[灵敏度 68.2%；特异性 96.7%；治疗 7.6%；随访 15.9%]中，对 hrHPV（任何一种）和 hrHPV（16/18）进行 DNA 检测是普遍接受的最佳策略，属于中等风险类别（早期随访）。相比之下，同时使用 HPV（16/18）和细胞学（ASCUS +）作为 hrHPV 阳性女性的辅助检测，会减少随访[HPW 13.8%，HNW 9.6%]，但会增加治疗[HPW 34.7%，HNW 13.9%]：结论：使用 hrHPV（任何一种）作为主要检测方法，HPV16/18 和细胞学作为辅助检测方法，在没有中级风险组的情况下是普遍可接受的。有随访组的策略提高了筛查效果，减少了治疗人数，但前提是对中危人群进行有效管理。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

求助全文

约1分钟内获得全文求助全文

来源期刊

Infectious Agents and Cancer ONCOLOGY-IMMUNOLOGY

CiteScore

5.80

自引率

2.70%

发文量

期刊介绍： Infectious Agents and Cancer is an open access, peer-reviewed online journal that encompasses all aspects of basic, clinical, epidemiological and translational research providing an insight into the association between chronic infections and cancer. The journal welcomes submissions in the pathogen-related cancer areas and other related topics, in particular: • HPV and anogenital cancers, as well as head and neck cancers; • EBV and Burkitt lymphoma; • HCV/HBV and hepatocellular carcinoma as well as lymphoproliferative diseases; • HHV8 and Kaposi sarcoma; • HTLV and leukemia; • Cancers in Low- and Middle-income countries. The link between infection and cancer has become well established over the past 50 years, and infection-associated cancer contribute up to 16% of cancers in developed countries and 33% in less developed countries. Preventive vaccines have been developed for only two cancer-causing viruses, highlighting both the opportunity to prevent infection-associated cancers by vaccination and the gaps that remain before vaccines can be developed for other cancer-causing agents. These gaps are due to incomplete understanding of the basic biology, natural history, epidemiology of many of the pathogens that cause cancer, the mechanisms they exploit to cause cancer, and how to interrupt progression to cancer in human populations. Early diagnosis or identification of lesions at high risk of progression represent the current most critical research area of the field supported by recent advances in genomics and proteomics technologies.