Clinical Trials/NCT02369406

NCT02369406

Active, not recruiting

Phase 2

BHP Early Infant Treatment Study: A Clinical Treatment Trial of HIV+ Infants in Botswana

Harvard School of Public Health (HSPH)1 site in 1 country67 target enrollmentMay 4, 2015

ConditionsHIV Pediatric AIDS

InterventionsNevirapine Kaletra Lamivudine Zidovudine

DrugsNevirapine Kaletra Lamivudine Zidovudine

Overview

Phase: Phase 2
Intervention: Nevirapine
Conditions: HIV
Sponsor: Harvard School of Public Health (HSPH)
Enrollment: 67
Locations: 1
Primary Endpoint: To determine the proportion of infants who have treatment-limiting adverse events within the first 14 days of treatment
Status: Active, not recruiting
Last Updated: 2 months ago

Overview Investigators Eligibility Criteria Arms & Interventions Outcomes Sites Similar Trials

Overview

Brief Summary

The overall objective of this study is to determine whether very early antiretroviral treatment (ART) initiation in HIV-infected infants limits the seeding of viral reservoirs and maintains immune responses, potentially allowing future periods off ART.

Detailed Description

HIV-1 infection during adulthood leads to a stable, long-lasting viral reservoir in CD4 T cells that persists despite suppressive antiretroviral therapy (ART), and is responsible for rapid viral rebound once treatment is stopped in most cases. In neonates, HIV-1 infection occurs at a time when the adaptive immune system is still in development, which may alter the establishment of a long-lasting viral reservoir and offer opportunities to reduce viral persistence through early antiretroviral treatment. Recently, scientific understanding of neonatal HIV infection has been challenged by the description of an infant who tested positive for HIV at birth, was treated with potent combination antiretroviral therapy (ART) within the first 30 hours of life, and achieved long-term remission of HIV infection when ART was stopped approximately 18 months later. Unfortunately, after 2 years off ART, rebound viremia occurred in this child, yet this case raises the provocative question of whether ART initiated within the first days of life for an antepartum infection, or in the first days/weeks of life for a peripartum infection, can prevent the seeding of a long-lasting reservoir of HIV infected cells in some infants (and therefore lead to long periods of HIV remission off ART).

Registry

clinicaltrials.gov

Start Date

May 4, 2015

End Date

June 30, 2029

Last Updated

2 months ago

Study Type

Interventional

Study Design

Parallel

Sex

All

Investigators

Sponsor

Harvard School of Public Health (HSPH)

Responsible Party

Principal Investigator

Roger Shapiro

Principal Investigator

Harvard School of Public Health (HSPH)

Eligibility Criteria

Inclusion Criteria

•(antepartum infection cohort):
•Mother/guardian ≥18 years of age and able to provide informed consent
•Gestational age at birth ≥35 weeks
•Birth weight ≥2000 grams
•Age is less than 7 days\*
•HIV-infection identified by testing conducted within 96 hours after birth NOTE: HIV-infection is defined as DNA PCR positive on at least one specimen, with confirmation specimen either positive or pending\*\*
•Ability to initiate ART within 7 days after birth
•Eligible for ART through the Botswana government program
•Ability to be followed in BHP clinic for up to 240 weeks from enrollment#
•Blood samples collected and submitted for real-time safety lab evaluations; results may be pending at the time of entry.

Exclusion Criteria

•(for antepartum and peripartum infection cohort):
•Hospitalization for life-threatening medical illness
•Medical condition making it unlikely that the infant will survive to 96 weeks
•If lab values are available prior to enrollment, the following Division of AIDS 2014 graded results, from samples collected within 7 days prior to entry without subsequent testing, will exclude an infant:
•Grade ≥3 ALT
•Grade ≥3 AST
•Grade ≥4 hemoglobin
•Note: Baseline lab values may not be available at the time of ART start. However, as soon as these values are available (occasionally within \<24 hours), they will be used to make rapid treatment decisions. Neonates with baseline Grade 4 hemoglobin will be called immediately to have ZDV discontinued if the value is confirmed. Neonates with baseline Grade 3 or 4 ALT or AST will be called immediately to stop either NVP or LPV/r if the value is confirmed. Neonates who remain on ART may remain on study. Neonates who discontinue all ART for pre-ART laboratory abnormalities will not be counted against total enrollments.
•Exclusion Criteria (control group):
•1\) \< 85% reported adherence to prescribed doses or interruption of ART for more than 7 consecutive days since its initiation.

Arms & Interventions

Antepartum Cohort

40 children who test HIV-positive within 96 hours after birth (antepartum HIV infection) and are able to initiate ART \< 7 days after birth. This cohort will include at least 15 children who start ART \< 3 days after birth. All infants in the antepartum cohort will initiate ART with Nevirapine, Zidovudine, Lamivudine, and later switch to Kaletra, Zidovudine, Lamivudine.

Intervention: Nevirapine

Antepartum Cohort

Intervention: Kaletra

Antepartum Cohort

Intervention: Lamivudine

Antepartum Cohort

Intervention: Zidovudine

Peripartum Cohort

10 children who test HIV-negative within 96 hours after birth but test HIV-positive \<57 days after birth (peripartum HIV infection) and who are able to initiate ART \<57 days after birth. This cohort will include at least 10 children who start ART \< 21 days after birth. The majority of infants in the peripartum cohort will be able to start Kaletra, Zidovudine, Lamivudine as their first regimen, but a minority may start Nevirapine, Zidovudine, Lamivudine and then switch to Kaletra, Zidovudine, Lamivudine.

Intervention: Nevirapine

Peripartum Cohort

Intervention: Kaletra

Peripartum Cohort

Intervention: Lamivudine

Peripartum Cohort

Intervention: Zidovudine

Control Cohort

25 HIV-infected children who initiated ART at later age ranges (30-365 days for antepartum infection, 57-365 days for peripartum infection or for those with unknown timing of infection) will be enrolled for a single visit that will occur between 24 and 36 months of age. These children will serve as a control group for virologic and immunologic comparisons with children in the prospective cohorts.

Outcomes

Primary Outcomes

To determine the proportion of infants who have treatment-limiting adverse events within the first 14 days of treatment

Time Frame: 14 days

To determine the proportion of infants who fail to achieve at least a 1.5 log10 copies/mL reduction in HIV-1 RNA by the 14th day of treatment

Time Frame: 14 days

To determine the proportion of infants in the antepartum cohort with trough drug concentrations below defined therapeutic ranges at 7 and 14 days of treatment (trough concentrations will be evaluated for NVP, ZDV, 3TC)

Time Frame: 14 days

To evaluate virologic and immunologic outcomes of very early ART in infancy

Time Frame: 84-96 weeks

Virologic outcomes after early ART: We will evaluate how the timing of HIV infection and the timing of ART initiation affect the size and composition of the viral reservoir over time. Immunologic outcomes after early ART: We will evaluate how immune activation and immune activity against HIV-1 contribute to the size and composition of the HIV-1 reservoir over time in infants treated early with suppressive ART. Control Group Comparisons. We will evaluate virologic and immunologic outcomes at a single time point in children for whom ART initiation was later than in the prospective cohorts, and compared with immunologic testing of stored specimens from HIV exposed uninfected and HIV unexposed children.

Secondary Outcomes

Number of participants with HIV-1 RNA levels <40 copies/mL(up to 576 weeks)
Number of participants with reservoir HIV-1 DNA (in copies/million peripheral blood mononuclear cells, PBMCs) below the level of detection for total virus(up to 576 weeks)
Median CD4 cell count (cells/mm3) and 95% confidence intervals among participants(up to 576 weeks)