Inhibition of the iron-catalysed formation of hydroxyl radicals by nitrosouracil derivatives: protection of mitochondrial membranes against lipid peroxidation.

A Rabion, J B Verlhac, L Fraisse, B Roche, J L Seris
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Abstract

A new series of metal ligands containing the 1,3-dimethyl-6-amino-5- nitrosouracil moiety has been synthesized and they have been studied as potential inhibitors of iron-dependent lipid peroxidation. For this purpose, these new derivatives have been tested in the Fenton induced deoxyribose degradation assay, which allows a quantitative measurement of their inhibitory effect towards hydroxyl radical generation. When iron(II) is complexed by these ligands, a strong inhibition of deoxyribose degradation is observed, especially in the case of tris-[2-(1,3-dimethyl-5-nitrosouracil-6-yl)aminoethyl] amine (5). This inhibitory effect is clearly related to a specific complexation of iron(II) and is not due to the direct scavenging of hydroxyl radical by the ligand. Inhibition of the iron mediated Fenton reaction presumably results from inactivation of the reactivity of the metal center towards hydrogen peroxide. These derivatives, as well as long alkyl chain substituted nitrosouracils were evaluated in the protection of biological membranes against lipid peroxidation (induced by iron(II)/dihydroxyfumaric acid and determined with the 2-thiobarbituric acid test). Ligand 5 inhibited lipid peroxidation at a rate similar to Desferal (desferrioxamine B) and slightly higher than bathophenanthroline sulphonate (BPS), which are respectively good iron(III) and iron(II) chelators. When covalently bound with a long alkyl chain, the increase of lipophilic character of the ligand allows its location near the mitochondrial membrane, where lipid peroxidation occurs. Lower concentrations (IC50 = 4 microM) are then necessary to inhibit lipid peroxidation. This IC50 concentration should be compared to those obtained for Trolox (IC50 = 3 microM) or the 21-aminosteroid U74500A (IC50 = 1 microM) described previously.

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亚硝基酸衍生物对铁催化羟基自由基形成的抑制:线粒体膜抗脂质过氧化的保护。
合成了一系列新的含有1,3-二甲基-6-氨基-5-硝基酸的金属配体,并研究了它们作为铁依赖性脂质过氧化的潜在抑制剂。为此,这些新的衍生物已经在芬顿诱导脱氧核糖降解试验中进行了测试,该试验可以定量测量它们对羟基自由基产生的抑制作用。当铁(II)与这些配体络合时,观察到对脱氧核糖降解的强烈抑制,特别是在三-[2-(1,3-二甲基-5-硝基-6-基)氨基乙基]胺的情况下(5)。这种抑制作用显然与铁(II)的特定络合有关,而不是由于配体直接清除羟基自由基。铁介导的芬顿反应的抑制可能是由于金属中心对过氧化氢的反应活性失活。这些衍生物,以及长烷基链取代的硝基脲对生物膜抗脂质过氧化的保护作用进行了评估(由铁(II)/二羟基富马酸诱导,并通过2-硫代巴比妥酸试验确定)。配体5抑制脂质过氧化的速率与去铁胺B(去铁胺B)相似,略高于邻菲罗啉磺酸盐(BPS),它们分别是良好的铁(III)和铁(II)螯合剂。当与长烷基链共价结合时,配体亲脂性的增加允许其靠近线粒体膜,在那里脂质过氧化发生。较低浓度(IC50 = 4微米)则需要抑制脂质过氧化。该IC50浓度应与先前描述的Trolox (IC50 = 3微米)或21-氨基类固醇U74500A (IC50 = 1微米)的IC50浓度进行比较。
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