We also addressed the safety and tolerability of etravirine-based

We also addressed the safety and tolerability of etravirine-based therapy in these patients. We performed a multicentre retrospective study of 23 vertically infected children (5–12 years old) and adolescents (13–18 years old) receiving highly active antiretroviral Proteases inhibitor therapy who were enrolled in the Spanish HIV Paediatric Cohort. All except one NNRTI-naïve adolescent had documented genotypic evidence of resistance to NNRTIs and had begun etravirine-based therapy under

the Spanish compassionate use programme. Weight-adjusted doses of 5.2 mg/kg twice daily [7] following a meal and 200 mg twice daily were administered to children and adolescents, respectively. Backbone regimens including nucleoside reverse transcriptase inhibitors (NRTIs) and a boosted protease inhibitor, with or without newer agents (raltegravir, maraviroc and/or enfuvirtide), were prescribed. When available, plasma samples were analysed using Trofile® (Monogram Biosciences, San Francisco, CA, USA). Adherence to antiretrovirals (expressed as a percentage) was evaluated by paediatricians who assessed the dose taken by interviewing parents/guardians. Genotypic susceptibility was determined Talazoparib using the Stanford Resistance Database [8] based on a scoring system: 0–9, total

response to antiretrovirals; 10–14, potential low-level drug resistance; 15–29, low-level drug resistance; 30–59, degree of drug resistance greater than low-level resistance but lower than high-level resistance; and ≥60, little or no virological response to treatment. Visits were scheduled every 3 months according to international guidelines. Demographic data and clinical and laboratory parameters were recorded longitudinally. The Ethics Committees of the participating hospitals approved Adenosine the study and parents and guardians gave their informed consent. Several biological samples were provided by the Spanish HIV BioBank of the Spanish AIDS Research Network [9]. Values were recorded as absolute numbers/percentages, and medians were calculated with

their interquartile ranges (IQRs). The statistical analysis was performed using spss (version 15) (SPSS, Chicago, IL, USA). Between 1 September 2007 and 28 February 2010, we enrolled 23 vertically infected patients born between 1989 and 2002 and treated at six Spanish hospitals (see Appendix). All patients fulfilled the inclusion criteria. Five were children (22%) and 18 (78%) were adolescents. Their median age was 14.2 years (IQR 12.5–15.8 years). Most patients were Caucasian (n=19; 83%) with the HIV B subtype (n=16; 70%) (Table 1). The patient from sub-Saharan Africa harboured a non-B subtype. Only one patient was vertically coinfected with the hepatitis C virus. The baseline median plasma HIV-1 RNA level was 29 000 (4.5 log10) HIV-1 RNA copies/mL, with a range from 4300 to 83 000 copies/mL. The median CD4 T-cell count was 445 cells/μL (range 221–655 cells/μL) and the median CD4 percentage was 19.6% (IQR 13.0-31.

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