Scientific Publication

Strategies for Nevirapine Initiation in HIV-Infected Children Taking Pediatric Fixed-Dose Combination “Baby Pills” in Zambia: A Randomized Controlled Trial

author(s) Cook, A.. - Walker, A.S.. - Kityo, C.. - Gibb, D.M.. - Mulenga, V.. - Chintu, C.. - Kabamba, D.. - Kankasa, C.. - Ferrier, A.. - Burger, D.. - Thomason, M.. - Chijoka, C.. - Kalengo, C.
from UK Foreign, Commonwealth & Development Office (FCDO)
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  • Eastern Africa
  • Sub-Saharan Africa
  • Africa
  • World
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Mulenga, V.; Cook, A.; Walker, A.S.; Kabamba, D.; Chijoka, C.; Ferrier, A.; Kalengo, C.; Kityo, C.; Kankasa, C.; Burger, D.; Thomason, M.; Chintu, C.; Gibb, D.M. Strategies for Nevirapine Initiation in HIV& ;Infected Children Taking Pediatric Fixed& ;Dose Combination & 8220;Baby Pills& 8221; in Zambia: A Randomized Controlled Trial. Clinical Infectious Diseases (2010) 51 (9) 1081-1089. (DOI: 10.1086/656628)

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Abstract

Background. Fixed-dose combination scored dispersible stavudine, lamivudine, and nevirapine minitablets (Triomune Baby and Junior; Cipla Ltd) are simpler and cheaper than liquid formulations and have correct dose ratios for human immunodeficiency virus-infected children. However, they cannot be used for dose escalation (DE) of nevirapine. Methods. Children were randomized to initiate antiretroviral therapy with full-dose (FD) nevirapine (Triomune Baby or Junior in the morning and evening) versus DE (half-dose nevirapine for 14 days (Triomune in the morning and stavudine-lamivudine (Lamivir-S) in the evening), then FD), in accordance with World Health Organization weight-band dosing tables. The primary end point was nevirapine-related clinical or laboratory grade 3 or 4 adverse events (AEs). Results. In total, 211 children (median (interquartile range (IQR)) age, 5 (2–9) years; median (IQR) CD4 cell percentage, 13% (8%-18%)) were enrolled and followed up for a median (IQR) of 92 (68–116) weeks. There were 31 grade 3 or 4 AEs that were definitely/probably or uncertainly related to nevirapine in the FD group (18.0 per 100 child-years), compared with 29 in the DE group (16.5 per 100 child-years) (incidence rate ratio, 1.09; 95% confidence interval, 0.63–1.87; P = .74). All were asymptomatic; 11 versus 3 were single grade 3 or 4 elevations in alanine aminotransferase (ALT) or aspartate aminotransferase (AST) levels, all of which resolved without a change in nevirapine dose or interruption. Thirteen (12%) FD versus 2 (2%) DE children had grade 1 (2 in FD) or grade 2 (11 in FD and 2 in DE) rashes. Three (2 in FD and 1 in DE) substituted efavirenz, 3 (FD) continued FD nevirapine, and 9 (8 in FD and 1 in DE) temporarily interrupted nevirapine, followed by successful DE. Predictors of nevirapine rash were older age (P = .003) and higher CD4 cell count for age (P = .03). Twenty-two children died (12 in FD and 10 in DE), 1 FD and 5 DE children at !4 weeks; none were considered to be drug related by independent review. Conclusions. Rash was more frequent with FD nevirapine, but 88% had no clinical toxicity; elevated AST or ALT levels were transient and resolved spontaneously, suggesting that routine laboratory monitoring has limited value. Dual pediatric stavudine-lamivudine minitablets are preferred for safe and simple DE; if unavailable, initiating FD Triomune requires timely review for rash, which could be managed by temporary reduction to half-dose Triomune or efavirenz substitution

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