Persistence of Plasmodium falciparum parasitemia after artemisinin combination therapy: evidence from a randomized trial in Uganda

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作者
Hsiao-Han Chang
Elamaran Meibalan
Justin Zelin
Rachel Daniels
Alice C. Eziefula
Evan C. Meyer
Fitsum Tadesse
Lynn Grignard
Regina C. Joice
Chris Drakeley
Dyann F. Wirth
Sarah K. Volkman
Caroline Buckee
Teun Bousema
Matthias Marti
机构
[1] Center for Communicable Disease Dynamics,Department of Epidemiology
[2] Harvard T.H. Chan School of Public Health,Department of Immunology and Infectious Diseases
[3] 665 Huntington Ave,Immunology and Infection Department
[4] Boston,undefined
[5] MA 02115,undefined
[6] USA,undefined
[7] Harvard T.H. Chan School of Public Health,undefined
[8] 665 Huntington Ave,undefined
[9] Boston,undefined
[10] MA 02115,undefined
[11] USA,undefined
[12] Broad Institute of MIT and Harvard,undefined
[13] 415 Main Street,undefined
[14] Cambridge,undefined
[15] MA 02142,undefined
[16] USA ,undefined
[17] London School of Hygiene and Tropical Medicine,undefined
[18] Keppel Street,undefined
[19] London,undefined
[20] WC1E 7HT,undefined
[21] UK,undefined
[22] Simmons College,undefined
[23] 300 Fenway,undefined
[24] Boston,undefined
[25] MA 02115,undefined
[26] USA ,undefined
[27] Institute for Molecular Life Sciences,undefined
[28] Radboud University,undefined
[29] Geert Grooteplain Zuid 28,undefined
[30] 6525 GA Nijmegen,undefined
[31] The Netherlands ,undefined
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摘要
Artemisinin resistance is rapidly spreading in Southeast Asia. The efficacy of artemisinin-combination therapy (ACT) continues to be excellent across Africa. We performed parasite transcriptional profiling and genotyping on samples from an antimalarial treatment trial in Uganda. We used qRT-PCR and genotyping to characterize residual circulating parasite populations after treatment with either ACT or ACT-primaquine. Transcripts suggestive of circulating ring stage parasites were present after treatment at a prevalence of >25% until at least 14 days post initiation of treatment. Greater than 98% of all ring stage parasites were cleared within the first 3 days, but subsequently persisted at low concentrations until day 14 after treatment. Genotyping demonstrated a significant decrease in multiplicity of infection within the first 2 days in both ACT and ACT-primaquine arms. However, multiple clone infections persisted until day 14 post treatment. Our data suggest the presence of genetically diverse persisting parasite populations after ACT treatment. Although we did not demonstrate clinical treatment failures after ACT and the viability and transmissibility of persisting ring stage parasites remain to be shown, these findings are of relevance for the interpretation of parasite clearance transmission dynamics and for monitoring drug effects in Plasmodium falciparum parasites.
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