Concomitant nevirapine impacts pharmacokinetic exposure to the antimalarial artemether-lumefantrine in African children

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المؤلفون: Huang, Liusheng; Carey, Vincent; Lindsey, Jane C; Marzan, Florence; Gingrich, David; Graham, Bobbie; Barlow-Mosha, Linda; Ssemambo, Phionah K; Kamthunzi, Portia; Nachman, Sharon; Parikh, Sunil; Aweeka, Francesca T; team, the IMPAACT P1079 protocol
المصدر:
PLOS ONE. 12(10)
الوصف المادي :
e0186589
الموضوع:
Medical Microbiology; Biomedical and Clinical Sciences; Clinical Sciences; Orphan Drug; Rare Diseases; HIV/AIDS; Pediatric AIDS; Sexually Transmitted Infections; Infectious Diseases; Clinical Research; Vector-Borne Diseases; Malaria; Clinical Trials and Supportive Activities; Pediatric; 6.1 Pharmaceuticals; Evaluation of treatments and therapeutic interventions; Infection; Good Health and Well Being; Africa South of the Sahara; Antimalarials; Artemether; Artemisinins; Child; Child; Preschool; Ethanolamines; Female; Fluorenes; Humans; Lumefantrine; Male; Nevirapine; IMPAACT P1079 protocol team; General Science & Technology
نوع التسجيلة:
article
الدخول الالكتروني :
https://escholarship.org/uc/item/3h6108ht
https://escholarship.org/content/qt3h6108ht/qt3h6108ht.pdf

معلومة اضافية
- بيانات النشر:
  eScholarship, University of California, 2017.
- الموضوع:
  2017
- نبذة مختصرة :
  BackgroundThe antiretroviral drug nevirapine and the antimalarial artemisinin-based combination therapy artemether-lumefantrine are commonly co-administered to treat malaria in the context of HIV. Nevirapine is a known inhibitor of cytochrome P450 3A4, which metabolizes artemether and lumefantrine. To address the concern that the antiretroviral nevirapine impacts the antimalarial artemether-lumefantrine pharmacokinetics, a prospective non-randomized controlled study in children presenting with uncomplicated malaria and HIV in sub-Saharan Africa was carried out.MethodsParticipants received artemether-lumefantrine (20/120 mg weight-based BID) for 3 days during nevirapine-based antiretroviral therapy (ART) co-administration (158-266 mg/m2 QD). HIV positive participants who were not yet on ART drugs were also enrolled as the control group. The target enrollment was children aged 3-12 years (n = 24 in each group). Intensive pharmacokinetics after the last artemether-lumefantrine dose was assessed for artemether, its active metabolite dihydroartemisinin, and lumefantrine. Pharmacokinetic parameters (area under the plasma concentration vs. time curve (AUC), maximum concentration and day 7 lumefantrine concentrations) were estimated using non-compartmental methods and compared to controls.ResultsNineteen children (16 on nevirapine and three not on ART) enrolled. Fifteen of the 16 (aged 4 to 11 years) on nevirapine-based ART were included in the pharmacokinetic analysis. Due to evolving WHO HIV treatment guidelines, insufficient children were enrolled in the control group (n = 3), so the pharmacokinetic data were compared to a historical control group of 20 HIV-uninfected children 5-12 years of age who also presented with malaria and underwent identical study procedures. Decreases of pharmacokinetic exposure [as estimated by AUC (AUC0-8hr)] were marginally significant for artemether (by -46%, p = 0.08) and dihydroartemisinin (-22%, p = 0.06) in the children on nevirapine-based ART, compared to when artemether-lumefantrine was administered alone. Similarly, peak concentration was decreased by 50% (p = 0.07) for artemether and 36% (p = 0.01) for dihydroartemisinin. In contrast, exposure to lumefantrine increased significantly in the context of nevirapine [AUC0-120hr:123% (p
- File Description:
  application/pdf
- Rights:
  public
- الرقم المعرف:
  edssch.oai:escholarship.org:ark:/13030/qt3h6108ht

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Concomitant nevirapine impacts pharmacokinetic exposure to the antimalarial artemether-lumefantrine in African children

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