Please use this identifier to cite or link to this item: https://doi.org/10.1128/AAC.02235-17
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dc.titleImidazolopiperazines kill both rings and dormant rings in wild-type and K13 artemisinin-resistant plasmodium falciparum In Vitro
dc.contributor.authorDembele, L
dc.contributor.authorGupta, D.K
dc.contributor.authorLim, M.Y.-X
dc.contributor.authorAng, X
dc.contributor.authorSelva, J.J
dc.contributor.authorChotivanich, K
dc.contributor.authorNguon, C
dc.contributor.authorDondorp, A.M
dc.contributor.authorBonamy, G.M.C
dc.contributor.authorDiagana, T.T
dc.contributor.authorBifania, P
dc.date.accessioned2020-09-09T04:08:57Z
dc.date.available2020-09-09T04:08:57Z
dc.date.issued2018
dc.identifier.citationDembele, L, Gupta, D.K, Lim, M.Y.-X, Ang, X, Selva, J.J, Chotivanich, K, Nguon, C, Dondorp, A.M, Bonamy, G.M.C, Diagana, T.T, Bifania, P (2018). Imidazolopiperazines kill both rings and dormant rings in wild-type and K13 artemisinin-resistant plasmodium falciparum In Vitro. Antimicrobial Agents and Chemotherapy 62 (5) : e02235-17. ScholarBank@NUS Repository. https://doi.org/10.1128/AAC.02235-17
dc.identifier.issn0066-4804
dc.identifier.urihttps://scholarbank.nus.edu.sg/handle/10635/175115
dc.description.abstractArtemisinin (ART) resistance has spread through Southeast Asia, posing a serious threat to the control and elimination of malaria. ART resistance has been associated with mutations in the Plasmodium falciparum kelch-13 (Pfk13) propeller domain. Phenotypically, ART resistance is defined as delayed parasite clearance in patients due to the reduced susceptibility of early ring-stage parasites to the active metabolite of ART dihydroartemisinin (DHA). Early rings can enter a state of quiescence upon DHA exposure and resume growth in its absence. These quiescent rings are referred to as dormant rings or DHA-pretreated rings (here called dormant rings). The imidazolopiperazines (IPZ) are a novel class of antimalarial drugs that have demonstrated efficacy in early clinical trials. Here, we characterized the stage of action of the IPZ GNF179 and evaluated its activity against rings and dormant rings in wild-type and ART-resistant parasites. Unlike DHA, GNF179 does not induce dormancy. We show that GNF179 is more rapidly cidal against schizonts than against ring and trophozoite stages. However, with 12 h of exposure, the compound effectively kills rings and dormant rings of both susceptible and ART-resistant parasites within 72 h. We further demonstrate that in combination with ART, GNF179 effectively prevents recrudescence of dormant rings, including those bearing pfk13 propeller mutations. © 2018 Dembele et al.
dc.publisherAmerican Society for Microbiology
dc.sourceUnpaywall 20200831
dc.subjectantimalarial agent
dc.subjectdihydroartemisinin
dc.subjectdimethyl sulfoxide
dc.subjectgnf 179
dc.subjectimidazole derivative
dc.subjectkdu 691
dc.subjectkelch 13 protein
dc.subjectmembrane protein
dc.subjectmicroorganism protein
dc.subjectpiperazine derivative
dc.subjectunclassified drug
dc.subjectantimalarial agent
dc.subjectartemisinin derivative
dc.subjectimidazole derivative
dc.subjectpiperazine derivative
dc.subjectprotozoal protein
dc.subjectantimalarial activity
dc.subjectantimalarial drug resistance
dc.subjectantimalarial drug susceptibility
dc.subjectapoptosis
dc.subjectArticle
dc.subjectcell viability
dc.subjectcombination drug therapy
dc.subjectcontrolled study
dc.subjectdevelopment
dc.subjectdormancy
dc.subjectdrug efficacy
dc.subjectdrug mechanism
dc.subjectdrug potentiation
dc.subjecterythrocyte
dc.subjectgenotype
dc.subjectIC50
dc.subjectin vitro study
dc.subjectnonhuman
dc.subjectPlasmodium falciparum
dc.subjectpriority journal
dc.subjectrecrudescence
dc.subjectschizont
dc.subjecttrophozoite
dc.subjectwild type
dc.subjectdrug effect
dc.subjectdrug sensitivity
dc.subjectgenetics
dc.subjectmetabolism
dc.subjectPlasmodium falciparum
dc.subjectAntimalarials
dc.subjectArtemisinins
dc.subjectImidazoles
dc.subjectParasitic Sensitivity Tests
dc.subjectPiperazines
dc.subjectPlasmodium falciparum
dc.subjectProtozoan Proteins
dc.subjectSchizonts
dc.subjectTrophozoites
dc.typeArticle
dc.contributor.departmentMICROBIOLOGY AND IMMUNOLOGY
dc.description.doi10.1128/AAC.02235-17
dc.description.sourcetitleAntimicrobial Agents and Chemotherapy
dc.description.volume62
dc.description.issue5
dc.description.pagee02235-17
dc.published.statePublished
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