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IBJ-Iranian Biomedical Journal. 2013; 17 (1): 22-28
Dans Anglais | IMEMR | ID: emr-193080

Résumé

Background: oxidative modification of low-density lipoprotein [LDL] appears to be an early step in the pathogenesis of atherosclerosis. Meanwhile, myeloperoxidase [MPO]-catalyzed reaction is one of the potent pathways for LDL oxidation in vivo. The aim of this study was to evaluate in vitro antioxidant effects of vitamins C and E on LDL oxidation mediated by MPO


Methods: MPO was isolated from fresh plasma by sequential centrifugation using density ultracentrifugation. It was incubated with LDL and the LDL oxidation level was determined spectrophotometrically by measuring conjugated diene absorbance at 234 nm. Furthermore, vitamin C [50-200 mM] and vitamin E [10-40 mM] were added and the LDL oxidation level was determined


Results: the purity index of MPO and its enzymatic activity were 0.69 and 1127 U/mg protein, respectively. It was demonstrated that vitamin C in vitro inhibited LDL oxidation mediated by MPO; however, vitamin E was unable to act in the same way. The protection by vitamin C was concentration dependent and maximum protective effect of vitamin C was observed at 150 mM, where about 64% of the LDL oxidation was inhibited. Vitamin C increased lag time of LDL oxidation mediated by MPO up to 2.4 times


Conclusion: it can be concluded from our results that vitamin C is able to improve LDL resistance to oxidative modification in vitro. In addition, vitamin C might be effective in LDL oxidation mediated by MPO in vivo, resulting in reduction of atherosclerosis process rate. Iran. Biomed. J. 17 [1]: 22-28, 2013

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