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首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Increased Nrf2 activation in livers from Keap1-knockdown mice increases expression of cytoprotective genes that detoxify electrophiles more than those that detoxify reactive oxygen species.
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Increased Nrf2 activation in livers from Keap1-knockdown mice increases expression of cytoprotective genes that detoxify electrophiles more than those that detoxify reactive oxygen species.

机译:Keap1-nockdown小鼠肝脏中Nrf2活化的增加,使排毒亲电的细胞保护基因的表达增加,而使对活性氧排毒的细胞保护基因的表达增加。

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摘要

Nuclear factor erythroid 2-related factor 2 (Nrf2) is a transcription factor critical for protection against electrophilic and oxidative stress. In a recently engineered mouse with knockdown of kelch-like ECH associated protein 1 (Keap1-kd mice), the cytosolic repressor of Nrf2, there is a 55% decrease in Keap1 mRNA and a 200% increase in Nrf2 protein in liver. Experiments with Nrf2-null mice have demonstrated the effects of a lack of Nrf2. However, little is known about the biological effects of more Nrf2 activation. Accordingly, the hepatic phenotype of Keap1-kd mice, as well as the hepatic mRNA expression of cytoprotective genes were compared among wild-type, Nrf2-null, and Keap1-kd mice. Three distinct patterns of hepatic gene expression were identified among wild-type, Nrf2-null, and Keap1-kd mice. The first pattern encompassed genes that were lower in Nrf2-null mice and considerably higher in Keap1-kd mice than wild-type mice, which included genes mainly responsible for the detoxification and elimination of electrophiles, such as NAD(P)H:quinone oxidoreductase 1 and glutathione-S-transferases (Gst), and multidrug resistance-associated proteins. The second pattern encompassed genes that were lower in Nrf2-null mice but not increased in Keap1-kd mice, and included genes, such as epoxide hydrolase-1, UDP-glucuronosyltransferases, aldehyde dehydrogenases, as well as genes important in the detoxification of reactive oxygen species, such as superoxide dismutase 1 and 2, catalase, and peroxiredoxin 1. The third pattern encompassed genes that were not different among wild-type, Nrf2-null, and Keap1-kd mice and included genes such as glutathione peroxidase, microsomal Gsts, and uptake transporters. In conclusion, the present study suggests that increased activation of hepatic Nrf2 is more important for the detoxification and elimination of electrophiles than reactive oxygen species.
机译:核因子类胡萝卜素2相关因子2(Nrf2)是转录因子,对于保护亲电子和氧化应激至关重要。在最近工程化的小鼠中,Nelf2的胞质阻遏物抑制了海藻样ECH相关蛋白1(Keap1-kd小鼠),肝脏中Keap1 mRNA减少了55%,Nrf2蛋白增加了200%。 Nrf2无效小鼠的实验证明了缺少Nrf2的影响。但是,人们对更多Nrf2激活的生物学效应知之甚少。因此,比较了野生型,Nrf2-null和Keap1-kd小鼠的Keap1-kd小鼠的肝表型以及细胞保护基因的肝mRNA表达。在野生型,Nrf2-null和Keap1-kd小鼠中鉴定出三种不同的肝基因表达模式。第一种模式包含的基因在Nrf2空小鼠中较低,而在Keap1-kd小鼠中则比野生型小鼠高,其中包括主要负责亲电子的解毒和消除的基因,例如NAD(P)H:醌氧化还原酶1和谷胱甘肽S转移酶(Gst),以及与多药耐药性相关的蛋白质。第二种模式包括在Nrf2-null小鼠中较低的基因,但在Keap1-kd小鼠中未增加的基因,包括基因,例如环氧化物水解酶-1,UDP-葡糖醛酸糖基转移酶,醛脱氢酶以及对反应性排毒重要的基因。氧物种,例如超氧化物歧化酶1和2,过氧化氢酶和过氧化物酶1。第三种模式包括野生型,Nrf2-null和Keap1-kd小鼠之间无差异的基因,包括谷胱甘肽过氧化物酶,微粒体Gsts ,并吸收转运蛋白。总而言之,本研究表明,肝Nrf2的活化增强对亲电子的排毒和消除比活性氧更为重要。

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