Glutathione stability and oxidative stress in P. falciparum infection in vitro: Responses of normal and G6PD deficient cells |
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| Authors: | Eugene F. Roth Carmen Raventos-Suarez Margaret Perkins Ronald L. Nagel |
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| Affiliation: | 1. Mount Sinai School of Medicine, Department of Medicine, Polly Annenberg Levee Hematology Center, One Gustave L. Levy Place, New York City 10029 USA;2. Albert Einstein College of Medicine, Division of Experimental Hematology, Department of Medicine, Bronx, New York 10461 USA;3. Rockefeller University, 1230 York Avenue, New York City 10021 USA |
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| Abstract: | Red cell oxidative stress in P. falciparum infection in vitro was investigated in relation to the G6PD-Malaria hypothesis. Glutathione stability was enhanced in infected red cells; glucose consumption and pentose pathway activity were not different in normal and G6PD deficient cells, although parasite growth was impaired in G6PD deficiency. Evidence for a response to oxidative stress was not found. Infected red cells have glutamate dehydrogenase activity which was not found in uninfected cells. This enzyme provides a separate pathway for the generation of NADPH independent from the pentose shunt. The data suggest that a significant oxidative stress is not present in falciparum malaria and that another mechanism may be operative in G6PD deficiency. |
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