期刊
JOURNAL OF INFECTIOUS DISEASES
卷 208, 期 3, 页码 468-478出版社
OXFORD UNIV PRESS INC
DOI: 10.1093/infdis/jit171
关键词
Artemisinins; PfATP6; yeast; malaria; Plasmodium falciparum; drug resistance; thaperoxides; cyclopiazonic acid; desferioxamine
资金
- EU FP7 Marie Curie-funded Initial Training Network InterMal [215281-2]
- EU-FP7 MALSIG programme
- European Union Seventh Framework Programme [304948 - NANOMAL]
- MRC [MR/K011782/1, G0900109] Funding Source: UKRI
- Medical Research Council [MR/K011782/1, G0900109] Funding Source: researchfish
Background. The mechanism of action of artemisinins against malaria is unclear, despite their widespread use in combination therapies and the emergence of resistance. Results. Here, we report expression of PfATP6 (a SERCA pump) in yeast and demonstrate its inhibition by artemisinins. Mutations in PfATP6 identified in field isolates (such as S769N) and in laboratory clones (such as L263E) decrease susceptibility to artemisinins, whereas they increase susceptibility to unrelated inhibitors such as cyclopiazonic acid. As predicted from the yeast model, Plasmodium falciparum with the L263E mutation is also more susceptible to cyclopiazonic acid. An inability to knockout parasite SERCA pumps provides genetic evidence that they are essential in asexual stages of development. Thaperoxides are a new class of potent antimalarial designed to act by inhibiting PfATP6. Results in yeast confirm this inhibition. Conclusions. The identification of inhibitors effective against mutated PfATP6 suggests ways in which artemisinin resistance may be overcome.
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