FEM-PrEP (Truvada®): Study to Assess the Role of Truvada® in Preventing HIV Acquisition in Women

Phase 3

Completed

Conditions: HIV Infections

Interventions: Other: Placebo
Drug: Truvada

Registration Number: NCT00625404

Lead Sponsor: FHI 360

Brief Summary: This Phase III, double-blind, randomized, placebo-controlled trial enrolled HIV-negative women from 4 sites in 3 countries (Kenya, Tanzania, South Africa). The study's purpose was to investigate the safety and effectiveness of a once-daily Truvada® pill (compared with placebo) in preventing HIV among HIV-uninfected women at risk of becoming infected through sexual intercourse.

The study population included HIV-antibody-negative women between the ages of 18-35 who were at risk of HIV acquisition through sexual intercourse. Each participant was randomized to take either a daily single oral tablet of Truvada®, which is a fixed-dose combination of emtricitabine (FTC; 200 mg) and tenofovir disoproxil fumarate (TDF; 300 mg), or an identical placebo.

After enrollment, each participant was followed every four weeks. All participants were followed for an additional eight weeks after study drug was stopped. Incidence rates of HIV infection were compared between the two groups (active drug and placebo) using the intent-to-treat principle.

Detailed Description: This Phase III, double-blind, randomized, placebo-controlled trial enrolled HIV-negative women from 4 sites in 3 countries (Kenya, Tanzania, South Africa). The study's purpose was to investigate the safety and effectiveness of a once-daily Truvada® pill (compared with placebo) in preventing HIV among HIV-uninfected women at risk of becoming infected through sexual intercourse.

The study population included HIV-antibody-negative women between the ages of 18-35 who were at risk of HIV acquisition through sexual intercourse. Each participant was randomized to take either a daily single oral tablet of Truvada®, which is a fixed-dose combination of emtricitabine (FTC; 200 mg) and tenofovir disoproxil fumarate (TDF; 300 mg), or an identical placebo. All participants received risk reduction counseling and condoms. Women had to be using a study-approved effective non-barrier contraceptive method at the time of enrollment and were asked to do so for the whole period they were on study drug. They received contraceptive counseling throughout the study. Any diagnosed, treatable sexually transmitted infection was treated free of charge.

After enrollment, each participant was followed every four weeks. All participants were followed for an additional eight weeks after study drug was stopped. Participants at risk for Hepatitis B Virus (HBV) flare were followed every four weeks for 12 weeks after stopping study product. Participants who acquired HIV infection during the study stopped taking the study drug at the time of HIV diagnosis, and will be followed for 52 weeks post diagnosis and were referred for care and treatment. Participants who became pregnant stopped taking the study drug but continued follow-up visits. Incidence rates of HIV infection were compared between the two groups (active drug and placebo) using the intent-to-treat principle.

Recruitment & Eligibility

Status: COMPLETED

Sex: Female

Target Recruitment: 2120

Inclusion Criteria

Willing and able (see criterion 2) to provide written informed consent to be screened for and to participate in the trial
Able to answer a percentage of informed consent screening (75%) and enrollment (100%) comprehension quiz questions correctly
Between 18-35 years old, inclusive
At higher risk of becoming HIV infected
Have a final negative result according to the site-specific screening HIV testing algorithm and a final negative result at enrollment according to the study HIV testing algorithm
Willing to participate in all aspects of the study and to comply with study procedures, for up to 60 weeks, including:
- Be randomized
- Use study product as directed
- Adhere to follow-up schedule and willing to be contacted by site staff between study visits (by phone and/or in person)
- Use a study-approved effective non-barrier method of contraception for the duration of the study
- Take study product, as evidenced by swallowing a vitamin tablet that is similar in size to the study product at enrollment
- Provide contact information and agrees to some form of contact method throughout the study
Not intending to relocate out of the area for the duration of the study participation and does not have a job or other obligations that may require long absences from the area ( > 1 month at a time)
In general good health and have no condition (social or medical) which, in the opinion of the Site Investigator, would make study participation unsafe or complicate data interpretation
Not pregnant or breastfeeding, and does not anticipate a desire for pregnancy during the 52 weeks of on-product participation
Medically eligible at screening including:
- Adequate renal function (serum creatinine ≤ upper limit of normal (ULN) of local range and creatinine clearance ≥ 60ml/min estimated by the Cockcroft-Gault Creatinine Clearance Formula
- Adequate hepatic function (hepatic transaminases ALT and AST < 2x ULN [according to local normal ranges])
- HBsAg negative
- Serum phosphorus levels above the lower limit of the local normal range (according to local normal ranges - grade 3 & 4 hypophosphatemia will be excluded even if within normal local ranges)
Not received or receiving an experimental HIV vaccine, participating in another HIV prevention study or participating in any other clinical trial with a biomedical intervention
No clinical signs of liver disease (e.g., ascites, spider angiomata, hepatomegaly, jaundice)
No definite evidence of glycosuria or proteinuria (i.e., no repeated positive [ ≥ + 1 ] urine dipstick). If a urine dipstick is positive for either glucose and/or protein at the first test, a second urine sample will be tested.
No history of pathological bone fractures
No history of adverse reaction to latex
Not taking any of the following medications: nephrotoxic agents; aminoglycoside antibiotics (including gentamicin); intravenous (IV) amphotericin B; cidofovir; cisplatin; foscarnet; IV pentamidine; oral or IV vancomycin; oral or IV gancyclovir; other agents with significant nephrotoxic potential; drugs that slow renal excretion; probenecid; immune system modulators; systemic chemotherapeutic agents (i.e. cancer treatment medications); systemic corticosteroids; interleukin-2 (IL-2); immunomodulators; interferon (alpha, beta, or gamma); other antiretrovirals (including nucleoside analogs, non-nucleoside reverse transcriptase inhibitors, protease inhibitors or investigational antiretroviral agents)

Exclusion Criteria

Not provided

Study & Design

Study Type: INTERVENTIONAL

Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Placebo Arm	Placebo	Daily single oral tablet of Placebo. Tablets are identical to Truvada tablets in taste and appearance; however, they contain no active ingredients.
Truvada Arm	Truvada	Daily single oral tablet of Truvada (TDF/FTC), a fixed-dose combination of emtricitabine (FTC; 200 mg) and tenofovir disoproxil fumarate (TDF; 300 mg).

Primary Outcome Measures

Name	Time	Method
HIV Infection	Cumulative HIV infection between enrollment and 52 weeks	HIV Seroconversion, with time to infection refined based on PCR results obtained from stored specimens.
Confirmed Grade 2 or Higher Serum Creatinine Toxicity	cumulative toxicity through 52 weeks of product use and 4 weeks post product	Repeat specimens were collected to confirm chemistry toxicities. Grade 2 or higher serum creatinine toxicity was defined as ≥1.4 times the upper limit of normal
Frequency of Adverse Events (AEs) During and Within 4 Weeks After Study Product Administration	10-26 months per site	The total number of adverse events in the placebo and Truvada arms during and within 4 weeks after study product administration.
Confirmed Grade 3 or Higher AST Elevation	Through 52 weeks on product and 4 weeks post-product	Grade 3 or higher AST elevation was defined as ≥ 2.6 times the upper limit of normal
Confirmed Grade 3 or Higher Reduction in Phosphorus	Through 52 weeks on product and 4 weeks post-product	Repeat specimens were collected to confirm chemistry toxicities. Grade 3 phosphorus reduction was defined as ≤2.4mg/dL
Confirmed Grade 3 or Higher ALT Elevation	Through 52 weeks on product and 4 weeks post-product	Grade 3 or higher ALT elevation was defined as ≥ 2.6 times the upper limit of normal

Secondary Outcome Measures

Name	Time	Method
CD4+ T-cell Count	Up to 16 weeks	CD4+ T-cell Count at the Time of HIV Seroconversion through 16 weeks
FTC and/or Tenofovir Resistance	up to 52 weeks	Genotypic resistance to FTC and/or tenofovir at the time of HIV diagnosis and 4 weeks later. If resistance was present, testing was repeated at weeks 12, 24, 36 and 52 as necessary (resistance testing will stop if no resistance is detected). participants were classified as having resistance if they had one or more visits in which resistance was detected, even if the resistance became undetectable over time.
Pregnancy Complications	up to 60 weeks	Reported complications during pregnancy, including spontaneous abortion, vaginal or uterine bleeding, emergency c-section and other complications
Pill Counts and Participant Report of Adherence to Once-daily Pill Taking	Up to 52 weeks	Pill counts and participant report of adherence to once-daily pill taking reported as mean days study product could have been used according to pill counts
Plasma HIV RNA Level (HIV-1 Viral Load)	up to 16 weeks	Viral load at the time of HIV detection, HIV conversion and through 16 weeks
Participant Report of Change in Number of Sexual Partners	Up to 52 weeks	Difference in mean number of reported sexual partners between final study visit and enrollment visit

Trial Locations

Locations (4): Josha Research Center
🇿🇦
Bloemfontein, South Africa
Setshaba Research Centre
🇿🇦
Pretoria, Gauteng, South Africa
Arusha Clinic, Levolosi Health Center
🇹🇿
Arusha, Tanzania
Bondo Clinic, Bondo District Hospital
🇰🇪
Bondo, Nyanza, Kenya