首页> 外文期刊>The British Journal of Nutrition >High dietary vitamin C intake reduces glucocorticoid-induced immunosuppression and measures of oxidative stress in vitamin C-deficient senescence marker protein 30 knockout mice
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High dietary vitamin C intake reduces glucocorticoid-induced immunosuppression and measures of oxidative stress in vitamin C-deficient senescence marker protein 30 knockout mice

机译:高膳食维生素C摄入量可减少糖皮质激素诱导的免疫抑制和维生素C缺陷衰弱衰老标志物蛋白30敲除小鼠的氧化胁迫措施

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摘要

Vitamin C (VC) is a vital micronutrient for humans and some other mammals and also has antioxidant activity. Stress-induced elevation of glucocorticoid production is well known to cause immunosuppression. The present study evaluated the effect of high VC intake on glucocorticoid-induced immune changes in mice. Senescence marker protein 30 knockout mice with genetic VC deficiency were fed a diet containing the recommended VC content (20 mg/kg per d; 0·02 %VC group) or a high VC content (200 mg/kg per d; 0·2 %VC group) for 2 months, then dexamethasone was given by intraperitoneal injection. After administration of dexamethasone, the plasma ascorbic acid concentration decreased significantly in the 0·02 %VC group and was unchanged in wild-type C57BL/6 mice on a VC-deficient diet (wild-type group), while it was significantly higher in the 0·2 %VC group compared with the other two groups. In the 0·02 %VC and wild-type groups, dexamethasone caused a significant decrease in the cluster of differentiation (CD)4+ and CD8+ T cells among splenocytes as well as a significant decrease in IL-2, IL-12p40 and interferon-γ protein production by splenocytes and a significant decrease in T-cell proliferation among splenocytes. In the 0·2 %VC group, these dexamethasone-induced immunosuppression improved when compared with the other two groups. In addition, reduction in the intracellular levels of ascorbic acid, superoxide dismutase and glutathione in splenocytes by dexamethasone as well as elevation in thiobarbituric acid-reactive substances were significantly suppressed in the 0·2 %VC group. These findings suggest that high dietary VC intake reduces glucocorticoid-induced T-cell dysfunction by maintaining intracellular antioxidant activity.
机译:维生素C(VC)是人类和其他一些哺乳动物的重要微量营养素,也具有抗氧化活性。应激诱导的糖皮质激素产生的升高是众所周知的,导致免疫抑制。本研究评估了高VC摄入对小鼠糖皮质激素诱导的免疫变化的影响。衰老标志物30敲除具有遗传VC缺乏的小鼠含有推荐的VC含量的饮食(每D 20mg / kg,0·02%VC组)或高VC含量(每D 200 mg / kg; 0·2 %VC组)2个月,然后通过腹膜内注射给出地塞米松。在施用地塞米松后,在0·02%VC组中,血浆抗坏血酸浓度显着下降,在缺乏缺乏饮食(野生型组)的野生型C57BL / 6小鼠中没有变化,同时它显着提高与其他两组相比,0·2%VC组。在0·02%VC和野生型组中,地塞米松在脾细胞中的分化(CD)4+和CD8 + T细胞中的显着降低以及IL-2,IL-12P40和干扰素的显着降低通过脾细胞产生-γ蛋白产生,脾细胞中T细胞增殖显着降低。在0·2%VC组中,与其他两组相比,这些地塞米松诱导的免疫抑制改善。此外,在0·2%VC组中,通过地塞米松的脾细胞中抗坏血酸,超氧化物歧化酶和谷胱甘肽的细胞内水平的降低以及硫酰脲酸反应性物质的升高。这些发现表明,通过维持细胞内抗氧化活性,高膳食VC Intrake通过维持细胞内抗氧化活性来减少糖皮质激素诱导的T细胞功能障碍。

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