Pretreatment HIV drug resistance predicts accumulation of new mutations in ART-naïve Ugandan children.

Abstract

To assess the prevalence of pretreatment drug resistance (PDR) and its association with virologic outcomes after 24weeks of antiretroviral therapy (ART), within an urban cohort of Ugandan children. Prospective observational study. Baseline and 24-week assessments of viral load (VL) and genotypic drug resistance to nucleoside reverse transcriptase inhibitors (NRTI) and non-nucleoside reverse transcriptase inhibitors (NNRTI) were performed. Ninety-nine ART-naïve children (3-12years) initiated efavirenz-based ART 2015-2016 and 18/90 (20%) had baseline NRTI/NNRTI associated drug resistance mutations (DRMs). By 24weeks, 72/93 (77%) children had VL<40copies/mL and a total of 23 children had DRMs. Children with PDR accumulated new DRMs with a mean number (SD) of 1.4 (2.35) new mutations compared to 0.26 (0.98) in 67 children with wild-type virus (P=.003). High pretreatment VL and PDR (number of baseline DRMs) predicted viremia (P=.003; P=.023) as well as acquired drug resistance (P=.02; P=.04). Pretreatment drug resistance to NNRTI/NRTI was common among ART-naïve Ugandan children and predicted viremia and new resistance mutations after only 24weeks of efavirenz-based therapy. PDR may compromise long-term ART outcomes-especially when access to resistance testing and VL monitoring is poor. The long-term importance of PDR for non-NNRTI-based regimens needs further evaluation.