In vitro radical-scavenging mechanism of melatonin and its in vivo protective effect against radiation-induced lipid peroxidation

Kailash Manda , Kei Ohkubo , Yoshimi Shoji , A. K. M. Raushan Kabir Zoardar , Masato Kamibayashi , Toshihiko Ozawa , Kazunori Anzai , Ikuo Nakanishi
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引用次数: 1

Abstract

Melatonin (N-acetyl-5-methoxytryptamine, MLT), an evolutionarily conserved indoleamine, is known to act as an antioxidant. However, the evidence indicating the role of MLT as a powerful chain-breaking antioxidant by scavenging peroxyl radical remains controversial. The radical-scavenging rate of MLT determined in this study in methanol using galvinoxyl radical (GO) was much lower than that of an α-tocopherol model compound. The acceleration of the GO-scavenging reaction by MLT was observed in the presence of magnesium ion (Mg2+), a bio-related redox-inactive metal ion, suggesting that this reaction may proceed via a rate-determining electron transfer followed by proton transfer. The coordination of Mg2+ to the carbonyl oxygen in the one-electron reduced species of GO (GO) may stabilize the product, resulting in the acceleration of the electron-transfer process. We also demonstrated that prophylactically administrated MLT efficiently inhibited the lipid peroxide-derived protein modification, which can be detected by a sensitive marker, Nε-(hexanoyl)lysine adduct, in the plasma of X-irradiated mice. The relatively weak GO-scavenging activity of MLT suggests that the ameliorative effect of MLT against in vivo lipid peroxidation does not result from the direct scavenging of lipid peroxyl radicals by MLT. Therefore, the observed superior protective efficiency of MLT against in vivo lipid peroxidation may partly support the earlier studies, which reported the synergistic antioxidative effect of the metabolites of MLT.

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褪黑素的体外自由基清除机制及其对辐射诱导的脂质过氧化的体内保护作用
褪黑激素(N-乙酰基-5-甲氧基色胺,MLT)是一种进化上保守的吲哚胺,已知具有抗氧化剂的作用。然而,有证据表明MLT作为一种强大的破链抗氧化剂通过清除过氧自由基的作用仍然存在争议。本研究中使用甲氧基自由基(GO•)在甲醇中测定的MLT的自由基清除率远低于α-生育酚模型化合物。在镁离子(Mg2+)存在的情况下,观察到MLT对GO•-清除反应的加速,镁离子是一种生物相关的氧化还原非活性金属离子,这表明该反应可能通过决定速率的电子转移和质子转移进行。在单电子还原的GO•(GO–)物种中,Mg2+与羰基氧的配位可以稳定产物,从而加速电子转移过程。我们还证明,预防性给药MLT有效地抑制了脂质过氧化物衍生的蛋白质修饰,这可以通过敏感标记物Nε-(己酰基)赖氨酸加合物在X射线照射小鼠的血浆中检测到。MLT相对较弱的GO•-清除活性表明,MLT对体内脂质过氧化的改善作用不是由MLT直接清除脂质过氧自由基引起的。因此,观察到的MLT对体内脂质过氧化的卓越保护作用可能部分支持早期的研究,这些研究报道了MLT代谢产物的协同抗氧化作用。
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