Mutations in the Plasmodium falciparum chloroquine resistance transporter, PfCRT, enlarge the parasite’s food vacuole and alter drug sensitivities

Pulcini, Serena; Staines, Henry M.; Lee, Andrew H.; Shafik, Sarah H.; Bouyer, Guillaume; Moore, Catherine; Daley, Daniel A.; Hoke, M.; Altenhofen, Lindsey M.; Painter, Heather J.; Mu, Jianbing; Ferguson, David J. P.; Llinás, Manuel; Martin, R. L.; Fidock, David A.; Cooper, Roland A.; Krishna, Sanjeev

doi:10.1038/srep14552

Cited by 66 publications

(65 citation statements)

References 70 publications

(107 reference statements)

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“…3; Table S1), consistent with the appearance of this mutation in the AMT-resistant FCB C101F parasites (69). Our data also documented a 2-fold increase in the BSD IC 50 s of Dd2 Dd2+C101F clones compared to Dd2 Dd2 ( P < 0.001).…”

Section: Resultssupporting

confidence: 77%

A Variant PfCRT Isoform Can Contribute to Plasmodium falciparum Resistance to the First-Line Partner Drug Piperaquine

Dhingra

Redhi

Combrinck

et al. 2017

mBio

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107

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Current efforts to reduce the global burden of malaria are threatened by the rapid spread throughout Asia of Plasmodium falciparum resistance to artemisinin-based combination therapies, which includes increasing rates of clinical failure with dihydroartemisinin plus piperaquine (PPQ) in Cambodia. Using zinc finger nuclease-based gene editing, we report that addition of the C101F mutation to the chloroquine (CQ) resistance-conferring PfCRT Dd2 isoform common to Asia can confer PPQ resistance to cultured parasites. Resistance was demonstrated as significantly higher PPQ concentrations causing 90% inhibition of parasite growth (IC90) or 50% parasite killing (50% lethal dose [LD50]). This mutation also reversed Dd2-mediated CQ resistance, sensitized parasites to amodiaquine, quinine, and artemisinin, and conferred amantadine and blasticidin resistance. Using heme fractionation assays, we demonstrate that PPQ causes a buildup of reactive free heme and inhibits the formation of chemically inert hemozoin crystals. Our data evoke inhibition of heme detoxification in the parasite’s acidic digestive vacuole as the primary mode of both the bis-aminoquinoline PPQ and the related 4-aminoquinoline CQ. Both drugs also inhibit hemoglobin proteolysis at elevated concentrations, suggesting an additional mode of action. Isogenic lines differing in their pfmdr1 copy number showed equivalent PPQ susceptibilities. We propose that mutations in PfCRT could contribute to a multifactorial basis of PPQ resistance in field isolates.

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Section: Resultssupporting

confidence: 77%

A Variant PfCRT Isoform Can Contribute to Plasmodium falciparum Resistance to the First-Line Partner Drug Piperaquine

Dhingra

Redhi

Combrinck

et al. 2017

mBio

Self Cite

107

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“…These mutations include K76T, ubiquitous to all CQ-resistant alleles irrespective of origin and a sensitive marker of in vivo CQ treatment failure (Supplementary Table 1). In addition, several novel PfCRT mutations have been observed that can revert parasites to a CQ-sensitive status despite the presence of K76T, including C101F—which arose under pip-eraquine (PPQ) or amantadine pressure in vitro 42,166 —or C350R, which has recently spread throughout French Guiana 167 . Some PfCRT variants also mediate resistance to the active metabolite of AQ (monodesethyl-AQ), which might have been an important driving force for selection 168,169 .…”

Section: Multidrug Resistance (Mdr)mentioning

confidence: 99%

Antimalarial drug resistance: linking Plasmodium falciparum parasite biology to the clinic

Blasco

Leroy

Fidock

2017

Nat Med

440

419

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The global adoption of artemisinin-based combination therapies (ACTs) in the early 2000s heralded a new era in effectively treating drug-resistant Plasmodium falciparum malaria. However, several Southeast Asian countries have now reported the emergence of parasites that have decreased susceptibility to artemisinin (ART) derivatives and ACT partner drugs, resulting in increasing rates of treatment failures. Here we review recent advances in understanding how antimalarials act and how resistance develops, and discuss new strategies for effectively combatting resistance, optimizing treatment and advancing the global campaign to eliminate malaria.

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“…It was demonstrated that P. falciparum lines subjected to selection by amantadine or blasticidin carried the mutations in PfCRT (C101F or L272F) resulting in the enlargement of the parasite's food vacuole and alter the drug sensitivity, manifested by increased susceptibility to choloroquine and other quinoline antimalarials [50]. The swollen DV may be accounted for by presence of mutations interfering with the transport of the natural substrates of PfCRT out of the food vacuole, resulting in increased osmotic pressure in the food vacuole.…”

Section: Discussionmentioning

confidence: 99%

“…Two independent genome-wide association studies (GWAS) showed that amplification of the PM2 gene was associated with reduced PPQ sensitivity [19,20]. Targeted gene disruption of either PM2 or PM3 in P. falciparum 3D7 background accounted for a slight decrease in PPQ IC 50 value, but a significantly increased sensitivity to PPQ in a modified PSA [28]. However, the overexpression of PM2 and PM3 in the 3D7 genetic background did not alter the sensitivity of P. falciparum to PPQ, suggesting that the increase in PM2 copy number alone is not the sole modulator of PPQ resistance [29].…”

Section: Introductionmentioning

confidence: 99%

Piperaquine resistant Cambodian Plasmodium falciparum clinical isolates: in vitro genotypic and phenotypic characterization

Boonyalai

Vesely

Thamnurak

et al. 2020

Preprint

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Background: High rates of dihydroartemisinin-piperaquine (DHA-PPQ) treatment failures have been documented for uncomplicated Plasmodium falciparum in Cambodia. It is essential to establish sensitive and reliable markers of PPQ resistance which can be adopted for monitoring the prevalence of drug resistance and guide drug policy change. Several genetic markers have been proposed such as copy numbers of P. falciparum multidrug resistance 1 ( pfmdr1 ) and plasmepsin 2 (PM2), and mutations in exonuclease (exo-E415G) and P. falciparum chloroquine resistance transporter (PfCRT) genes.Methods: To examine the relative contribution of each marker to PPQ resistance, in vitro culture and the PPQ survival assay were performed on seventeen P. falciparum isolates from northern Cambodia and the presence of exo-E415G and PfCRT mutations as well as PM2 copy number polymorphisms were determined. Parasites were then cloned by limiting dilution and the cloned parasites were tested for drug susceptibility. The efficacy of several drug combinations between standard clones and newly cloned P. falciparum Cambodian isolates was also measured.Results: The characterization of culture-adapted isolates revealed that exo-E415G and novel PfCRT mutations can confer PPQ-resistance, in the absence of PM2 amplification. In vitro testing of PPQ resistant parasites showed bimodal dose-response phenotype as previously reported in both Cambodian isolates and genome-edited Dd2 strains. Our finding is the first PPQ resistant clinical isolate with documented swollen digestive vacuole phenotype. From the field isolates, we were able to clone a new parasite line, 14-B5, which is sensitive to arteminsinin and piperaquine but resistant to chloroquine. Most of the drug combinations tested revealed antagonistic interaction against the 14-B5 line, indicating its different genetic background from other P. falciparum laboratory reference lines.Conclusions: Surveillance for PPQ resistance in regions that rely on DHA-PPQ as the first line treatment should depend on the monitoring of the reflective molecular markers. Bimodal dose response curves and swelling of the food vacuole can be used as PPQ resistant phenotype. The use of currently circulating parasite isolates is necessary for relevant drug combination development against current P. falciparum resistance profiles.

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Mutations in the Plasmodium falciparum chloroquine resistance transporter, PfCRT, enlarge the parasite’s food vacuole and alter drug sensitivities

Cited by 66 publications

References 70 publications

A Variant PfCRT Isoform Can Contribute to Plasmodium falciparum Resistance to the First-Line Partner Drug Piperaquine

A Variant PfCRT Isoform Can Contribute to Plasmodium falciparum Resistance to the First-Line Partner Drug Piperaquine

Antimalarial drug resistance: linking Plasmodium falciparum parasite biology to the clinic

Piperaquine resistant Cambodian Plasmodium falciparum clinical isolates: in vitro genotypic and phenotypic characterization

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