The randomized drug was substituted in 21 participants (7%) recei

The randomized drug was substituted in 21 participants (7%) receiving abacavir vs. 34 (11%) receiving nevirapine (P=0.09). At 48 weeks, 62% of participants receiving abacavir vs. 77% of those receiving nevirapine had viral loads <50 copies/mL (P<0.001), and mean SAHA HDAC datasheet CD4 count increases from baseline were

+147 vs. +173 cells/μL, respectively (P=0.006). Nine participants (3%) receiving abacavir vs. 16 (5%) receiving nevirapine died [hazard ratio (HR) 0.55; 95% confidence interval (CI) 0.24–1.25; P=0.15]; 20 receiving abacavir vs. 32 receiving nevirapine developed new or recurrent WHO 4 events or died (HR=0.60; 95% CI 0.34–1.05; P=0.07) and 48 receiving abacavir vs. 68 receiving nevirapine developed new or recurrent WHO 3 or 4 events or died (HR=0.67; 95% CI 0.46–0.96; P=0.03). Seventy-one participants (24%) receiving Belnacasan molecular weight abacavir experienced 91 grade 4 adverse events compared with 130 events in 109 participants (36%) on nevirapine (P<0.001). Conclusions The clear virological/immunological superiority of nevirapine over abacavir was not reflected in clinical outcomes

over 48 weeks. The inability of CD4 cell count/viral load to predict initial clinical treatment efficacy is unexplained and requires further evaluation. The World Health Organization (WHO) currently recommends two nucleoside reverse transcriptase inhibitors (NRTIs) plus a nonnucleoside reverse transcriptase inhibitor (NNRTI) as first-line antiretroviral therapy (ART) [1]. In view of recognized limitations, triple NRTI regimens using a standard NRTI backbone with either abacavir or tenofovir disoproxil fumarate (DF) are recommended by WHO as a ‘simplification strategy’ for NNRTI toxicity Amisulpride and drug–drug interactions in first-line ART [2]. Abacavir/zidovudine/lamivudine in particular has the advantage of being available as a fixed-dose formulation. However, few data on triple NRTI regimens have been published for low-income settings, and there are concerns about lower virological potency [3]. Cost remains an issue and many countries reserve abacavir and/or tenofovir DF for second-line ART. In Uganda, the randomized Nevirapine

OR Abacavir (NORA) substudy of the DART trial was designed in 2002 to compare the toxicities of nevirapine and abacavir (both with zidovudine/lamivudine) to 24 weeks. This primary analysis demonstrated a trend towards a lower rate of serious adverse reactions [the primary endpoint; hazard ratio (HR) 0.42; 95% confidence interval (CI) 0.16–1.09; P=0.06] with abacavir and a significantly lower discontinuation rate of abacavir vs. nevirapine to 24 weeks [4]. Because the clinical, immunological and virological efficacies of nevirapine and abacavir have not been compared in Africa, here we report exploratory analyses of 48-week clinical, immunological and virological efficacy data from NORA, which were collected as part of the ongoing DART trial; drug resistance data are published elsewhere [5].

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