TY - JOUR
T1 - The effect of dose on the antimalarial efficacy of artemether-lumefantrine
T2 - A systematic review and pooled analysis of individual patient data
AU - Worldwide Antimalarial Resistance Network (WWARN) AL Dose Impact Study Group
AU - Anstey, N. M.
AU - Price, R. N.
AU - Davis, T. M.E.
AU - Karunajeewa, H. A.
AU - Mueller, I.
AU - D'Alessandro, U.
AU - Massougbodji, A.
AU - Nikiema, F.
AU - Ouédraogo, J. B.
AU - Tinto, H.
AU - Zongo, I.
AU - Same-Ekobo, A.
AU - Koné, M.
AU - Menan, H.
AU - Yavo, W.
AU - Touré, A. O.
AU - Kofoed, P. E.
AU - Alemayehu, B. H.
AU - Jima, D.
AU - Baudin, E.
AU - Espié, E.
AU - Nabasumba, C.
AU - Pinoges, L.
AU - Schramm, B.
AU - Cot, M.
AU - Deloron, P.
AU - Faucher, J. F.
AU - Guthmann, J. P.
AU - Lell, B.
AU - Borrmann, S.
AU - Adjei, G. O.
AU - Ursing, J.
AU - Tjitra, E.
AU - Marsh, K.
AU - Peshu, J.
AU - Juma, E.
AU - Ogutu, B. R.
AU - Omar, S. A.
AU - Sawa, P.
AU - Talisuna, A. O.
AU - Khanthavong, M.
AU - Mayxay, M.
AU - Newton, P. N.
AU - Piola, P.
AU - Djimdé, A. A.
AU - Doumbo, O. K.
AU - Fofana, B.
AU - Sagara, I.
AU - Bassat, Q.
AU - González, R.
N1 - Publisher Copyright:
© 2015 Elsevier Ltd.
PY - 2015/6/1
Y1 - 2015/6/1
N2 - Background: Artemether-lumefantrine is the most widely used artemisinin-based combination therapy for malaria, although treatment failures occur in some regions. We investigated the effect of dosing strategy on efficacy in a pooled analysis from trials done in a wide range of malaria-endemic settings. Methods: We searched PubMed for clinical trials that enrolled and treated patients with artemether-lumefantrine and were published from 1960 to December, 2012. We merged individual patient data from these trials by use of standardised methods. The primary endpoint was the PCR-adjusted risk of Plasmodium falciparum recrudescence by day 28. Secondary endpoints consisted of the PCR-adjusted risk of P falciparum recurrence by day 42, PCR-unadjusted risk of P falciparum recurrence by day 42, early parasite clearance, and gametocyte carriage. Risk factors for PCR-adjusted recrudescence were identified using Cox's regression model with frailty shared across the study sites. Findings: We included 61 studies done between January, 1998, and December, 2012, and included 14 327 patients in our analyses. The PCR-adjusted therapeutic efficacy was 97·6% (95% CI 97·4-97·9) at day 28 and 96·0% (95·6-96·5) at day 42. After controlling for age and parasitaemia, patients prescribed a higher dose of artemether had a lower risk of having parasitaemia on day 1 (adjusted odds ratio [OR] 0·92, 95% CI 0·86-0·99 for every 1 mg/kg increase in daily artemether dose; p=0·024), but not on day 2 (p=0·69) or day 3 (0·087). In Asia, children weighing 10-15 kg who received a total lumefantrine dose less than 60 mg/kg had the lowest PCR-adjusted efficacy (91·7%, 95% CI 86·5-96·9). In Africa, the risk of treatment failure was greatest in malnourished children aged 1-3 years (PCR-adjusted efficacy 94·3%, 95% CI 92·3-96·3). A higher artemether dose was associated with a lower gametocyte presence within 14 days of treatment (adjusted OR 0·92, 95% CI 0·85-0·99; p=0·037 for every 1 mg/kg increase in total artemether dose). Interpretation: The recommended dose of artemether-lumefantrine provides reliable efficacy in most patients with uncomplicated malaria. However, therapeutic efficacy was lowest in young children from Asia and young underweight children from Africa; a higher dose regimen should be assessed in these groups. Funding: Bill & Melinda Gates Foundation.
AB - Background: Artemether-lumefantrine is the most widely used artemisinin-based combination therapy for malaria, although treatment failures occur in some regions. We investigated the effect of dosing strategy on efficacy in a pooled analysis from trials done in a wide range of malaria-endemic settings. Methods: We searched PubMed for clinical trials that enrolled and treated patients with artemether-lumefantrine and were published from 1960 to December, 2012. We merged individual patient data from these trials by use of standardised methods. The primary endpoint was the PCR-adjusted risk of Plasmodium falciparum recrudescence by day 28. Secondary endpoints consisted of the PCR-adjusted risk of P falciparum recurrence by day 42, PCR-unadjusted risk of P falciparum recurrence by day 42, early parasite clearance, and gametocyte carriage. Risk factors for PCR-adjusted recrudescence were identified using Cox's regression model with frailty shared across the study sites. Findings: We included 61 studies done between January, 1998, and December, 2012, and included 14 327 patients in our analyses. The PCR-adjusted therapeutic efficacy was 97·6% (95% CI 97·4-97·9) at day 28 and 96·0% (95·6-96·5) at day 42. After controlling for age and parasitaemia, patients prescribed a higher dose of artemether had a lower risk of having parasitaemia on day 1 (adjusted odds ratio [OR] 0·92, 95% CI 0·86-0·99 for every 1 mg/kg increase in daily artemether dose; p=0·024), but not on day 2 (p=0·69) or day 3 (0·087). In Asia, children weighing 10-15 kg who received a total lumefantrine dose less than 60 mg/kg had the lowest PCR-adjusted efficacy (91·7%, 95% CI 86·5-96·9). In Africa, the risk of treatment failure was greatest in malnourished children aged 1-3 years (PCR-adjusted efficacy 94·3%, 95% CI 92·3-96·3). A higher artemether dose was associated with a lower gametocyte presence within 14 days of treatment (adjusted OR 0·92, 95% CI 0·85-0·99; p=0·037 for every 1 mg/kg increase in total artemether dose). Interpretation: The recommended dose of artemether-lumefantrine provides reliable efficacy in most patients with uncomplicated malaria. However, therapeutic efficacy was lowest in young children from Asia and young underweight children from Africa; a higher dose regimen should be assessed in these groups. Funding: Bill & Melinda Gates Foundation.
UR - http://www.scopus.com/inward/record.url?scp=84929505628&partnerID=8YFLogxK
U2 - 10.1016/S1473-3099(15)70024-1
DO - 10.1016/S1473-3099(15)70024-1
M3 - Article
C2 - 25788162
AN - SCOPUS:84929505628
SN - 1473-3099
VL - 15
SP - 692
EP - 702
JO - The Lancet Infectious Diseases
JF - The Lancet Infectious Diseases
IS - 6
ER -