HIV-1 Infection Clinical Trial
Official title:
A Randomized Trial To Compare An HPV Test-And-Treat Strategy To A Cytology-Based Strategy For Prevention Of CIN 2+ In HIV-Infected Women
Women sometimes develop cancer in an area called the cervix, which is the opening to the
uterus, or womb. Women who have HIV are more likely to get this kind of cancer than women who
do not have HIV. Nearly all of these cancers are caused by another virus, called human
papilloma virus (or HPV). Other times, the cause of this cancer is not known.
The investigators are looking for a better way to prevent cervical cancer. This study is
comparing two different methods to prevent cancer of the cervix in women who have HIV. This
study will also see if these methods are safe and tolerable in women who have HIV.
The study had two components:
1. a randomized open-label comparison between immediate cryotherapy (test-and-treat
strategy; Arm A) and cytology-based strategy (Arm B) in participants detected with
high-risk HPV (hr-HPV), and
2. a brief cohort follow-up for participants for whom cryotherapy was inappropriate (Arm
C).
The study's primary objective was to evaluate the effectiveness of immediate cryotherapy (Arm
A) compared to the cytology-based strategy (Arm B).
The total target sample size was up to 450 (280 for Arms A and B, approximately 170 for Arm
C). Randomization to Arms A and B was stratified by use of antiretroviral therapy (ART) at
screening (taking any ART or not taking any ART) with institutional balancing.
All study participants were screened with the Abbott RealTime hr-HPV test (aHPV) to detect
hr-HPV infection.
At screening, the examiner also performed a visual inspection and colposcopy without biopsies
to determine whether the candidate's cervix was suitable for cryotherapy (see inclusion
criteria for definition).
Participants with cervical lesions inappropriate for cryotherapy were not eligible for
randomization (to Arms A or B) but were eligible to register to Arm C. Participants without
hr-HPV (by aHPV) were also eligible to register to Arm C if lesions were seen on the
screening colposcopy or if the screening cytology showed high-grade squamous intraepithelial
lesions (HSIL). Arm C provided a larger number of participants for assessments of HPV
genotypes found in CIN2+ (cervical intraepithelial neoplasia grade 2, 3, or invasive cancer)
biopsy specimens and of the effect of LEEP on prevalent hr-HPV infections. In addition, Arm C
provided important data for implementation of the HPV test-and-treat strategy including the
role of HPV testing in the management of women with extensive cervical lesions inappropriate
for cervical cryotherapy, hr-HPV negative women with cervical lesions or HSIL cytology.
Participants in Arm A undergo one or two cervical biopsies followed by immediate cervical
cryotherapy at entry. Up to two visible lesions were biopsied. If no lesions were seen, then
one normal-appearing area of the cervix was biopsied. Participants in Arm A received the
results of the biopsy, but participants received cryotherapy treatment regardless of the
results.
Participants in Arm B followed a cytology-based management plan involving three steps -
cytology, colposcopy with directed biopsies, and loop electrosurgical excision procedure
(LEEP), as needed.
Participants in Arms A and B were seen at weeks 26, 52, 78, 104 and 130 post entry for
evaluation using aHPV, HPV DNA PCR, cervical cytology, and cervical colposcopy and directed
biopsies for a total follow-up length of 130 weeks. Biopsies were expected for participants
with abnormal cytology and with visible cervical lesions on colposcopy.
Participants in Arm C undergo colposcopy and directed biopsies. If CIN2+ was detected by
biopsy, then LEEP was performed and a follow-up visit 26 weeks after these procedures was
scheduled for evaluation using aHPV, HPV DNA PCR, Xpert HPV, cervical cytology, and cervical
colposcopy and directed biopsies. After the week 26 visit, Arm C participants went off study.
All participants who had cryotherapy or LEEP were seen 4 weeks post-procedure to evaluate
potential adverse events (AEs) from the procedure.
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