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Oxidation by DNA Charge Transport Damages Conserved Sequence Block II, a Regulatory Element in Mitochondrial DNA

机译:DNA电荷运输的氧化破坏保守的序列块II,线粒体DNA中的调节元件。

摘要

Sites of oxidative damage in mitochondrial DNA have been identified on the basis of DNA-mediated charge transport. Our goal is to understand which sites in mitochondrial DNA are prone to oxidation at long range and whether such oxidative damage correlates with cancerous transformation. Here we show that a primer extension reaction can be used to monitor directly oxidative damage to authentic mitochondrial DNA through photoreactions with a rhodium intercalator. The complex [Rh(phi)_2bpy]Cl_3 (phi = 9,10-phenanthrenequinone diimine) binds to DNA without sequence specificity and, upon photoactivation, either promotes strand breaks directly at the binding site or promotes one-electron oxidative damage; comparing the sites of base oxidation to direct strand breaks reveals the oxidative damage that arises from a distance through DNA-mediated charge transport. Significantly, base oxidation by charge transport overlaps with known mutational hot spots associated with cancers at nucleotides surrounding positions 263 and 303; the latter is known as conserved sequence block II and is vital to DNA replication. Since DNA base oxidation at conserved sequence block II should weaken the ability of damaged mitochondrial genomes to be replicated, DNA-mediated charge transport may provide a protection mechanism for excluding damaged DNA.
机译:线粒体DNA氧化损伤的站点已被确定基于DNA介导的电荷运输。我们的目标是了解线粒体DNA中的哪些位点易于长距离氧化,以及这种氧化损伤是否与癌变相关。在这里,我们表明引物延伸反应可用于通过铑嵌入剂的光反应直接监测对真实线粒体DNA的氧化损伤。复杂的[Rh(phi)_2bpy] Cl_3(phi = 9,10-菲醌二亚胺)与DNA结合而没有序列特异性,并且在光激活后,要么直接在结合位点促进链断裂,要么促进单电子氧化损伤。比较碱基氧化位点与直接链断裂的位点,揭示了通过DNA介导的电荷传输距离产生的氧化损伤。值得注意的是,通过电荷传输进行的碱基氧化与已知的与癌症相关的突变热点重叠在位置263和303周围的核苷酸上。后者被称为保守序列区II,对DNA复制至关重要。由于保守序列区II处的DNA碱基氧化会削弱受损的线粒体基因组复制的能力,因此DNA介导的电荷传输可能提供排除受损DNA的保护机制。

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