Stratified risk of high-grade cervical disease using onclarity HPV extended genotyping in women, ≥25 years of age, with NILM cytology

Stoler, Mark H.; Parvu, Valentin; Yanson, Karen; Cooper, Charles K.; Andrews, Jeffrey C

doi:10.1016/j.ygyno.2018.12.024

Cited by 40 publications

(48 citation statements)

References 30 publications

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“…In another study, however, Cuzick et al showed that HPV16 retains its high risk, while HPV31 and especially HPV33 emerge as important types with higher positive predictive values (PPVs) than HPV18 [19] . Thus, individual HPV genotypes within commonly grouped categories of "Other hrHPV types" do not carry equal risk, and separate assessment of HPV 33 and 31 needs to be reconsidered [19,20] . In this cohort, Other hrHPV infection was most prevalent, accounting for 79.9% of hrHPV infections, and contributed to substantial cytological abnormalities as well as large proportions of CIN2/CIN3 (62.7% and 43.9%, respectively) over 3-year follow-up.…”

Section: Discussionmentioning

confidence: 99%

“…Moreover, the current HPV assays may require a modification, such as adding more previously low prevalence hrHPV subtypes and separating each genotype [25] . Recently, a growing number of low-cost HPV tests have been developed to distinguish extended genotypes [20,26] , which makes the better understanding of individual types and the better evaluation of vaccine effects. In order to reduce the burden of cervical diseases, the bivalent vaccine (covering HPV16 and 18), quadrivalent vaccine (covering HPV 16,18,6 and 11) and nonvalent vaccine were licensed in China successively since 2016.…”

Section: Discussionmentioning

confidence: 99%

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Type-specific Distribution of Cervical hrHPV Infection and the Association with Cytological and Histological Results in a Large Population-based Cervical Cancer Screening Program: Baseline and 3-year Longitudinal Data

Song

Ai-min

et al. 2020

J. Cancer

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Objectives: This study aimed to describe the study design, and to analyze the type-specific distribution of cervical high-risk human papillomavirus (hrHPV) infection and its association with cytological and histological results in a large population-based screening program in Buji Street, Shenzhen, China. Methods: A total of 10,186 women aged 21-70 years were co-tested by Cobas4800 HPV assay and liquid-based cytology. Women were referred to colposcopy by virtue of being HPV16/18-positive, Other hrHPV-positive/ cytology >ASCUS, or HPV-negative/ cytology >LSIL. Three-year histological follow-up data were recorded. Results: The overall prevalence of hrHPV infection was 11.1%; among them, the highest type was Other hrHPV (8.9%), followed by HPV16 (1.6%) and HPV18 (0.6%). Moreover, the prevalence of hrHPV and that of HPV16 increased with cytological severity (Ptrend <0.001). In the baseline phase, 106 women had cervical intraepithelial neoplasia 2/3 (CIN2/3) and six had cervical cancers. During 3-year follow-up, 12 cases of CIN2/3 and no cancers were identified. For HPV16-positive women with normal cytology, the baseline risks of CIN2/3 or worse (CIN2+/CIN3+) were 15.5% (7.0-23.9%) and 4.2% (1.4-8.5%) respectively. For Other hrHPV-positive women with normal cytology, the cumulative 3-year risks of CIN2+/CIN3+ were 3.1% (1.0-5.2%) and 0.7% (0.3-2.1%) respectively. Strikingly, 75.8% (322/425) of abnormal cytology and 50.9% (29/57) HSIL cytology were attributed to Other hrHPV infection in HPV-positive women. Similarly, Other hrHPV infection led to large proportions of CIN2 (62.7%) and CIN3+ (43.9%) over 3-year follow-up. Conclusions: The co-testing modality is a feasible, effective and safe option for cervical cancer screening in urban population. Great importance should also be attached to 'genotypes excluding HPV16/18' and separate detection of each genotype when considering screening and vaccination strategy.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Type-specific Distribution of Cervical hrHPV Infection and the Association with Cytological and Histological Results in a Large Population-based Cervical Cancer Screening Program: Baseline and 3-year Longitudinal Data

Song

Ai-min

et al. 2020

J. Cancer

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“…Prevalence estimates were restricted to subjects with key demographic information, evaluable liquid-based cytology results, and valid HPV assay results for all genotypes. For risk determination, values were determined hierarchically using an order established previously by Stoler and colleagues [16]. In that report, a Bayesian model (derived by Markov-Chain Monte Carlo methods) was utilized to hierarchically rank the nine different genotype Onclarity channels based on ≥CIN3 baseline risk (for subjects with co-infections, the model assigned the ≥CIN3 risk as equal to the highest-risk genotype).…”

Section: Discussionmentioning

confidence: 99%

“…The design of the Onclarity HPV trial has been described previously in depth [8,15,16]. In brief, 33,858 subjects, ≥21 years, undergoing routine cervical cancer screening were recruited at 31 clinical sites in 17 states.…”

Section: Study Design and Enrollment Visitmentioning

confidence: 99%

Risk detection for high-grade cervical disease using Onclarity HPV extended genotyping in women, ≥21 years of age, with ASC-US or LSIL cytology

Stoler

Parvu

Yanson

et al. 2019

Gynecologic Oncology

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• HPV genotyping stratifies risk of ≥CIN2 or ≥CIN3 in women ≥21 years with ASC-US or LSIL cytology. • Women with HPV 16 had the greatest risk of ≥CIN2 or ≥CIN3 which is followed by those with HPV 31 in most instances. • HPV genotypes such as 51, 35/39/68, and 56/59/66 have a lower risk of ≥CIN2 or ≥CIN3 and may not require colposcopy. • These results support the use of HPV genotyping in risk-based management algorithms for women with either ASC-US or LSIL

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“…It is not known how many more would have been diagnosed with random biopsy. A US trial reported an 8.5% prevalence of CIN3 in women with normal cytology referred to colposcopy and biopsy (directed or random) after a single positive test for HPV16/18 . Women with HPV infection and normal cytology form the majority of the triage population, and there is an urgent need for better evidence to inform colposcopy management guidelines for these women.…”

Section: Discussionmentioning

confidence: 99%

Triaging women with human papillomavirus infection and normal cytology or low‐grade dyskaryosis: evidence from 10‐year follow up of the ARTISTIC trial cohort

Gilham

Sargent

Peto

2019

BJOG

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Objectives To estimate long‐term cervical intraepithelial neoplasia grade 3 (CIN3) risks associated with different triage strategies for human papillomavirus positive (HPV+) women with a view to reducing unnecessary referrals. Design The ARTISTIC trial cohort was recruited in Manchester in 2001–03 and was followed up for CIN3 and cancer notification through national registration until December 2015. Results The 10‐year cumulative risk of CIN3+ was much higher for women with HPV16/18 infection (19.4%, 95% CI 15.8–23.8% with borderline/low‐grade cytology and 10.7%, 95% CI 8.3–13.9% with normal cytology) than for those with other HPV types (7.3%, 95% CI 5.4–9.7% with borderline/low‐grade cytology and 3.2%, 95% CI 2.2–4.5% with normal cytology). Among the 379 women with normal to low‐grade cytology and new HPV infection, the 10‐year cumulative CIN3+ risk was 2.9% (95% CI 1.6–5.2%). Conclusions The CIN3 risk is confined to women with persistent type‐specific HPV so partial genotyping test assays identifying HPV16/18 as a minimum are essential for efficient risk stratification. Immediate referral to colposcopy for HPV+ women with borderline or low‐grade cytology and referral after a year if still HPV+ with normal cytology may be unnecessary. Low‐grade lesions can safely be retested to identify those with persistent HPV. Recall intervals of 1 year for HPV16/18 and 2 years for other high‐risk HPVs are justified for women with normal cytology and might also be considered for women with borderline/low‐grade cytology. The minimal risk of invasive cancer that has progressed beyond stage 1A must be weighed against the advantages for patients and the NHS of reducing the number of referrals to colposcopy. Tweetable abstract Cervical screening would be better for women and cheaper for the NHS if women with HPV and normal to low‐grade cytology were retested after a year or two when many infections will have cleared.

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Stratified risk of high-grade cervical disease using onclarity HPV extended genotyping in women, ≥25 years of age, with NILM cytology

Cited by 40 publications

References 30 publications

Type-specific Distribution of Cervical hrHPV Infection and the Association with Cytological and Histological Results in a Large Population-based Cervical Cancer Screening Program: Baseline and 3-year Longitudinal Data

Type-specific Distribution of Cervical hrHPV Infection and the Association with Cytological and Histological Results in a Large Population-based Cervical Cancer Screening Program: Baseline and 3-year Longitudinal Data

Risk detection for high-grade cervical disease using Onclarity HPV extended genotyping in women, ≥21 years of age, with ASC-US or LSIL cytology

Triaging women with human papillomavirus infection and normal cytology or low‐grade dyskaryosis: evidence from 10‐year follow up of the ARTISTIC trial cohort

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Stratified risk of high-grade cervical disease using onclarity HPV extended genotyping in women, ≥25 years of age, with NILM cytology

Cited by 40 publications

References 30 publications

Type-specific Distribution of Cervical hrHPV Infection and the Association with Cytological and Histological Results in a Large Population-based Cervical Cancer Screening Program: Baseline and 3-year Longitudinal Data

Type-specific Distribution of Cervical hrHPV Infection and the Association with Cytological and Histological Results in a Large Population-based Cervical Cancer Screening Program: Baseline and 3-year Longitudinal Data

Risk detection for high-grade cervical disease using Onclarity HPV extended genotyping in women, ≥21 years of age, with ASC-US or LSIL cytology

Triaging women with human papillomavirus infection and normal cytology or low‐grade dyskaryosis: evidence from 10‐year follow up of the ARTISTIC trial cohort

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Product

Resources

About

Stratified risk of high-grade cervical disease using onclarity HPV extended genotyping in women, ≥25 years of age, with NILM cytology

Risk detection for high-grade cervical disease using Onclarity HPV extended genotyping in women, ≥21 years of age, with ASC-US or LSIL cytology