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Effects of acute oral administration of vitamin C on the mouse liver transcriptome.

机译:急性口服维生素C对小鼠肝脏转录组的影响。

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摘要

Vitamin C is a strong antioxidant that alters gene expression in cells, and its effects can be modified by cellular oxidative stress. We investigated the genome-wide effects of vitamin C on the in vivo transcriptome in the liver, which synthesizes various enzymes and proteins to defend against cellular oxidative stress. We fed mice vitamin C (0.056 mg/g of body weight) for 1 week and performed DNA microarray analysis with hepatic mRNA in fasting and refeeding states to mimic physiological conditions of oxidative stress. Significance analysis of microarray data identified approximately 6,000 genes differentially expressed in both fasting and refeeding states. In the fasting state, vitamin C induced overall energy metabolism as well as radical scavenging pathways. These were ameliorated in the refeeding state. These findings suggest that vitamin C has profound and immediate global effects on hepatic gene expression, which may help prevent oxidative stress, and that long-term treatment with vitamin C might reduce the risk of chronic disease.
机译:维生素C是一种强抗氧化剂,可改变细胞中的基因表达,其作用可以通过细胞氧化应激来改变。我们研究了维生素C对肝脏体内转录组的全基因组影响,肝脏合成各种酶和蛋白质以防御细胞氧化应激。我们给小鼠喂食维生素C(体重的0.056mg / g)1周,并在禁食和再喂养状态下用肝脏mRNA进行DNA微阵列分析,以模拟氧化应激的生理条件。微阵列数据的显著性分析鉴定了大约 6,000 个在禁食和再喂养状态下差异表达的基因。在禁食状态下,维生素C诱导整体能量代谢以及自由基清除途径。这些在再喂养状态下得到改善。这些发现表明,维生素C对肝脏基因表达具有深远而直接的全球影响,这可能有助于预防氧化应激,并且长期使用维生素C治疗可能会降低患慢性病的风险。

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