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拉曼光谱在人血清白蛋白中自由基介导损伤鉴定中的应用。

Use of Raman spectroscopy for the identification of radical-mediated damages in human serum albumin.

机构信息

Istituto I.S.O.F., Consiglio Nazionale delle Ricerche, Bologna, Italy.

出版信息

Anal Bioanal Chem. 2011 Jul;400(9):2921-31. doi: 10.1007/s00216-011-4970-y. Epub 2011 Apr 16.

DOI:10.1007/s00216-011-4970-y
PMID:21494773
Abstract

Damages induced by free radicals on human serum albumin (HSA), the most prominent protein in plasma, were investigated by Raman spectroscopy. HSA underwent oxidative and reductive radical stress. Gamma-irradiation was used to simulate the endogenous formation of reactive radical species such as hydrogen atoms ((•)H), solvated electrons (e(aq)(-)) and hydroxyl radicals ((•)OH). Raman spectroscopy was shown to be a useful tool in identifying conformational changes of the protein structure and specific damages occurring at sensitive amino acid sites. In particular, the analysis of the S-S stretching region suggested the radical species caused modifications in the 17 disulphide bridges of HSA. The concomitant action of e(aq)(-) and (•)H atoms caused the formation of cyclic disulphide bridges, showing how cystine pairs act as efficient interceptors of reducing species, by direct scavenging and electron transfer reactions within the protein. This conclusion was further confirmed by the modifications visible in the Raman bands due to Phe and Tyr residues. As regards to protein folding, both oxidative and reductive radical stresses were able to cause a loss in α-helix content, although the latter remains the most abundant secondary structure component. β-turns motifs significantly increased as a consequence of the synergic action of e(aq)(-) and (•)H atoms, whereas a larger increase in the β-sheet content was found following the exposure to (•)OH and/or (•)H attack.

摘要

采用拉曼光谱研究了自由基对人血清白蛋白(HSA)的损伤,HSA 是血浆中最主要的蛋白质。HSA 经历了氧化和还原自由基应激。γ 射线辐照用于模拟内源性活性自由基物种的形成,如氢原子((•)H)、溶剂化电子(e(aq)(-))和羟基自由基((•)OH)。拉曼光谱被证明是一种有用的工具,可以识别蛋白质结构的构象变化和敏感氨基酸位点发生的特定损伤。特别是,S-S 伸缩区域的分析表明,自由基物种引起 HSA 中 17 个二硫键的修饰。e(aq)(-)和(•)H 原子的共同作用导致环状二硫键的形成,表明胱氨酸对作为有效的还原剂拦截器的作用,通过直接清除和电子转移反应在蛋白质内发生。这一结论进一步通过由于苯丙氨酸和酪氨酸残基引起的 Raman 带中的修饰得到证实。关于蛋白质折叠,氧化和还原自由基应激都能够导致α-螺旋含量的损失,尽管后者仍然是最丰富的二级结构成分。β-转角基序由于 e(aq)(-)和(•)H 原子的协同作用显著增加,而在暴露于(•)OH 和/或(•)H 攻击后,β-折叠含量的增加更大。

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