HIV Infections Clinical Trial
Official title:
Phase II, Parallel, Randomized, Clinical Trials Comparing the Responses to Initiation of NNRTI-Based Versus PI-Based Antiretroviral Therapy in HIV Infected Infants Who Have and Have Not Previously Received Single Dose Nevirapine for Prevention of Mother-to-Child HIV Transmission
A single dose of nevirapine (SD NVP) given to an HIV infected pregnant woman followed by a
single dose to her infant has been shown to be an effective way of reducing the risk of
mother-to-child transmission (MTCT) of HIV. The purpose of this study was to compare the
effectiveness of a non-nucleoside reverse transcriptase inhibitor (NNRTI)-based
antiretroviral regimen versus a protease inhibitor (PI)-based regimen in HIV infected
infants who had or had not been exposed to SD NVP for prevention of MTCT.
>>
>> A five year follow up has been added to the study.
Single dose nevirapine (SD NVP) has greatly reduced the rate of mother-to-child transmission
(MTCT) of HIV. Non-nucleoside reverse transcriptase inhibitor (NNRTI)-based regimens are
recommended for use by the World Health Organization (WHO) in resource-limited settings.
However, research suggests that mothers and infants exposed to SD NVP experience higher
virologic failure rates when treated with NNRTI-based regimens than their unexposed
counterparts. Data show that the use of SD NVP is associated with NNRTI resistance in HIV
infected women and infants. The purpose of this trial was to compare and evaluate virologic
responses to an NNRTI-based regimen versus a protease-inhibitor (PI)-based regimen in HIV
infected infants who had or had not been exposed to SD NVP intrapartum and after birth.
>>
>> Participants were enrolled into one of two Cohorts with proposed enrollment into each
Cohort of 288 participants. Cohort I participants must have received SD NVP for prevention
of MTCT. Cohort II participants and their mothers must not have previously received NVP or
any other NNRTIs. Participants in both Cohorts were randomly assigned to receive either an
NNRTI (Coh I:NVP and Coh II: NVP) or PI (Coh I: LPV/r and Coh II: LPV/r) -based regimen. The
NNRTI-based regimen included NVP, zidovudine (ZDV) and lamivudine (3TC). The PI-based
regimen included lopinavir/ritonavir (LPV/r), ZDV and 3TC. If participants experienced
adverse reactions to ZDV, stavudine (d4T) could be substituted. Randomization was stratified
by age (6-<12 months vs. >=12 months, with the 2-<6 month stratum added in protocol version
4.0 when the lower age limit was decreased from 6 months to 2 months).
>>
>> Study visits were scheduled at entry, weeks 2, 4, 8, 12, 16, 24 and then every 24 weeks.
A physical exam, blood collection, and assessments of HIV-related symptoms occurred at all
visits.
>>
>> Based on a Data Safety and Monitoring Committee (DSMB) review of study data on April 20
2009, enrollment to Cohort I was closed and interim results released. Data from this and
another similar study (AIDS Clinical Trials Group (ACTG) A5208) conducted in mothers, showed
that the PI-based regimen was more effective than the NNRTI-based regimen in infants who had
received SD NVP for prevention of MTCT. Cohort II was allowed to remain open for enrollment
and the lower age limit for enrollment reduced from 6 months to 2 months.
>>
>> In June 2010, follow-up for all subjects was extended from the original 24 weeks beyond
enrollment of the last subject to 48 weeks. On October 27 2010, the DSMB conducted a final
review of Cohort II data, and recommended results be unblinded and released. As found in
Cohort I, the PI-based regimen was more effective than the NNRTI-based regimen in infants
who had not been previously exposed to SD NVP for PMTCT. Primary and secondary outcome
results for Cohort I include all follow-up until April 20, 2009 and for Cohort II, all
follow-up until October 27, 2010. Adverse event summaries use all follow-up while on the
randomized study treatment regimen in both Cohorts until October 27, 2010.
>>
>> Version 5.0 of the protocol (March 21, 2011) extends follow-up on all subjects for an
additional 5 years to March 2016. The purpose of the extension is to collect long term
safety and virologic efficacy data in this study population and to pilot administration of a
series of neuropsychological tests. During the extension, participants will not receive any
medications through the study, but instead through their local clinics. Clinic visits will
take place every 3 months.
>>
>>
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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