Early virological suppression with three-class antiretroviral therapy in HIV-infected African infants
A Prendergast, W Mphatswe, G Tudor-Williams… - Aids, 2008 - journals.lww.com
A Prendergast, W Mphatswe, G Tudor-Williams, M Rakgotho, V Pillay, C Thobakgale…
Aids, 2008•journals.lww.comObjectives: Infants infected with HIV-1 perinatally despite single-dose nevirapine progress
rapidly. Data on treatment outcome in sub-Saharan African infants exposed to single-dose
nevirapine are urgently required. This feasibility study addresses efficacy of infant
antiretroviral therapy in this setting. Methods: HIV-infected infants in Durban, South Africa,
received randomized immediate or deferred (when CD4 cell count reached< 20%) four-drug
antiretroviral therapy (zidovudine/lamivudine/nelfinavir/nevirapine). Genotyping for non …
rapidly. Data on treatment outcome in sub-Saharan African infants exposed to single-dose
nevirapine are urgently required. This feasibility study addresses efficacy of infant
antiretroviral therapy in this setting. Methods: HIV-infected infants in Durban, South Africa,
received randomized immediate or deferred (when CD4 cell count reached< 20%) four-drug
antiretroviral therapy (zidovudine/lamivudine/nelfinavir/nevirapine). Genotyping for non …
Abstract
Objectives:
Infants infected with HIV-1 perinatally despite single-dose nevirapine progress rapidly. Data on treatment outcome in sub-Saharan African infants exposed to single-dose nevirapine are urgently required. This feasibility study addresses efficacy of infant antiretroviral therapy in this setting.
Methods:
HIV-infected infants in Durban, South Africa, received randomized immediate or deferred (when CD4 cell count reached< 20%) four-drug antiretroviral therapy (zidovudine/lamivudine/nelfinavir/nevirapine). Genotyping for non-nucleoside reverse transcriptase inhibitor (NNRTI) resistance was undertaken pre-antiretroviral therapy. Monthly follow-up to 1-year post-antiretroviral therapy included viral load, CD4 cell count and verbal/measured adherence monitoring.
Results:
All 63 infants were exposed to single-dose nevirapine. Twenty-one out of 51 (39%) infants with baseline genotyping results had NNRTI resistance (most frequently Y181C; 20%). Forty-three infants were randomized to immediate antiretroviral therapy (ART): three withdrew pre-antiretroviral therapy; 36 out of 40 completed 1-year of ART. Twenty infants received deferred ART: 17 reached CD4 cell counts less than 20%(median d99) and 13 out of 17 started antiretroviral therapy in year 1. Verbal and measured adherence was 99% and 95%, respectively. One-year post-ART, 49 out of 49 (100%) infants had a viral load less than 400 copies/ml; 46 out of 49 (94%) had viral load less than 50 copies/ml. Ten infants (20%) required second-line ART due to virological failure or tuberculosis treatment, therefore 39 out of 49 (80%) achieved viral load less than 400 copies/ml by intention-to-treat. Time to viral load less than 50 copies/ml correlated with maternal CD4 cell count (r=− 0.42; P= 0.005) and infant pre-ART viral load (r= 0.64; P< 0.001). NNRTI mutations had no significant effect on virological suppression. Infants starting immediate compared with deferred ART had fewer illness episodes (P= 0.003), but no significant difference in virological suppression.
Conclusion:
Excellent adherence and virological suppression are achievable in infants, despite high-frequency NNRTI mutations and rapid disease progression. Infants remain relatively neglected in roll-out programmes and ART provision must be expanded.
Lippincott Williams & Wilkins