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2
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3
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DT-diaphorase-catalysed reduction of 1,4-naphthoquinone derivatives and glutathionyl-quinone conjugates. Effect of substituents on autoxidation rates.DT-黄递酶催化的1,4-萘醌衍生物和谷胱甘肽基醌共轭物的还原反应。取代基对自氧化速率的影响。
Biochem J. 1989 Jan 15;257(2):561-71. doi: 10.1042/bj2570561.
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本文引用的文献

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A thermodynamic appraisal of the radical sink hypothesis.自由基阱假说的热力学评估。
Free Radic Biol Med. 1993 Jan;14(1):91-4. doi: 10.1016/0891-5849(93)90513-t.
2
Superoxide as an intracellular radical sink.超氧化物作为细胞内的自由基汇聚池。
Free Radic Biol Med. 1993 Jan;14(1):85-90. doi: 10.1016/0891-5849(93)90512-s.
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DNA-ferrous iron catalyzed hydroxyl free radical formation from hydrogen peroxide.DNA-亚铁离子催化过氧化氢形成羟基自由基。
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4
2- and 6-methyl-1,4-naphthoquinone derivatives and potential bioreductive alkylating agents.2-和6-甲基-1,4-萘醌衍生物及潜在的生物还原烷基化剂。
J Med Chem. 1982 Jun;25(6):730-5. doi: 10.1021/jm00348a023.
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Chemical mutagenesis.化学诱变
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Catecholamine toxicity: a proposal for the molecular pathogenesis of manganese neurotoxicity and Parkinson's disease.儿茶酚胺毒性:锰神经毒性和帕金森病分子发病机制的一种假说
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Superoxide-dependent formation of hydroxyl radicals in the presence of iron salts is a feasible source of hydroxy radicals in vivo.在铁盐存在的情况下,超氧化物依赖性羟基自由基的形成是体内羟基自由基的一个可行来源。
Biochem J. 1982 Aug 1;205(2):461-3. doi: 10.1042/bj2050461.
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Cytochrome c reduction by semiquinone radicals can be indirectly inhibited by superoxide dismutase.超氧化物歧化酶可间接抑制半醌自由基对细胞色素c的还原作用。
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Spin trapping of superoxide and hydroxyl radical: practical aspects.超氧阴离子和羟基自由基的自旋捕获:实际应用
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10
The metabolism of menadione (2-methyl-1,4-naphthoquinone) by isolated hepatocytes. A study of the implications of oxidative stress in intact cells.分离的肝细胞对维生素K3(2-甲基-1,4-萘醌)的代谢。完整细胞中氧化应激影响的研究。
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2-甲基-1,4-萘醌生物还原烷基化剂的单电子和双电子还原:动力学研究、自由基产生、硫醇氧化及DNA链断裂形成

One- and two-electron reduction of 2-methyl-1,4-naphthoquinone bioreductive alkylating agents: kinetic studies, free-radical production, thiol oxidation and DNA-strand-break formation.

作者信息

Giulivi C, Cadenas E

机构信息

Department of Molecular Pharmacology and Toxicology, University of Southern California, Los Angeles 90033.

出版信息

Biochem J. 1994 Jul 1;301 ( Pt 1)(Pt 1):21-30. doi: 10.1042/bj3010021.

DOI:10.1042/bj3010021
PMID:8037673
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1137137/
Abstract

The one- and two-electron enzymic reduction of the bioreductive alkylating agents 2-methylmethoxynaphthoquinone (quinone I) and 2-chloromethylnaphthoquinone (quinone II) was studied with purified NADPH-cytochrome P-450 reductase and DT-diaphorase respectively, and characterized in terms of kinetic constants, oxyradical production, thiol oxidation and DNA-strand-break formation. The catalytic-centre activity values indicated that DT-diaphorase catalysed the reduction of quinone I far more efficiently than NADPH-cytochrome P-450 reductase, although the Km values of the two enzymes for this quinone were similar (1.2-3.0 microM). The one-electron-transfer flavoenzyme also catalysed the reduction of quinone II, but the behaviour of DT-diaphorase towards this quinone did not permit calculation of kinetic constants. A salient feature of the redox transitions caused by the one- and two-electron catalysis of these quinones was the different contributions of disproportionation and autoxidation reactions respectively. In the former case, about 26% of NADPH consumed was accounted for in terms of autoxidation (as H2O2 formation), whereas in the latter, the autoxidation component accounted for most (98%) of the NADPH consumed. This difference was abrogated by superoxide dismutase, which enhanced autoxidation during NADPH-cytochrome P-450 catalysis to a maximal value. E.s.r. analysis indicated the formation of superoxide radicals, the signal of which was suppressed by superoxide dismutase and unaffected by catalase. The one- and two-electron reduction of these quinones in the presence of GSH was accompanied by formation of thiyl radicals. Although superoxide dismutase suppressed the thiol radical e.s.r. signal in both instances, the enzyme enhanced GSSG accumulation during NADPH-cytochrome P-450 catalysis of quinone I, whereas it inhibited GSSG formation during reduction of the quinone by DT-diaphorase. One- and two-electron reduction of quinone I led to calf thymus DNA-strand-break formation, a process that (a) was substantially decreased in experiments performed with dialysed DNA and in the presence of desferal and (b) was partially sensitive to superoxide dismutase and/or catalase. These findings are rationalized in terms of the occurrence of metal ions ligated to DNA, protecting against the toxic effects of superoxide radicals generated during enzymic reduction of quinones.

摘要

分别用纯化的NADPH - 细胞色素P - 450还原酶和DT - 黄递酶研究了生物还原烷基化剂2 - 甲基甲氧基萘醌(醌I)和2 - 氯甲基萘醌(醌II)的单电子和双电子酶促还原反应,并从动力学常数、氧自由基产生、硫醇氧化和DNA链断裂形成等方面进行了表征。催化中心活性值表明,尽管两种酶对该醌的Km值相似(1.2 - 3.0 microM),但DT - 黄递酶催化醌I的还原效率远高于NADPH - 细胞色素P - 450还原酶。单电子转移黄素酶也催化醌II的还原,但DT - 黄递酶对该醌的反应无法计算动力学常数。这些醌的单电子和双电子催化引起的氧化还原转变的一个显著特征是歧化反应和自氧化反应分别有不同的贡献。在前一种情况下,约26%消耗的NADPH可归因于自氧化(以H2O2形成计),而在后一种情况下,自氧化成分占消耗的NADPH的大部分(98%)。超氧化物歧化酶消除了这种差异,它在NADPH - 细胞色素P - 450催化过程中将自氧化增强到最大值。电子顺磁共振分析表明形成了超氧自由基,其信号被超氧化物歧化酶抑制,而过氧化氢酶对其无影响。在谷胱甘肽存在下,这些醌的单电子和双电子还原伴随着硫自由基的形成。尽管超氧化物歧化酶在两种情况下都抑制了硫自由基的电子顺磁共振信号,但该酶在醌I的NADPH - 细胞色素P - 450催化过程中增强了谷胱甘肽二硫化物的积累,而在DT - 黄递酶还原醌的过程中抑制了谷胱甘肽二硫化物的形成。醌I的单电子和双电子还原导致小牛胸腺DNA链断裂的形成,这一过程(a)在用透析过的DNA进行的实验中和在去铁胺存在下显著减少,并且(b)对超氧化物歧化酶和/或过氧化氢酶部分敏感。这些发现可以根据与DNA结合的金属离子的存在来解释,这些金属离子可防止醌的酶促还原过程中产生的超氧自由基的毒性作用。