Superoxide and hydrogen peroxide production and NADPH oxidation stimulated by nitrofurantoin in lung microsomes: possible implications for toxicity. |
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Authors: | H A Sasame M R Boyd |
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Affiliation: | Laboratory of Chemical Pharmacology, National Heart, Lung and Blood Institute, and Clinical Pharmacology Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20014 USA |
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Abstract: | The addition of nitrofurantoin to aerobic incubation mixtures containing rat lung microsomes strongly enhanced the generation of adrenochrome from epinephrine. Adrenochrome formation in this system was blocked by superoxide dismutase, but not by catalase. Hydrogen peroxide production was also strongly enhanced by nitrofurantoin in these preparations; superoxide dismutase did not significantly alter the amount of H2O2 measured, but no H2O2 was detected in incubation mixtures in the presence of catalase. Nitrofurantoin enhanced the oxidation of NADPH in lung microsomal suspensions under aerobic conditions; the enhancement was unaffected by catalase but was partially prevented by superoxide dismutase. Neither adrenochrome formation nor H2O2 production were enhanced by nitrofurantoin under anaerobic (N2) conditions, but NADPH oxidation in the presence of nitrofurantoin was greater under anaerobic conditions than under aerobic conditions. These results are consistent with the view that the redox cycling of nitrofurantoin in lung microsomes in the presence of oxygen results in the consumption of NADPH and the production of activated oxygen species, emphasizing some metabolic similarities with the lung-toxic herbicide, paraquat. |
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Keywords: | Inquiries and requests for reprints should be addressed Dr. M.R. Boyd Bldg. 10 Rm. 6N-105 National Cancer Institute Bethesda Md. 20014 USA |
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