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Integrated approach for the comprehensive characterization of lipoproteins from human plasma using FPLC and nano-HPLC-tandem mass spectrometry

机译:使用FPLC和纳米HPLC串联质谱法从人血浆中全面鉴定脂蛋白的综合方法

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摘要

The implication of the various lipoprotein classes in the development of atherosclerotic cardiovascular disease has served to focus a great deal of attention on these particles over the past half-century. Using knowledge gained by the sequencing of the human genome, recent research efforts have been directed toward the elucidation of the proteomes of several lipoprotein subclasses. One of the challenges of such proteomic experimentation is the ability to initially isolate plasma lipoproteins subsequent to their analysis by mass spectrometry. Although several methods for the isolation of plasma lipoproteins are available, the most commonly utilized techniques require large sample volumes and may cause destruction and dissociation of lipoprotein particle-associated proteins. Fast protein liquid chromatography (FPLC) is a nondenaturing technique that has been validated for the isolation of plasma lipoproteins from relatively small sample volumes. In this study, we present the use of FPLC in conjunction with nano-HPLC-ESI-tandem mass spectrometry as a new integrated methodology suitable for the proteomic analysis of human lipoprotein fractions. Results from our analysis show that only 200 μl of human plasma suffices for the isolation of whole high density lipoprotein (HDL) and the identification of the majority of all known HDL-associated proteins using mass spectrometry of the resulting fractions.
机译:在过去的半个世纪中,各种脂蛋白类别在动脉粥样硬化性心血管疾病发展中的作用已引起人们的极大关注。利用通过人类基因组测序获得的知识,最近的研究工作已指向阐明几种脂蛋白亚类的蛋白质组。这种蛋白质组学实验的挑战之一是在通过质谱法对其进行分析之后最初分离血浆脂蛋白的能力。尽管有几种分离血浆脂蛋白的方法可供使用,但最常用的技术需要大量的样品,并且可能导致脂蛋白颗粒相关蛋白的破坏和解离。快速蛋白质液相色谱(FPLC)是一种非变性技术,已被证实可从相对较小的样品量中分离血浆脂蛋白。在这项研究中,我们目前将FPLC与纳米HPLC-ESI串联质谱联用作为一种适用于人脂蛋白组分蛋白质组学分析的新型集成方法。我们的分析结果表明,仅200μl的人类血浆就足以分离整个高密度脂蛋白(HDL),并使用所得馏分的质谱法鉴定大多数已知的与HDL相关的大多数蛋白质。

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