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DNA oxidation in Alzheimer's disease.

机译:阿尔茨海默氏病中的DNA氧化。

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Oxidative damage to DNA may play an important role in aging and neurodegenerative diseases such as Alzheimer's disease (AD). Attack on DNA by reactive oxygen species, particularly hydroxyl radicals, can lead to strand breaks, DNA-DNA and DNA-protein cross-linking, sister chromatid exchange and translocation, and formation of at least 20 oxidized base adducts. Modification of DNA bases can lead to mutation and altered protein synthesis. In late-stage AD brain, several studies have shown an elevation of the base adducts 8 hydroxyguanine (8-OHG), 8-hydroxyadenine (8-OHA), 5-hydroxycytosine (5-OHC), and 5-hydroxyuracil, a chemical degradation product of cytosine. Several studies have shown a decline in repair of 8-OHG in AD. Most recently, our studies have shown elevated 8-OHG, 8-OHA, and 5,6-diamino-5-formamidopyrimidine in nuclear and mitochondrial DNA in mild cognitive impairment, the earliest detectable form of AD, suggesting that oxidative damage to DNA is an early event in AD and not a secondary phenomenon.
机译:DNA的氧化损伤可能在衰老和神经退行性疾病(例如阿尔茨海默氏病(AD))中发挥重要作用。活性氧特别是羟基对DNA的攻击可导致链断裂,DNA-DNA和DNA-蛋白质交联,姐妹染色单体交换和易位以及形成至少20个氧化碱基加合物。 DNA碱基的修饰可导致突变和蛋白质合成的改变。在晚期AD脑中,多项研究表明,碱性加合物8羟基鸟嘌呤(8-OHG),8-羟基腺嘌呤(8-OHA),5-羟基胞嘧啶(5-OHC)和5-羟基尿嘧啶是一种化学药品胞嘧啶的降解产物。几项研究表明,AD中8-OHG的修复下降。最近,我们的研究表明,在轻度认知障碍(最早可检测到的AD形式)中,核和线粒体DNA中的8-OHG,8-OHA和5,6-二氨基-5-甲酰胺基嘧啶含量升高,这表明对DNA的氧化损伤是是AD中的早期事件,不是次要现象。

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