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首页> 外文期刊>Free radical research >A method to produce fully characterized ubiquitin covalently modified by 4-hydroxy-nonenal, glyoxal, methylglyoxal, and malondialdehyde
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A method to produce fully characterized ubiquitin covalently modified by 4-hydroxy-nonenal, glyoxal, methylglyoxal, and malondialdehyde

机译:通过4-羟基 - 壬醇,乙二醛,甲基乙二醛和丙二醛共价改性生产完全表征泛素的方法

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Reactive carbonyl species (RCS) and the corresponding protein adducts (advanced glycoxidation or lipoxidation end products, i.e. AGEs and ALEs) are now widely studied from different points of view, since they can be considered as biomarkers, pathogenic factors, toxic mediators and drug targets. One of the main limits of the research in this field is the lack of standardized and fully characterized AGEs and ALEs to be used for biological, toxicological, and analytical studies. In this work, we set up a procedure to prepare and fully characterize a set of AGEs and ALEs by incubating ubiquitin - a model protein selected as target for carbonylation - with four different RCS: 4-hydroxy-trans-2-nonenal (HNE), methylglyoxal (MGO), glyoxal (GO), and malondialdehyde (MDA). After 24h of incubation, the extent of protein carbonylation was estimated using a recently developed quantitative strategy based on high-resolution mass spectrometry. The resulting AGEs and ALEs were fully characterized by both intact protein and bottom-up analyses in terms of: stoichiometry of the total amount of modified protein, elucidation of the structure of the RCS-deriving adducts, and localization of the RCS-modified amino acids. Each RCS exhibited different reactivity toward ubiquitin, as detected by quantifying the extent of protein modification. The order of reactivity was MGO>GO>HNE>MDA. A variety of reaction products was identified and mapped on lysine, arginine, and histidine residues of the protein. In summary, a highly standardized and reproducible method to prepare fully characterized AGEs/ALEs is here presented.
机译:现在广泛地研究了反应性羰基物种(RCS)和相应的蛋白质加合物(高糖氧化或富氧化末端产物,即年龄和ales),因为它们可以被视为生物标志物,致病因素,有毒介质和药物靶标。该领域研究的主要限制之一是缺乏用于生物,毒理学和分析研究的标准化和完全表征的年龄和ALES。在这项工作中,我们通过孵育泛素 - 选择作为羰基化靶标的模型蛋白质制备和完全表征一组年龄和铝的程序 - 用四种不同的RCS:4-羟基-Trans-2-Nonenal(HNE) ,甲基乙二醛(MgO),乙醛(GO)和丙二醛(MDA)。孵育24小时后,使用基于高分辨率质谱法的最近显影的定量策略估计蛋白质羰基化程度。由此产生的年龄和啤酒均通过完整的蛋白质和自下而上的分析来完全表征:修饰蛋白质总量的化学计量,阐明了RCS-导出的加合物的结构,以及RCS改性氨基酸的定位。通过量化蛋白质修饰的程度,每个RCS对泛素的反应性表现出不同的反应性。反应性顺序是MgO> Go> HNE> MDA。鉴定出各种反应产物并映射在蛋白质的赖氨酸,精氨酸和组氨酸残基上。总之,这里提出了一种高度标准化和可重复的方法来制备完全表征的年龄/啤酒。

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