Clinical Trial Details
— Status: Not yet recruiting
Administrative data
| NCT number |
NCT05173324 |
| Other study ID # |
PP202111-31 |
| Secondary ID |
|
| Status |
Not yet recruiting |
| Phase |
Phase 3
|
| First received |
|
| Last updated |
|
| Start date |
February 1, 2023 |
| Est. completion date |
June 30, 2027 |
Study information
| Verified date |
August 2022 |
| Source |
International Agency for Research on Cancer |
| Contact |
Armando Baena, MSc, PhD |
| Phone |
+33 4 72 73 88 55 |
| Email |
baenaa[@]iarc.who.int |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
A 3-dose HPV vaccination scheme has shown to be safe and immunogenic in people living with
HIV (PLWH), although evidence on 1-dose, which is important to improve coverage, is scarce.
Available HPV vaccines only prevent new infections. Since a large fraction of WLWH is already
infected with HPV (>50%), vaccines' efficacy to prevent HPV infections (and therefore
cervical disease) in this population is limited. Current WHO cervical cancer screening
guidelines recommend treatment of the transformation zone (TZ) of WLWH who harbor HPV
infections either at initial screening or one year later. Therefore, HPV vaccination at the
time of the screening may improve vaccines efficacy conferring protection to newly growing
cells of the treated TZ against HPV infections/re-infections. Consequently, a
dual-intervention of HPV vaccination and HPV-based cervical screening in WLWH may alleviate
the burden of HPV-related disease by improving HPV vaccination efficacy while extending
cervical screening intervals. Nevertheless, implementing the dual-intervention may be
challenging particularly in some contexts without well-established cervical cancer screening
such as sub-Saharan African (SSA) countries. However, in these countries, at least 60% of
PLWH regularly attend ARV clinics to be monitored and receive ARV treatment (cART).
Therefore, integrating the dual-intervention into ARV clinics seems to be an efficient
approach to reduce loss to follow-up while improving overall coverages of HPV vaccination and
cervical screening. Such integration may also facilitate the implementation of a platform for
the delivery of other HPV-related preventive measures such as HPV therapeutic vaccines.
Nevertheless, little is known about the efficacy of HPV vaccination in WLWH to prevent HPV
infections and HPV-related diseases, especially in young adults. Moreover, evidence on how
best to conduct cervical cancer prevention, particularly recently released WHO guidelines,
through ARV clinics is limited. Therefore, IARC/WHO in collaboration with HRP/WHO and
colleagues in SSA proposes to conduct a hybrid effectiveness-implementation trial (H2VICTORY)
to evaluate the effectiveness of the dual-intervention of HPV vaccination and HPV-based
cervical screening to reduce HPV infections (and therefore, the risk of cervical cancer) in
WLWH aged 25-35 years while conducting implementation research to identify facilitators and
barriers for adoption and sustainability of proven evidence-based cervical cancer prevention
approaches integrated into ARV clinics across sub-Saharan Africa.
Description:
An effectiveness-implementation hybrid study is proposed to evaluate the effectiveness of a
dual intervention of HPV vaccination and HPV-triage-and-treat to reduce the risk of cervical
cancer and to study its integration into ARV clinics. The overarching hypothesis will be that
offering the dual intervention of HPV vaccination and HPV-triage-treat in young WLWH will
catalyze the preventive effect of both evidence-based interventions as: (i) the HPV
vaccination efficacy will be improved when applied after HPV infections are (progressively)
removed by treatment of the TZ (enrolment, 12 months, both) as the vaccine will confer
protection from new infections to new TZ growing cells; and (ii) the reduction of new HPV
infections may allow extension of HPV-triage-treat intervals, contributing to feasible
scale-up of comprehensive cervical cancer preventive care to WLWH attending ARV clinics. The
H2VICTORY specific aims are:
1. To assess the readiness ARV clinics in sub-Saharan African countries to inform
contextually relevant strategies to de-implement current interventions (i.e. Pap, VIA)
and implement and integrate the dual-intervention of HPV vaccination and HPV-based
cervical screening and treatment.
2. To study the implementation of the dual-intervention into ARV clinics in sub-Saharan
African countries while evaluating its effectiveness (HPV vaccination & cervical
screening vs cervical screening alone) in reducing HPV infections (and therefore, the
risk of cervical precancer and cancer) among WLWH aged 25-35 years.
3. To assess the integration of the dual intervention in HIV clinical services and identify
facilitators and barriers for the sustainability of proven effective interventions
(dual-intervention, HPV cervical screening) in SSA.
H2VICTORY will include WLWH aged 25-35 years attending ARV clinics to complete HPV
vaccination schemes (0-2-6-month) and to be screened with HPV testing. Participants will be
evenly allocated (1:1:1) to receive HPV vaccine (3-doses or 1-dose) or placebo. WLWH in a
single-dose HPV vaccination scheme will receive placebo at months 2 and 6. Follow-up visits
would be scheduled at i) 2 and 6 months to complete vaccination schemes, ii) 12 months 12
(only HPV positives at screening) to complete HPV-based cervical screening according to WHO
guidelines, and iii) at 24 months (all participants) to measure efficacy outcomes. Ablative
treatment would be offered to those who test positive on HPV at entry and/or at 12 months
according to WHO cervical cancer screening and treatment guidelines to progressively remove
HPV infections present at baseline. Ablative treatment will be thermal ablation (TA) or
cryotherapy (whichever is available) for eligible women (i.e., visualization of the
transformation zone and no suspicion of cervical cancer). Women not eligible for
TA/cryotherapy would be referred to colposcopy to assess the type of treatment (e.g., LLETZ).
Cervical samples for HPV testing and genotyping will be collected at entry, 12 months (for
HPV positives at entry), and 24 months (for everyone), and blood samples for neutralizing HPV
antibodies detection will be collected at entry and 24 months (for everyone). The study will
initially start in four study centers in South Africa (Cape Town and Durban), Kenya
(Nairobi), and Eswatini (Mbabane) where at least 500 participants will be included in each
center. HPV vaccine available in school-based programs in each country will be used (i.e.,
bivalent in South Africa, quadrivalent in Kenya and Eswatini). Hepatitis A (HAV) vaccine will
be administrated as a placebo. An experienced pharmacist will be in charge of preparing jabs
according to randomization. Central computed randomization will be done. An experienced
pharmacist will prepare identical appearance jabs with HPV vaccine or HAV vaccine according
to assignation. Allocation will be blinded for participants, care providers, statisticians,
and any other staff members. Permuted blocks size 3, and 6 will be used. Additional study
centers and collaborators will be involved to extend the study to other countries and
settings in order to reach the sample size.
