Little polymorphism at the K13 propeller locus in worldwide Plasmodium falciparum populations prior to the introduction of artemisinin combination therapies

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dc.contributor.author Mita, Toshihiro
dc.contributor.author Culleton, Richard
dc.contributor.author Takahashi, Nobuyuki
dc.contributor.author Nakamura, Masatoshi
dc.contributor.author Tsukahara, Takahiro
dc.contributor.author Hunja, Carol W.
dc.contributor.author Win, Zin Z.
dc.contributor.author Htike, Wah W.
dc.contributor.author Marma, Aung S.
dc.contributor.author Dysoley, Lek
dc.contributor.author Ndounga, Mathieu
dc.contributor.author Dzodzomenyo, Mawuli
dc.contributor.author Akhwale, Willis S.
dc.contributor.author Kobayashi, Jun
dc.contributor.author Uemura, Haruki
dc.contributor.author Kaneko, Akira
dc.contributor.author Hombhanje, Francis
dc.contributor.author Ferreira, Marcelo U.
dc.contributor.author Björkman, Anders
dc.contributor.author Endo, Hiroyuki
dc.contributor.author Ohashi, Jun
dc.date.accessioned 2016-04-11T08:35:38Z
dc.date.available 2016-04-11T08:35:38Z
dc.date.issued 2016
dc.identifier.citation Antimicrobial Agents and Chemotherapy en_US
dc.identifier.uri http://aac.asm.org/content/early/2016/03/15/AAC.02370-15.abstract
dc.identifier.uri http://repository.seku.ac.ke/handle/123456789/2054
dc.description.abstract The emergence and spread of artemisinin-resistant Plasmodium falciparum is of huge concern for the global effort toward malaria control and elimination. Artemisinin resistance, defined as a delayed time to parasite clearance following administration of artemisinin, is associated with mutations in the Pfkelch13 gene of resistant parasites. To date, as many as 60 non-synonymous mutations have been identified in this gene, but whether these mutations have been selected by artemisinin usage or merely reflect natural polymorphism independent of selection is currently unknown. To clarify this, we sequenced the Pfkelch13-propeller domain in 581 isolates collected before (420) and after (161) the implementation of artemisinin combination therapies (ACTs), from various endemic regions worldwide. Non-synonymous mutations were observed in 1% of parasites isolated prior to the introduction of ACTs. Frequencies of mutant isolates, nucleotide diversity and haplotype diversity were significantly higher in the parasites isolated from populations exposed to artemisinin compared to those from populations that had not been exposed to the drug. In the artemisinin-exposed population, a significant excess of dN compared to dS was observed, suggesting the presence of positive selection. In contrast, pairwise comparison of dN and dS and the McDonald and Kreitman test indicates that purifying selection acts on the Pfkelch13-propeller domain in populations not exposed to ACTs. These population-genetic analyses reveal a low baseline of Pfkelch13 polymorphism, probably due to purifying selection in the absence of artemisinin selection. In contrast, various Pfkelch13 mutations have been selected under artemisinin pressure. en_US
dc.language.iso en en_US
dc.publisher American Society for Microbiology en_US
dc.title Little polymorphism at the K13 propeller locus in worldwide Plasmodium falciparum populations prior to the introduction of artemisinin combination therapies en_US
dc.type Article en_US


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