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Preservation of biological function despite oxidative modification of the apolipoprotein A-I mimetic peptide 4F

机译:尽管载脂蛋白A-I模拟肽4F进行了氧化修饰但仍保留了生物学功能

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摘要

Myeloperoxidase (MPO)-derived hypochlorous acid induces changes in HDL function via redox modifications at the level of apolipoprotein A-I (apoA-I). As 4F and apoA-I share structural and functional properties, we tested the hypothesis that 4F acts as a reactive substrate for hypochlorous acid (HOCl). 4F reduced the HOCl-mediated oxidation of the fluorescent substrate APF in a concentration-dependent manner (ED50 ∼ 56 ± 3 μM). This reaction induced changes in the physical properties of 4F. Addition of HOCl to 4F at molar ratios ranging from 1:1 to 3:1 reduced 4F band intensity on SDS-PAGE gels and was accompanied by the formation of a higher molecular weight species. Chromatographic studies showed a reduction in 4F peak area with increasing HOCl and the formation of new products. Mass spectral analyses of collected fractions revealed oxidation of the sole tryptophan (Trp) residue in 4F. 4F was equally susceptible to oxidation in the lipid-free and lipid-bound states. To determine whether Trp oxidation influenced its apoA-I mimetic properties, we monitored effects of HOCl on 4F-mediated lipid binding and ABCA1-dependent cholesterol efflux. Neither property was altered by HOCl. These results suggest that 4F serves as a reactive substrate for HOCl, an antioxidant response that does not influence the lipid binding and cholesterol effluxing capacities of the peptide.
机译:髓过氧化物酶(MPO)衍生的次氯酸通过载脂蛋白A-I(apoA-I)的氧化还原修饰诱导HDL功能的改变。由于4F和apoA-I共享结构和功能特性,因此我们检验了4F充当次氯酸(HOCl)的反应性底物的假设。 4F以浓度依赖的方式(ED50〜56±3μM)减少了HOCl介导的荧光底物APF的氧化。该反应引起4F物理性质的变化。在1:1至3:1的摩尔比范围内向4F添加HOCl会降低SDS-PAGE凝胶上的4F带强度,并伴随着更高分子量物种的形成。色谱研究表明,随着HOCl的增加和新产物的形成,4F峰面积减小。收集的馏分的质谱分析揭示了4F中唯一的色氨酸(Trp)残留物的氧化。 4F在无脂质和脂质结合状态下同样容易受到氧化。为了确定Trp氧化是否影响其apoA-I模拟物性能,我们监测了HOCl对4F介导的脂质结合和ABCA1依赖性胆固醇外排的影响。 HOCl均未更改这两个属性。这些结果表明4F充当HOCl的反应性底物,HOCl是一种抗氧化剂反应,其不影响肽的脂质结合和胆固醇外排能力。

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