Low-Frequency Nevirapine (NVP)–Resistant HIV-1 Variants Are Not Associated With Failure of Antiretroviral Therapy in Women Without Prior Exposure to Single-Dose NVP

Valerie F. Boltz,Yajing Bao,Shahin Lockman,Elias K. Halvas,Mary Kearney,James McIntyre,Robert T. Schooley,Michael Hughes,John M. Coffin,John W. Mellors,Arrow trial team,Beth Zwickl,CissyKityo Mutuluuza,Christine Kaseba,Charles C. Maponga,Heather Watts,Daniel R. Kuritzkes,Thomas B. Campbell,Lynn Kidd-Freeman,Monica Carten,Jane Hitti,Mary Marovich,Peter Mugyenyi,Sandra Rwambuya,Ian Sanne,Beverly Putnam,Cheryl Marcus,Carolyn Wester,Robin DiFrancesco,Elias K. Halvas,Annie Beddison,Sandra Nusinoff-Lehrman,Francesca T. Aweeka,Betty J. Dong,Peter Ndhleni Ziba,Michael S. Saag,William C. Holmes,Scott M. Hammer

Low-Frequency Nevirapine (NVP)–Resistant HIV-1 Variants Are Not Associated With Failure of Antiretroviral Therapy in Women Without Prior Exposure to Single-Dose NVP

2014

Mutations in the human immunodeficiency virus type 1 (HIV-1) genome have been hypothesized to occur at all nucleotide positions, including those that confer drug resistance, as the result of high rates of HIV-1 replication, mutation, and recombination [1–3]. Consequently, after exposure to one antiretroviral drug such as nevirapine (NVP), given as a single dose to prevent mother-to-child HIV-1 transmission, drug-resistant variants can rapidly emerge [4–7]. It is well established that such drug-resistant variants, when detected by standard genotype, can compromise virologic responses to combination antiretroviral therapy (cART) [8–10]. For example, in the OCTANE/A5208 trial 1, conducted in African women with prior exposure to single-dose NVP (sdNVP) and who subsequently initiated NVP-based cART, NVP resistance detected by standard genotype at study entry was associated with virologic failure (VF) or death, and lopinavir/ritonavir (LPV/r) was superior to NVP-based cART in sdNVP-exposed women [11]. The impact of minor populations of drug-resistant variants on the response to initial cART has been more controversial, with some studies reporting their association with VF and others finding no association [12–19]. We reported that the risk of VF with NVP-based cART was significantly associated with low frequency (>1%), NVP-resistant variants in African women with prior exposure to sdNVP (OCTANE/A5208 trial 1) [20]. In women who had never been exposed to sdNVP (OCTANE/A5208 trial 2), however, NVP- or LPV/r-based cART showed equivalent virologic efficacy [21]. To investigate the different outcomes of the NVP-based cART arms of trial 1 and trial 2, we performed allele-specific polymerase chain reaction (PCR) on pre-cART samples from women without prior sdNVP exposure (trial 2), to quantify frequencies of the 3 most common NVP resistance mutations (K103N, Y181C, and G190A) and their association with VF or death.

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