HIV Clinical Trial
Official title:
A Randomized Clinical Trial on the Effects of Progestin-based Contraception in the Genital Tract of HIV-infected and Uninfected Women
The purpose of this study is to determine the acceptability of randomization to contraceptive options and estimate the effect of progestin contraception on HIV genital shedding and inflammatory/immune perturbations in women who may or may not be on antiretroviral therapy, as well as in HIV-uninfected women controls. It is hypothesized that progestin-containing contraception will lead to inflammatory changes that may affect the local immune activity, influencing HIV acquisition or transmissibility risk.
Hormonal contraception is a central component in the prevention of unintended pregnancy;
however there are concerns that certain methods may increase the risk of heterosexual HIV
acquisition and transmission. Some studies, but not others, have suggested a link between
hormonal contraceptive use and enhanced HIV-susceptibility, more rapid HIV disease
progression, and increased transmissibility to partners. Hormonal contraception modifies the
genital mucosa in several ways, and the interactions of the endocrine and immune system are
complex but incompletely understood. In some cross-sectional studies, hormonal contraceptives
appear to be associated with increased shedding of HIV DNA, but not RNA, in the genital
tract, and the significance of these findings for HIV transmissibility are unclear. Very few
studies have examined genital HIV shedding prospectively before and after initiation of
contraception. The effects of hormonal contraception in the setting of antiretroviral therapy
(ART) are also unknown.
Hormonal contraception, particularly injectable DMPA, is widely used in many parts of the
world, including settings with high HIV prevalence. It is important that the effects of
hormonal contraception on HIV acquisition and HIV shedding and subsequent transmissibility be
determined. The effect of progestin contraceptive implants, such as the levonorgestrel rod
implant (LNG implant), on HIV shedding is unknown, and it will be of interest to evaluate it
compared with the injectable progestin (DMPA), given their different kinetics of hormone
release, differences in progestin type, and the high efficacy of both methods.
We propose a pilot study among 100 HIV-infected women and 30 uninfected women in Lilongwe,
Malawi randomized to either DMPA or LNG implant to: 1) assess the effect and compare the
impact of type of progestin-containing contraception (injectable versus implant) on HIV viral
shedding in the genital tract of HIV+ women, 2) assess the effect and compare the impact of
type of progestin-containing contraception (injectable versus implant) on inflammatory/immune
markers in the genital tract of both HIV+ and HIV- women, and 3) assess the interaction of
progestin-based hormonal contraception and ART by examining: i. contraceptive efficacy
(measured by systemic hormone levels and pregnancy rate during follow-up), and ii. ART
efficacy (by drug concentrations in blood and genital tract and HIV viral load response in
the plasma in women on ART).
An overall study aim is to determine the feasibility and need for a larger study of
determinants of HIV transmissibility and acquisition in this population.
The study would take place at Bwaila Maternity Hospital, which was the site of the
CDC-sponsored Breastfeeding, Antiretrovirals, and Nutrition (BAN) clinical trial, a partner
project with this study. Women attending the clinics at Bwaila (a large proportion of whom
participated in the BAN study) who desire to start hormonal contraception will be informed of
the new study and counseled on the progestin-based contraceptives that are available within
the study. BAN women will be specifically targeted for recruitment through radio messages.
Eligible women who provide informed consent and agree to randomization to either DMPA or the
LNG implant will be enrolled. HIV-infected women may be on ART or they may be pre-ART.
To address the primary outcomes of HIV shedding and mucosal immune activation, we will
quantify genital tract HIV RNA and inflammatory/immune markers at two time points before and
four time points after randomization of the 100 HIV-infected and 30 HIV-uninfected women to
DMPA or LNG-implant. The two time points prior to randomization will occur within the prior
menstrual cycle, so that one visit occurs in the follicular phase and the other occurs in the
luteal phase of the cycle. Assessments after initiation of contraception will occur on days
3, 30, 90, and 6 months. Antiretroviral levels in the blood and genital tract will also be
assessed at these time points.
Based on recent evidence suggesting that the LNG implant may have decreased contraceptive
efficacy when used in combination with the antiretroviral efavirenz, study follow-up will be
extended to include visits at about 9, 12, 15, 18, 21, 24, 27, 30, and 33 months after
initiation of contraception for a total of 6 additional visits per participant. Not all
participants will start the study extension at the same time point, so the 6 additional
visits can span from about 9 months to 24 months after contraceptive initiation to about 18
months to 33 months after contraceptive initiation. Assessments at these visits will address
the outcomes of contraceptive and ART efficacy and HIV shedding.
To analyze the effects of progestin contraception on HIV shedding, as well as the effect of
each contraceptive type, HIV-infected women on progestin-based contraception will be compared
within each study arm (before and after initiation of contraception), as well as between the
two contraceptive arms. Antiretroviral use will be evaluated for an independent effect on HIV
shedding and also to determine if it modifies the effect of menstrual cycle or progestin
contraception on HIV shedding. To analyze the effects of progestin contraception on genital
inflammatory/immune markers, both HIV-infected and HIV-uninfected women on progestin-based
contraception will be compared separately and combined, with HIV status treated as a
potential effect modifier, within each study arm (before and after initiation of
contraception), as well as between the two contraceptive arms. This study will provide
information on acceptability of randomization to contraceptive options, overall study
retention, and estimates of the effect of progestin contraception on HIV genital shedding and
inflammatory/immune perturbations in women who may or may not be on antiretroviral therapy,
as well as in HIV-uninfected women controls. This information will be instrumental in
determining the need for and feasibility of a larger study to address these outcomes.
;
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Recruiting |
NCT06162897 -
Case Management Dyad
|
N/A | |
| Completed |
NCT03999411 -
Smartphone Intervention for Smoking Cessation and Improving Adherence to Treatment Among HIV Patients
|
Phase 4 | |
| Completed |
NCT02528773 -
Efficacy of ART to Interrupt HIV Transmission Networks
|
||
| Active, not recruiting |
NCT05454839 -
Preferences for Services in a Patient's First Six Months on Antiretroviral Therapy for HIV in South Africa
|
||
| Recruiting |
NCT05322629 -
Stepped Care to Optimize PrEP Effectiveness in Pregnant and Postpartum Women
|
N/A | |
| Completed |
NCT02579135 -
Reducing HIV Risk Among Adolescents: Evaluating Project HEART
|
N/A | |
| Active, not recruiting |
NCT01790373 -
Evaluating a Youth-Focused Economic Empowerment Approach to HIV Treatment Adherence
|
N/A | |
| Not yet recruiting |
NCT06044792 -
The Influence of Primary HIV-1 Drug Resistance Mutations on Immune Reconstruction in PLWH
|
||
| Completed |
NCT04039217 -
Antiretroviral Therapy (ART) Persistence in Different Body Compartments in HIV Negative MSM
|
Phase 4 | |
| Active, not recruiting |
NCT04519970 -
Clinical Opportunities and Management to Exploit Biktarvy as Asynchronous Connection Key (COMEBACK)
|
N/A | |
| Completed |
NCT04124536 -
Combination Partner HIV Testing Strategies for HIV-positive and HIV-negative Pregnant Women
|
N/A | |
| Recruiting |
NCT05599581 -
Tu'Washindi RCT: Adolescent Girls in Kenya Taking Control of Their Health
|
N/A | |
| Active, not recruiting |
NCT04588883 -
Strengthening Families Living With HIV in Kenya
|
N/A | |
| Completed |
NCT02758093 -
Speed of Processing Training in Adults With HIV
|
N/A | |
| Completed |
NCT02500446 -
Dolutegravir Impact on Residual Replication
|
Phase 4 | |
| Completed |
NCT03805451 -
Life Steps for PrEP for Youth
|
N/A | |
| Active, not recruiting |
NCT03902431 -
Translating the ABCS Into HIV Care
|
N/A | |
| Completed |
NCT00729391 -
Women-Focused HIV Prevention in the Western Cape
|
Phase 2/Phase 3 | |
| Recruiting |
NCT05736588 -
Elimisha HPV (Human Papillomavirus)
|
N/A | |
| Recruiting |
NCT03589040 -
Darunavir and Rilpivirine Interactions With Etonogestrel Contraceptive Implant
|
Phase 2 |