首页> 外文期刊>Free radical research >Contribution of haemoglobin and membrane constituents modification to human erythrocyte damage promoted by peroxyl radicals of different charge and hydrophobicity.
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Contribution of haemoglobin and membrane constituents modification to human erythrocyte damage promoted by peroxyl radicals of different charge and hydrophobicity.

机译:血红蛋白和膜成分修饰对不同电荷和疏水性的过氧自由基促进的人红细胞损害的贡献。

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摘要

We have investigated the influence of the free radical initiator characteristics on red blood cell lipid peroxidation, membrane protein modification, and haemoglobin oxidation. 2,2'-Azobis(2-amidinopropane) (AAPH) and 4,4'-azobis(4-cyanovaleric acid) (ACV) were employed as free radical sources. Both azo-compounds are water-soluble, although ACV presents a lowed hydrophilicity, evaluated from octanol/water partition constants. At physiological pH, they are a di-cation and a di-anion, respectively. AAPH and ACV readily oxidise purified oxyhemoglobin in a very efficient free radical-mediated process, particularly for ACV-derived radicals, where nearly one heme moiety was modified per radical introduced into the system, suggesting that negatively charged radicals react preferentially at the heme group. The radicals derived from both azo-compounds lead to different oxidation products. Methemoglobin, hemichromes and choleglobin were produced in AAPH-promoted hemoglobin oxidation, while ACV-derived radicals predominantly form hemichromes, with very low production of choleglobin. Red cell damage was evaluated at the level of hemoglobin and membrane constituents modification, and was expressed in terms of free radical doses. Before the onset of the lytic process, ACV leads to more lipid peroxidation than AAPH, and induces a moderate oxidation of intracellular Hb. This intracellular oxidation is markedly increased if ACV hydrophilicity is decreased by lowering the pH. On the other hand, AAPH-derived radicals are considerable more efficient in promoting protein band 3 modification and cell lysis, without significant intracellular hemoglobin oxidation. These results show that the lytic process is not triggered by lipid peroxidation or hemichrome formation, and suggest that membrane protein modification is the relevant factor leading to red blood cell lysis.
机译:我们已经研究了自由基引发剂特性对红细胞脂质过氧化,膜蛋白修饰和血红蛋白氧化的影响。 2,2'-偶氮二(2-ami基丙烷)(AAPH)和4,4'-偶氮二(4-氰基戊酸)(ACV)被用作自由基源。两种偶氮化合物都是水溶性的,尽管从辛醇/水分配常数评估,ACV的亲水性较低。在生理pH下,它们分别是二阳离子和二阴离子。 AAPH和ACV可以在非常有效的自由基介导的过程中轻易氧化纯化的氧合血红蛋白,特别是对于ACV衍生的自由基而言,引入系统的每个自由基几乎修饰了一个血红素部分,表明带负电荷的自由基优先在血红素基团上反应。由两种偶氮化合物衍生的自由基会导致不同的氧化产物。在AAPH促进的血红蛋白氧化过程中会产生高铁血红蛋白,半色素和胆红素,而ACV衍生的自由基主要形成半色素,而胆红素的产生率很低。在血红蛋白和膜成分修饰水平上评估红细胞损伤,并以自由基剂量表示。在裂解过程开始之前,ACV比AAPH导致更多的脂质过氧化,并诱导细胞内Hb的中等氧化。如果通过降低pH值降低ACV亲水性,则这种细胞内氧化作用会显着增加。另一方面,在没有明显的细胞内血红蛋白氧化的情况下,AAPH衍生的基团在促进蛋白带3修饰和细胞裂解方面更为有效。这些结果表明裂解过程不是由脂质过氧化或半色素形成触发的,并且表明膜蛋白修饰是导致红细胞裂解的相关因素。

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