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人体血浆中的抗氧化防御与脂质过氧化

Antioxidant defenses and lipid peroxidation in human blood plasma.

作者信息

Frei B, Stocker R, Ames B N

机构信息

Department of Biochemistry, University of California, Berkeley 94720.

出版信息

Proc Natl Acad Sci U S A. 1988 Dec;85(24):9748-52. doi: 10.1073/pnas.85.24.9748.

Abstract

The temporal disappearance in human blood plasma of endogenous antioxidants in relation to the appearance of various classes of lipid hydroperoxides measured by HPLC postcolumn chemiluminescence detection has been investigated under two types of oxidizing conditions. Exposure of plasma to aqueous peroxyl radicals generated at a constant rate leads immediately to oxidation of endogenous ascorbate and sulfhydryl groups, followed by sequential depletion of bilirubin, urate, and alpha-tocopherol. Stimulating polymorphonuclear leukocytes in plasma initiates very rapid oxidation of ascorbate, followed by partial depletion of urate. Once ascorbate is consumed completely, micromolar concentrations of hydroperoxides of plasma phospholipids, triglycerides, and cholesterol esters appear simultaneously, even though sulfhydryl groups, bilirubin, urate, and alpha-tocopherol are still present at high concentrations. Nonesterified fatty acids, the only lipid class in plasma not transported in lipoproteins but bound to albumin, are preserved from peroxidative damage even after complete oxidation of ascorbate, most likely due to site-specific antioxidant protection by albumin-bound bilirubin and possibly by albumin itself. Thus, in plasma ascorbate and, in a site-specific manner, bilirubin appear to be much more effective in protecting lipids from peroxidative damage by aqueous oxidants than all the other endogenous antioxidants. Hydroperoxides of linoleic acid, phosphatidylcholine, and cholesterol added to plasma in the absence of added reducing substrates are degraded, in contrast to hydroperoxides of trilinolein and cholesterol linoleate. These findings indicate the presence of a selective peroxidase activity operative under physiological conditions. Our data suggest that in states of leukocyte activation and other types of acute or chronic oxidative stress such a simple regimen as controlled ascorbate supplementation could prove helpful in preventing formation of lipid hydroperoxides, some of which cannot be detoxified by endogenous plasma activities and thus might cause damage to critical targets.

摘要

在两种氧化条件下,研究了通过高效液相色谱柱后化学发光检测法测定的内源性抗氧化剂在人血浆中的暂时消失与各类脂质氢过氧化物出现之间的关系。将血浆暴露于以恒定速率产生的水相过氧自由基中,会立即导致内源性抗坏血酸和巯基氧化,随后胆红素、尿酸盐和α-生育酚依次耗尽。刺激血浆中的多形核白细胞会引发抗坏血酸的快速氧化,随后尿酸盐部分耗尽。一旦抗坏血酸完全消耗,血浆磷脂、甘油三酯和胆固醇酯的微摩尔浓度的氢过氧化物会同时出现,尽管巯基、胆红素、尿酸盐和α-生育酚仍以高浓度存在。非酯化脂肪酸是血浆中唯一不通过脂蛋白运输而是与白蛋白结合的脂质类别,即使在抗坏血酸完全氧化后仍能免受过氧化损伤,这很可能是由于白蛋白结合的胆红素以及可能是白蛋白本身提供的位点特异性抗氧化保护。因此,在血浆中,抗坏血酸以及以位点特异性方式存在的胆红素,在保护脂质免受水相氧化剂的过氧化损伤方面,似乎比所有其他内源性抗氧化剂更有效。与三油精和胆固醇亚油酸酯的氢过氧化物不同,在没有添加还原底物的情况下添加到血浆中的亚油酸、磷脂酰胆碱和胆固醇的氢过氧化物会被降解。这些发现表明在生理条件下存在一种选择性过氧化物酶活性。我们的数据表明,在白细胞活化以及其他类型的急性或慢性氧化应激状态下,像控制抗坏血酸补充这样简单的方案可能有助于预防脂质氢过氧化物的形成,其中一些脂质氢过氧化物无法通过内源性血浆活性解毒,因此可能会对关键靶点造成损害。

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Antioxidant defenses and lipid peroxidation in human blood plasma.人体血浆中的抗氧化防御与脂质过氧化
Proc Natl Acad Sci U S A. 1988 Dec;85(24):9748-52. doi: 10.1073/pnas.85.24.9748.

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