Plasmodium falciparum resistance to ACTs: Emergence, mechanisms, and outlook

Siddiqui, Faiza Amber; Liang, Xiaoying

doi:10.1016/j.ijpddr.2021.05.007

Cited by 47 publications

(40 citation statements)

References 268 publications

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“…Cox’s Bazar reported a median (range) slope of parasite clearance half-life (PC 1/2 ) of 2.5 (0.7 to 5.4) between 6 and 24 h after administration. Unlike many studies that report K13 polymorphism with either RSA or parasite clearance data ( 30 – 32 ), we established both, because it was important to undertake correlative analyses between RSA values and slope half-lives of <5.5 h and to obtain insight that the RSA value is a better indicator of low levels of AR than PC 1/2 . Notably, RSA values of >1.0% are recognized by WHO to signify resistance and low RSA values ranging from 1 to 4 are consequential.…”

Section: Discussionmentioning

confidence: 99%

Assessment of Plasmodium falciparum Artemisinin Resistance Independent of kelch13 Polymorphisms and with Escalating Malaria in Bangladesh

Nima

Mukherjee

Sazed

et al. 2022

mBio

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Section: Discussionmentioning

confidence: 99%

Assessment of Plasmodium falciparum Artemisinin Resistance Independent of kelch13 Polymorphisms and with Escalating Malaria in Bangladesh

Nima

Mukherjee

Sazed

et al. 2022

mBio

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“…To simulate parasite growth and evolution in the absence and/or presence of drug, we created a more sophisticated version of DARPS (Discrete Asexually Reproducing Population Simulator) [74], dubbed DARPS2. Each simulation was initiated with a monoculture of one of the 11 parasite lines under investigation, which was intended to simulate a population of parasites that was exiting the liver one week after initial sporozoite infection (here, we used an initial population 5×10 5 new asexual blood stage parasites [83]). During each synchronous discrete timestep, the number of parasites for each given line was updated by multiplying the number…”

Section: Simulation Modelmentioning

confidence: 99%

“…However, delayed parasite clearance after ART treatment is now present throughout SE Asia. Resistance has also emerged to the ACT partner drug piperaquine (PPQ), leading to up to 50% treatment failures with this combination in some areas of the Greater Mekong Subregion [4,5]. Mutations in the transmembrane protein Plasmodium falciparum chloroquine resistance transporter (PfCRT) have been shown to be the major drivers of high-grade CQ and more recently, PPQ resistance [6][7][8][9][10].…”

Section: Introductionmentioning

confidence: 99%

Evidence for the early emergence of piperaquine-resistant Plasmodium falciparum malaria and modeling strategies to mitigate resistance

et al. 2022

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Multidrug-resistant Plasmodium falciparum parasites have emerged in Cambodia and neighboring countries in Southeast Asia, compromising the efficacy of first-line antimalarial combinations. Dihydroartemisinin + piperaquine (PPQ) treatment failure rates have risen to as high as 50% in some areas in this region. For PPQ, resistance is driven primarily by a series of mutant alleles of the P. falciparum chloroquine resistance transporter (PfCRT). PPQ resistance was reported in China three decades earlier, but the molecular driver remained unknown. Herein, we identify a PPQ-resistant pfcrt allele (China C) from Yunnan Province, China, whose genotypic lineage is distinct from the PPQ-resistant pfcrt alleles currently observed in Cambodia. Combining gene editing and competitive growth assays, we report that PfCRT China C confers moderate PPQ resistance while re-sensitizing parasites to chloroquine (CQ) and incurring a fitness cost that manifests as a reduced rate of parasite growth. PPQ transport assays using purified PfCRT isoforms, combined with molecular dynamics simulations, highlight differences in drug transport kinetics and in this transporter’s central cavity conformation between China C and the current Southeast Asian PPQ-resistant isoforms. We also report a novel computational model that incorporates empirically determined fitness landscapes at varying drug concentrations, combined with antimalarial susceptibility profiles, mutation rates, and drug pharmacokinetics. Our simulations with PPQ-resistant or -sensitive parasite lines predict that a three-day regimen of PPQ combined with CQ can effectively clear infections and prevent the evolution of PfCRT variants. This work suggests that including CQ in combination therapies could be effective in suppressing the evolution of PfCRT-mediated multidrug resistance in regions where PPQ has lost efficacy.

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“…Concerning the ‘in vivo’ action of artemisinin, artemisinin is thought to be activated (radicalized) primarily by heme, which is mainly derived from hemoglobin digestion in the food vacuole of malaria parasites in red blood cells [ 10 ]. Activated artemisinin and the resulting reactive oxygen species (ROS) can react promiscuously with a wide range of cellular targets, disrupting cellular protein homeostasis [ 22 , 24 ]. Several mutations associated with artemisinin resistance were reported in the P. falciparum genes, including PfFd and ribosomal protein S10 in apicoplasts, autophagy-related protein, purine nucleoside phosphorylase, and chloroquine resistance transporter.…”

Section: Resultsmentioning

confidence: 99%

“…Several mutations associated with artemisinin resistance were reported in the P. falciparum genes, including PfFd and ribosomal protein S10 in apicoplasts, autophagy-related protein, purine nucleoside phosphorylase, and chloroquine resistance transporter. Among them, the mutations of the kelch family protein K13 (assumed to be either a regulator of polyubiquitination of PfPI3K or a ubiquitin E3 ligase substrate adaptor) are considered as the key determinant of artemisinin resistance [ 24 ]. The molecular mechanisms of K13-mediated artemisinin resistance involve reduced hemoglobin uptake/digestion and an increased cellular stress response against ROS, in which K13 mutations alter multiple aspects of the parasite’s intra-erythrocytic developmental program.…”

Section: Resultsmentioning

confidence: 99%

Effect of Artemisinin on the Redox System of NADPH/FNR/Ferredoxin from Malaria Parasites

Kimata‐Ariga

Morihisa

2022

Antioxidants

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FNR and ferredoxin constitute a redox cascade, which provides reducing power in the plastid of malaria parasites. Recently, mutation of ferredoxin (D97Y) was reported to be strongly related to the parasite’s resistance to the front-line antimalarial drug artemisinin. In order to gain insight into the mechanism for the resistance, we studied the effect of dihydroartemisinin (DHA), the active compound of artemisinin, on the redox cascade of NADPH/FNR/ferredoxin in in vitro reconstituted systems. DHA partially inhibited the diaphorase activity of FNR by decreasing the affinity of FNR for NADPH. The activity of the electron transfer from FNR to wild-type or D97Y mutant ferredoxin was not significantly affected by DHA. An in silico docking analysis indicated possible binding of DHA molecule in the binding cavity of 2′5′ADP, a competitive inhibitor for NADPH, on FNR. We previously showed that the D97Y mutant of ferredoxin binds to FNR more strongly than wild-type ferredoxin, and ferredoxin and FNR are generally known to be involved in the oxidative stress response. Thus, these results suggest that ferredoxin is not a direct target of artemisinin, but its mutation may be involved in the protective response against the oxidative stress caused by artemisinin.

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Plasmodium falciparum resistance to ACTs: Emergence, mechanisms, and outlook

Cited by 47 publications

References 268 publications

Assessment of Plasmodium falciparum Artemisinin Resistance Independent of kelch13 Polymorphisms and with Escalating Malaria in Bangladesh

Assessment of Plasmodium falciparum Artemisinin Resistance Independent of kelch13 Polymorphisms and with Escalating Malaria in Bangladesh

Evidence for the early emergence of piperaquine-resistant Plasmodium falciparum malaria and modeling strategies to mitigate resistance

Effect of Artemisinin on the Redox System of NADPH/FNR/Ferredoxin from Malaria Parasites

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