h High-risk human papillomavirus (HPV) DNA/RNA testing provides higher sensitivity but lower specificity than cytology for the identification of high-grade cervical intraepithelial neoplasia (CIN). Several new HPV tests are now available for this purpose, and a direct comparison of their properties is needed. Seven tests were evaluated with samples in liquid PreservCyt transport medium from 1,099 women referred for colposcopy: the Hybrid Capture 2 (Qiagen), Cobas (Roche), PreTect HPV-Proofer (NorChip), Aptima HPV (Gen-Probe), and Abbott RealTime assays, the BD HPV test, and CINtec p16INK4a cytology (mtm laboratories) immunocytochemistry. Sensitivity, specificity, and positive predictive value (PPV) were based on the worst histology found on either the biopsy or the treatment specimen after central review. Three hundred fifty-nine women (32.7%) had CIN grade 2؉ (CIN2؉), with 224 (20.4%) having CIN3؉. For detection of CIN2؉, Hybrid Capture 2 had 96.3% sensitivity, 19.5% specificity, and 37.4% PPV. Cobas had 95.2% sensitivity, 24.0% specificity, and 37.6% PPV. The BD HPV test had 95.0% sensitivity, 24.2% specificity, and 37.8% PPV. Abbott RealTime had 93.3% sensitivity, 27.3% specificity, and 38.2% PPV. Aptima had 95.3% sensitivity, 28.8% specificity, and 39.3% PPV. PreTect HPV-Proofer had 74.1% sensitivity, 70.8% specificity, and 55.4% PPV. CINtec p16INK4a cytology had 85.7% sensitivity, 54.7% specificity, and 49.1% PPV. Cytology of a specimen taken at colposcopy (mild dyskaryosis or worse) had 88.9% sensitivity, 58.1% specificity, and 50.7% PPV. Our study confirms that, in a referral setting, HPV testing by a number of different tests provides high sensitivity for high-grade disease. Further work is needed to confirm these findings in a routine screening setting.
High-risk (HR) human papillomavirus (HPV) is a necessary factor for the development of cervical cancer (31), but the presence of HR HPV DNA does not invariably lead to disease. We have shown that the detection of HR HPV DNA provides high sensitivity but has lower specificity than cytology for the identification of high-grade cervical lesions in a screening population in the United Kingdom (9), and this finding has been replicated in several other studies (1, 3, 8, 15-17, 21, 22, 26, 27). In addition, prospective studies have shown that HPV DNA-positive women who do not have disease initially are significantly more likely to develop high-grade squamous intraepithelial lesions (SILs) within 10 years than women with a negative HPV DNA test (4,12,14,18). If testing for HR HPV DNA is to be used as a primary cervical screening test, refinements or additional tests are highly desirable to improve its specificity while retaining its very high sensitivity. Candidates include HPV typing, detection of HPV E6/E7 mRNA tests, and p16INK4a cytology, which have shown higher specificity than HPV DNA testing (10,19).The introduction of a liquid-based medium for collection of cytological specimens has allowed other molecular techniques to be evaluated more easily as adjunc...
