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Antimalarial chemoprophylaxis for forest goers in southeast Asia: an open-label, individually randomised controlled trial

Authors :
Tripura, Rupam
von Seidlein, Lorenz
Sovannaroth, Siv
Peto, Thomas J
Callery, James J
Sokha, Meas
Ean, Mom
Heng, Chhouen
Conradis-Jansen, Franca
Madmanee, Wanassanan
Peerawaranun, Pimnara
Waithira, Naomi
Khonputsa, Panarasri
Jongdeepaisal, Monnaphat
Pongsoipetch, Kulchada
Chotthanawathit, Paphapisa
Soviet, Ung
Pell, Christopher
Duanguppama, Jureeporn
Rekol, Huy
Tarning, Joel
Imwong, Mallika
Mukaka, Mavuto
White, Nicholas J
Dondorp, Arjen M
Maude, Richard
Tripura, Rupam
von Seidlein, Lorenz
Sovannaroth, Siv
Peto, Thomas J
Callery, James J
Sokha, Meas
Ean, Mom
Heng, Chhouen
Conradis-Jansen, Franca
Madmanee, Wanassanan
Peerawaranun, Pimnara
Waithira, Naomi
Khonputsa, Panarasri
Jongdeepaisal, Monnaphat
Pongsoipetch, Kulchada
Chotthanawathit, Paphapisa
Soviet, Ung
Pell, Christopher
Duanguppama, Jureeporn
Rekol, Huy
Tarning, Joel
Imwong, Mallika
Mukaka, Mavuto
White, Nicholas J
Dondorp, Arjen M
Maude, Richard

Abstract

Background Malaria in the eastern Greater Mekong subregion has declined to historic lows. Countries in the Greater Mekong subregion are accelerating malaria elimination in the context of increasing antimalarial drug resistance. Infections are now increasingly concentrated in remote, forested foci. No intervention has yet shown satisfactory efficacy against forest-acquired malaria. The aim of this study was to assess the efficacy of malaria chemoprophylaxis among forest goers in Cambodia. MethodsWe conducted an open-label, individually randomised controlled trial in Cambodia, which recruited participants aged 16-65 years staying overnight in forests. Participants were randomly allocated 1:1 to antimalarial chemoprophylaxis, a 3-day course of twice-daily artemether-lumefantrine followed by the same daily dosing once a week while travelling in the forest and for a further 4 weeks after leaving the forest (four tablets per dose; 20 mg of artemether and 120 mg of lumefantrine per tablet), or a multivitamin with no antimalarial activity. Allocations were done according to a computer-generated randomisation schedule, and randomisation was in permuted blocks of size ten and stratified by village. Investigators and participants were not masked to drug allocation, but laboratory investigations were done without knowledge of allocation. The primary outcome was a composite endpoint of either clinical malaria with any Plasmodium species within 1-28, 29-56, or 57-84 days, or subclinical infection detected by PCR on days 28, 56, or 84 using complete-case analysis of the intention-to-treat population. Adherence to study drug was assessed primarily by self-reporting during follow-up visits. Adverse events were assessed in the intention-to-treat population as a secondary endpoint from self-reporting at any time, plus a physical examination and symptom questionnaire at follow-up. This trial is registered at ClinicalTrials.gov (NCT04041973) and i

Details

Database :
OAIster
Notes :
application/pdf, application/pdf, https://oro.open.ac.uk/85546/8/85546final.pdf, English, English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1358938636
Document Type :
Electronic Resource

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