Mechanisms of Artemisinin Resistance in the Rodent Malaria Pathogen
            <i>Plasmodium yoelii</i>

Walker, Daniel J.; Pitsch, Jessica L.; Peng, Michael; Robinson, B. L.; Peters, W.; Bhisutthibhan, Jamaree; Meshnick, Steven R.

doi:10.1128/aac.44.2.344-347.2000

Cited by 70 publications

(54 citation statements)

References 18 publications

(18 reference statements)

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“…Several proteins have been shown to interact with artemisinin. The translationally controlled tumor protein (TCTP) binds to radioactively labeled dihydroartemisinin (5) and is overexpressed in rodent Plasmodium yoelii parasite lines with decreased susceptibility to artemisinin (44). Another protein that may interact with artemisinins is the sarcoplasmic reticulum Ca 2ϩ ATPase 6 (PfATP6); this enzyme, when expressed in Xenopus oocytes, was specifically inhibited by artemisinin derivatives containing an endoperoxide bridge (11).…”

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confidence: 99%

Role ofpfmdr1Amplification and Expression in Induction of Resistance to Artemisinin Derivatives inPlasmodium falciparum

Chavchich

Gerena

Peters

et al. 2010

Antimicrob Agents Chemother

105

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Artemisinin and its derivatives are the most rapidly acting and efficacious antimalarial drugs currently available. Although resistance to these drugs has not been documented, there is growing concern about the potential for resistance to develop. In this paper we report the selection of parasite resistance to artelinic acid (AL) and artemisinin (QHS) in vitro and the molecular changes that occurred during the selection. Exposure of three Plasmodium falciparum lines (W2, D6, and TM91C235) to AL resulted in decreases in parasite susceptibilities to AL and QHS, as well as to mefloquine, quinine, halofantrine, and lumefantrine. The changes in parasite susceptibility were accompanied by increases in the copy number, mRNA expression, and protein expression of the pfmdr1 gene in the resistant progenies of W2 and TM91C235 parasites but not in those of D6 parasites. No changes were detected in the coding sequences of the pfmdr1, pfcrt, pfatp6, pftctp, and pfubcth genes or in the expression levels of pfatp6 and pftctp. Our data demonstrate that P. falciparum lines have the capacity to develop resistance to artemisinin derivatives in vitro and that this resistance is achieved by multiple mechanisms, to include amplification and increased expression of pfmdr1, a mechanism that also confers resistance to mefloquine. This observation is of practical importance, because artemisinin drugs are often used in combination with mefloquine for the treatment of malaria.

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confidence: 99%

Role ofpfmdr1Amplification and Expression in Induction of Resistance to Artemisinin Derivatives inPlasmodium falciparum

Chavchich

Gerena

Peters

et al. 2010

Antimicrob Agents Chemother

105

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“…Since the food vacuole is rich in heme (29), it is possible that artemisinin might react with the TCTP molecules associated with this structure. Artemisinin-resistant strains of Plasmodium yoelii express higher levels of TCTP than do artemisinin-sensitive strains (33). However, there is no direct evidence that the alkylation of TCTP by artemisinin is responsible for the antimalarial effects of the drug.…”

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confidence: 84%

Immunoprecipitation of [ ³ H]Dihydroartemisinin Translationally Controlled Tumor Protein (TCTP) Adducts from Plasmodium falciparum -Infected Erythrocytes by Using Anti-TCTP Antibodies

Bhisutthibhan

Meshnick

2001

Antimicrob Agents Chemother

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“…Overexpression of TCTP in mammalian cells resulted in slow growth and a delay in cell cycle progression [31]. An increase in TCTP levels was reported to be associated with increased chemoresistance [34,35]. Overexpression of mammalian TCTP results in microtubule stabilization and alteration of cell morphology [31].…”

Section: Discussionmentioning

confidence: 99%

Proteomic analysis of tumor tissue in CT-26 implanted BALB/C mouse after treatment with ascorbic acid

Lee¹,

Lee²,

Park³

et al. 2012

Cellular and Molecular Biology Letters

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Abbreviations used: ATP -adenosine triphosphate; DTT -dithiothreitol; ECMextracellular matrix; GDT -guanosine diphosphate; LR -log ratio; MALDI TOF-MS/MS -Matrix-assisted laser-desorption ionization time-of-flight tandem mass spectroscopy; MMPs -matrix metalloproteinases; PAGE -polyacrylamide gel electrophoresis; PBSphosphate buffered solution; PCR -polymerase chain reaction; SDS -sodium dodecyl sulfate; TCA -trichloroacetic acid; TCTP -translationally controlled tumor protein; 2-DE -two-dimensional gel electrophoresis Abstract: Tumor establishment and penetration consists of a series of complex processes involving multiple changes in gene expression and protein modification. Proteome changes of tumor tissue were investigated after intraperitoneal administration of a high concentration of ascorbic acid in BALB/C mice implanted with CT-26 cancer cells using two-dimensional gel electrophoresis and mass spectrometry. Eighteen protein spots were identified whose expression was different between control and ascorbic acid treatment groups. In particular, eukaryotic translation initiation factor 3 subunit 1, nucleophosmin, latexin, actin-related protein 2/3 complex subunit 5, M2-type pyruvate kinase, vimentin, tumor protein translationally-controlled 1, RAS oncogene family Ran, plastin 3 precursor, ATPase, Rho GDT dissociation inhibitor β, and proteasome activator subunit 2 expression were quantitatively up-regulated. The increase in the level of these proteins was accompanied by an increase in mRNA level. The cytoskeleton protein actin, vimentin, and tumor protein translationally-controlled 1 showed quantitative expression profile differences. A change in actin cytoskeleton distribution, functionally relevant to the proteome result, was observed after treatment with ascorbic acid. These

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Mechanisms of Artemisinin Resistance in the Rodent Malaria Pathogen Plasmodium yoelii

Cited by 70 publications

References 18 publications

Role ofpfmdr1Amplification and Expression in Induction of Resistance to Artemisinin Derivatives inPlasmodium falciparum

Role ofpfmdr1Amplification and Expression in Induction of Resistance to Artemisinin Derivatives inPlasmodium falciparum

Immunoprecipitation of [ ³ H]Dihydroartemisinin Translationally Controlled Tumor Protein (TCTP) Adducts from Plasmodium falciparum -Infected Erythrocytes by Using Anti-TCTP Antibodies

Proteomic analysis of tumor tissue in CT-26 implanted BALB/C mouse after treatment with ascorbic acid

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Mechanisms of Artemisinin Resistance in the Rodent Malaria Pathogen Plasmodium yoelii

Cited by 70 publications

References 18 publications

Role ofpfmdr1Amplification and Expression in Induction of Resistance to Artemisinin Derivatives inPlasmodium falciparum

Role ofpfmdr1Amplification and Expression in Induction of Resistance to Artemisinin Derivatives inPlasmodium falciparum

Immunoprecipitation of [ 3 H]Dihydroartemisinin Translationally Controlled Tumor Protein (TCTP) Adducts from Plasmodium falciparum -Infected Erythrocytes by Using Anti-TCTP Antibodies

Proteomic analysis of tumor tissue in CT-26 implanted BALB/C mouse after treatment with ascorbic acid

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Immunoprecipitation of [ ³ H]Dihydroartemisinin Translationally Controlled Tumor Protein (TCTP) Adducts from Plasmodium falciparum -Infected Erythrocytes by Using Anti-TCTP Antibodies