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dc.contributor.authorChecchi, Francesco
dc.contributor.authorPiola, Patrice
dc.contributor.authorFogg, Carole
dc.contributor.authorBajunirwe, Francis
dc.contributor.authorBiraro, Samuel
dc.contributor.authorGrandesso, Francesco
dc.contributor.authorRuzagira, Eugene
dc.contributor.authorBabigumira, Joseph
dc.contributor.authorKigozi, Isaac
dc.contributor.authorKiguli, James
dc.contributor.authorKyomuhendo, Juliet
dc.contributor.authorFerradini, Laurent
dc.contributor.authorTaylor, Walter RJ
dc.contributor.authorGuthmann, Jean-Paul
dc.date.accessioned2021-12-01T12:48:30Z
dc.date.available2021-12-01T12:48:30Z
dc.date.issued2006
dc.identifier.citationChecchi, F., Piola, P., Fogg, C., Bajunirwe, F., Biraro, S., Grandesso, F., ... & Guthmann, J. P. (2006). Supervised versus unsupervised antimalarial treatment with six-dose artemether-lumefantrine: pharmacokinetic and dosage-related findings from a clinical trial in Uganda. Malaria journal, 5(1), 1-8.en_US
dc.identifier.urihttp://ir.must.ac.ug/xmlui/handle/123456789/1058
dc.description.abstractBackground: A six-dose antimalarial regimen of artemether-lumefantrine (A/L) may soon become one of the most widely used drug combination in Africa, despite possible constraints with adherence and poor absorption due to inadequate nutrition, and a lack of pharmacokinetic and effectiveness data. Methods: Within a trial of supervised versus unsupervised A/L treatment in a stable Ugandan Plasmodium falciparum transmission setting, plasma lumefantrine concentrations were measured in a subset of patients on day 3 (C [lum]day3) and day 7 (C [lum]day7) post-inclusion. Predictors of lumefantrine concentrations were analysed to show how both C [lum]day7 and the weight-adjusted lumefantrine dose affect 28-day recrudescence and re-infection risks. The implications of these novel findings are discussed in terms of the emergence of lumefantrine-resistant strains in Africa. Results: C [lum]day3 and C [lum]day7 distributions among 241 supervised and 238 unsupervised patients were positively skewed. Unsupervised treatment and decreasing weight-adjusted lumefantrine dose were negatively associated with C [lum]day3. Unsupervised treatment and decreasing age showed strong negative associations with C [lum]day7. Both models were poorly predictive (R-squared < 0.25). There were no recrudescences in either arm, but decreasing lumefantrine dose per Kg resulted in up to 13-fold higher adjusted risks of re-infection. Re-infections occurred only among patients with C [lum]day7 below 400 ng/ mL (p < 0.001). Conclusion: Maintaining the present six-dose regimen and ensuring high adherence and intake are essential to maximize the public health benefits of this valuable drug combination.en_US
dc.description.sponsorshipMédecins Sans Frontières.en_US
dc.language.isoen_USen_US
dc.publisherMalaria Journalen_US
dc.subjectAntimalarial treatmenten_US
dc.subjectArtemether-lumefantrineen_US
dc.subjectPharmacokineticen_US
dc.subjectUgandaen_US
dc.titleSupervised versus unsupervised antimalarial treatment with six-dose artemether-lumefantrine: pharmacokinetic and dosage-related findings from a clinical trial in Ugandaen_US
dc.typeArticleen_US


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