The role of human papillomavirus testing in the management of women with low‐grade abnormalities: multicentre randomised controlled trial

Cotton, Seonaidh; Sharp, Linda; Little, Julian; Cruickshank, Margaret; Seth, Rashmi; Smart, Louise; Duncan, Ian D.; Harrild, Kirsten; Waugh, Norman

doi:10.1111/j.1471-0528.2010.02519.x

Cited by 25 publications

(24 citation statements)

References 50 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…4 At randomisation, an endocervical sample was taken to identify the presence of DNA of 14 high-risk human papillomavirus types (hrHPV) using a polymerase chain reaction (PCR) with GP5+/6+ primers and enzyme immunoassay identification. The results of HPV testing did not interfere with management.…”

Section: Tombola Trialmentioning

confidence: 99%

Human papillomavirus‐based triage of women showing a cervical cytology result of borderline or mild dyskaryosis

Arbyn

Martin‐Hirsch

Wentzensen

2010

BJOG

View full text Add to dashboard Cite

show abstract

Section: Tombola Trialmentioning

confidence: 99%

Human papillomavirus‐based triage of women showing a cervical cytology result of borderline or mild dyskaryosis

Arbyn

Martin‐Hirsch

Wentzensen

2010

BJOG

View full text Add to dashboard Cite

show abstract

“…Giving the fact that HPV testing has been shown to have similar sensitivity but more overdiagnosis than the Pap test [25][26][27][28], and also giving the fact that false negative results may be higher than previously suspected [25,26,32], primary screening with HPV testing in European countries as well as in the U.S. should be reconsidered. Resources saved in molecular testing may well be addressed in implementing vaccination strategies that are still underused and possibly must include males as well as women [44,45].…”

Section: Resultsmentioning

confidence: 99%

“…This false negative rate is similar to that observed by Cotton and coll. who showed that 22% of women who had CIN 2 or worse were HPV negative at baseline (TOMBOLA trial) [26]. It is difficult to accept these figures when one talks of extending rescreening intervals such as those proposed by HPV testing algorithms.…”

Section: Background Studiesmentioning

confidence: 99%

Reconsidering Primary HPV Testing in Cervical Cancer Screening

Liverani¹

2015

JLS

View full text Add to dashboard Cite

Abstract:Inappropriate testing for HPV types on healthy subjects increases costs without benefit and potentially results in overtreatment. HPV testing also has a negative psychosocial impact on women, increasing anxiety, stress, and concerns on sexual relationships. Giving the fact that HPV testing has been shown to have similar sensitivity but more overdiagnosis than cytology, and also giving the fact that false negative results may be higher than previously suspected, primary screening with HPV tests in European countries should be reconsidered. Resources saved in molecular testing may well be addressed in implementing vaccination strategies which are still underused, and may possibly include males as well as women.

show abstract

“…At the same conclusions arrived Cotton and coll. showing a false negative rate of 22% in women with a high grade lesions or worse who tested HPV negative at baseline (TOMBOLA trial) [14]. Nevertheless, a study designed to evaluate the efficacy of HPV-based strategies in four European randomised controlled trials showed that HPV testing was supposed to provide 60-70% greater protection against cervical cancer compared with cytology [15].…”

mentioning

confidence: 99%

Cervical Cancer Screening Strategies: Not the Test You Take, but the Decision You Make

Liverani¹,

Bolis²

2016

Gynecol Obstet

View full text Add to dashboard Cite

in Australia the National Cervical Screening Program will shift from cervical cytology every two years, to HPV DNA testing as the sole primary screening test every five years in women aged 25 to 74 years, together with the implementation of an active HPV vaccination program [1]. Conversely in Japan cervical screening using cytology every two years is still being recommended for population-based and opportunistic screening [2]. While Canadian guidelines also recommend cervical screening with cytology every 3 years [3], in Europe cervical cytology is recommended for women under 30-35 years, and HPV testing as the sole primary screening test every 5-10 years for women above 30-35 years [4]. Actually, guidelines do not represent the real situation in each European country. In the Netherlands, screening is well organised and relies on primary HPV testing every 5 years until 40 years of age and every 10 years for women aged 40 and beyond: no screening is provided for women under 30, nor over 60 years of age [5]. Other countries recommend cytology or HPV testing, and differences are marked even within the same country and sometimes within the same region. As a matter of fact in Italy there are regions employing cytology, other regions employing HPV DNA testing, and one local health unit employing HPV mRNA testing as the sole test, while some regions still do not implement organized screening programs [6]. In the U.S. guidelines for cervical cancer screening are well-structured and -in their effort to reach maximum cost-effectiveness -are articulated into several scenarios. Briefly, cytology alone every 3 years is recommended for women under 30 years, while women aged 30 to 65 years may either continue screening with cervical cytology every 3 years, or offered cotesting (cytology + HPV testing) if they want to be screened less frequently [7][8][9]. Interestingly, European guidelines insist that only one primary test (either cytology or HPV testing) should be used at any given age in cervical cancer screening. In the U.S. until more data and algorithm development will be available, it is judged premature to use HPV testing alone as a valid screening approach [10]. This is the reason why the latest edition of the CDC guidelines published in June 2015 state that HPV testing should not be performed in screening for cervical cancer as a stand-alone test (i.e., without a concurrent Pap test) [11].As we can see, there is considerable disagreement worldwide about cervical cancer screening strategies between countries that have similar population characteristics. The main problem employing HPV testing based strategies in cervical cancer screening is the fact that both positive and negative HPV results are often misinterpreted or overestimated. An HPV positive, cytology negative woman, should repeat both tests after one year interval. Actually, patients too often tend to undergo immediate colposcopic examination, increasing health care costs and patients' anxiety, without benefit and potentially resulting in overtreatments. Not r...

show abstract

The role of human papillomavirus testing in the management of women with low‐grade abnormalities: multicentre randomised controlled trial

Cited by 25 publications

References 50 publications

Human papillomavirus‐based triage of women showing a cervical cytology result of borderline or mild dyskaryosis

Human papillomavirus‐based triage of women showing a cervical cytology result of borderline or mild dyskaryosis

Reconsidering Primary HPV Testing in Cervical Cancer Screening

Cervical Cancer Screening Strategies: Not the Test You Take, but the Decision You Make

Contact Info

Product

Resources

About