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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Recycling of vitamin C from its oxidized forms by human endothelial cells
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Recycling of vitamin C from its oxidized forms by human endothelial cells

机译:人体内皮细胞从氧化形式回收维生素C

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摘要

Endothelial cells encounter oxidant stress due to their location in the vascular wall, and because they generate reactive nitrogen species. Because ascorbic acid is likely involved in the antioxidant defenses of these cells, we studied the mechanisms by which cultures of EA.hy926 endothelial cells recycle the vitamin from its oxidized forms. Cell lysates reduced the ascorbate free radical (AFR) by both NADH- and NADPH-dependent mechanisms. Most NADH-dependent AFR reduction occurred in the particulate fraction of the cells. NADPH-dependent reduction resembled that due to NADH in having a high affinity for the AFR, but was mediated largely by thioredoxin reductase. Reduction of dehydroascorbic acid (DHA) required GSH and was both direct and enzyme dependent. The latter was saturable, half-maximal at 100 μM DHA, and comparable to rates of AFR reduction. Loading cells to ascorbate concentrations of 0.3-1.6 mM generated intracellular DHA concentrations of 20-30μM, indicative of oxidant stress in culture. Whereas high-affinity AFR reduction is the initial and likely the preferred mechanism of ascorbate recycling, and DHA that accumulates during oxidant stress will be reduced by GSH-dependent mechanisms.
机译:内皮细胞由于其在血管壁中的位置,并且会产生活性氮,因此会遇到氧化应激。因为抗坏血酸可能参与了这些细胞的抗氧化防御,所以我们研究了EA.hy926内皮细胞培养物从氧化形式回收维生素的机制。细胞裂解物通过依赖NADH和NADPH的机制降低了抗坏血酸自由基(AFR)。大多数NADH依赖的AFR降低发生在细胞的颗粒部分。 NADPH依赖的还原类似于由于NADH对AFR具有高亲和力的还原,但主要由硫氧还蛋白还原酶介导。脱氢抗坏血酸(DHA)的还原需要GSH,并且直接和酶依赖性。后者是可饱和的,在100μMDHA时达到最大值的一半,与AFR降低的速度相当。加载抗坏血酸浓度为0.3-1.6 mM的细胞会产生20-30μM的细胞内DHA浓度,表明培养物中的氧化应激。高亲和力AFR降低是抗坏血酸再循环的最初且可能是首选的机制,而在氧化应激期间积累的DHA将通过GSH依赖性机制降低。

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