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采用气相色谱 - 质谱联用结合薄层色谱印迹法检测胆固醇酯氢过氧化物异构体。

Detection of cholesteryl ester hydroperoxide isomers using gas chromatography-mass spectrometry combined with thin-layer chromatography blotting.

作者信息

Kawai Yoshichika, Miyoshi Mariko, Moon Jae-Hak, Terao Junji

机构信息

Department of Food Science, Graduate School of Nutrition and Biosciences, The University of Tokushima, Tokushima 770-8503, Japan.

出版信息

Anal Biochem. 2007 Jan 1;360(1):130-7. doi: 10.1016/j.ab.2006.09.028. Epub 2006 Oct 24.

DOI:10.1016/j.ab.2006.09.028
PMID:17097596
Abstract

Oxidative modification of low-density lipoprotein (LDL) has been implicated in the pathogenesis of atherosclerosis. During the oxidation of LDL, cholesteryl esters, the major lipid components in LDL, are oxidized to cholesteryl ester hydroperoxides (CEOOH). The isomers of CEOOH may reflect the reactive species that initiate the peroxidation reaction. In the current study, a novel analytical method for the determination of CEOOH isomers, especially cholesteryl linoleate hydroperoxide isomers, was developed using the combination of two chromatographic techniques: (i) thin-layer chromatography blotting with diphenyl-1-pyrenylphosphine (DPPP) fluorescent detection (DPPP-TLC blotting) and (ii) gas chromatography-electron ionization-mass spectrometry (GC-EI-MS). CEOOH was applied to DPPP-TLC blotting, the obtained DPPP-derived fluorescent spots containing cholesteryl ester hydroxides were extracted and derivatized (hydrogenation, transmethylation, and trimethylsilylation), and the formed methyl ester/trimethylsilylether derivatives of hydroxyoctadecenoic acid were then analyzed by GC-EI-MS. The CEOOH isomers were determined by selected ion monitoring of isomer-specific fragment ions originated from the alpha-cleavage of the trimethylsilyloxyl group. Using these two chromatographic techniques, we were able to detect isomeric CEOOH in the oxidized human LDL. Our results indicated that GC-EI-MS analysis combined with DPPP-TLC blot is a specific method for analyzing cholesteryl ester hydroperoxide isomers in biological samples such as oxidized LDL.

摘要

低密度脂蛋白(LDL)的氧化修饰与动脉粥样硬化的发病机制有关。在LDL氧化过程中,LDL中的主要脂质成分胆固醇酯被氧化为胆固醇酯氢过氧化物(CEOOH)。CEOOH的异构体可能反映引发过氧化反应的活性物质。在本研究中,结合两种色谱技术开发了一种测定CEOOH异构体,特别是亚油酸胆固醇酯氢过氧化物异构体的新型分析方法:(i)用二苯基-1-芘基膦(DPPP)荧光检测的薄层色谱印迹法(DPPP-TLC印迹法)和(ii)气相色谱-电子电离-质谱法(GC-EI-MS)。将CEOOH应用于DPPP-TLC印迹法,提取含有胆固醇酯氢氧化物的所得DPPP衍生荧光斑点并进行衍生化(氢化、甲基化和三甲基硅烷化),然后通过GC-EI-MS分析形成的羟基十八碳烯酸甲酯/三甲基硅醚衍生物。通过对源自三甲基硅氧基α-裂解的异构体特异性碎片离子进行选择离子监测来确定CEOOH异构体。使用这两种色谱技术,我们能够检测氧化的人LDL中的异构体CEOOH。我们的结果表明,GC-EI-MS分析与DPPP-TLC印迹相结合是分析生物样品(如氧化LDL)中胆固醇酯氢过氧化物异构体的一种特异性方法。

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