Dictyostelium Discoideum Expresses a Malaria Chloroquine Resistance Mechanism upon Transfection with Mutant, but not Wild-type, Plasmodium Falciparum Transporter PfCRT
Autor: | Bronwen Naudé, Thomas E. Wellems, Joseph Brzostowski, Alan R. Kimmel |
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Jazyk: | angličtina |
Rok vydání: | 2005 |
Předmět: |
Mutant
Molecular Sequence Data Plasmodium falciparum Protozoan Proteins Gene Expression macromolecular substances Transfection Biochemistry Dictyostelium discoideum Article Antimalarials Chloroquine Piperaquine parasitic diseases Drug Resistance Bacterial medicine Animals Point Mutation Dictyostelium Amino Acid Sequence Molecular Biology Phylogeny Quinine biology fungi Cytoplasmic Vesicles Wild type Membrane Proteins Membrane Transport Proteins Cell Biology biology.organism_classification Virology Quinidine Phenotype Quinolines Efflux Acids medicine.drug |
Popis: | Chloroquine resistance in Plasmodium falciparum malaria results from mutations in PfCRT, a member of a unique family of transporters present in apicomplexan parasites and Dictyostelium discoideum. Mechanisms that have been proposed to explain chloroquine resistance are difficult to evaluate within malaria parasites. Here we report on the targeted expression of wild-type and mutant forms of PfCRT to acidic vesicles in D. discoideum. We show that wild-type PfCRT has minimal effect on the accumulation of chloroquine by D. discoideum, whereas forms of PfCRT carrying a key charge-loss mutation of lysine 76 (e.g. K76T) enable D. discoideum to expel chloroquine. As in P. falciparum, the chloroquine resistance phenotype conferred on transformed D. discoideum can be reversed by the channel-blocking agent verapamil. Although intravesicular pH levels in D. discoideum show small acidic changes with the expression of different forms of PfCRT, these changes would tend to promote intravesicular trapping of chloroquine (a weak base) and do not account for reduced drug accumulation in transformed D. discoideum. Our results instead support outward-directed chloroquine efflux for the mechanism of chloroquine resistance by mutant PfCRT. This mechanism shows structural specificity as D. discoideum transformants that expel chloroquine do not expel piperaquine, a bisquinoline analog of chloroquine used frequently against chloroquine-resistant parasites in Southeast Asia. PfCRT nevertheless may have some ability to act on quinine and quinidine. Transformed D. discoideum will be useful for further studies of the chloroquine resistance mechanism and may assist in the development and evaluation of new antimalarial drugs. |
Databáze: | OpenAIRE |
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