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临床蛋白质组学研究中的分析前因素:体外蛋白质修饰对多发性硬化症生物标志物发现的影响。

Pre-analytical factors in clinical proteomics investigations: impact of ex vivo protein modifications for multiple sclerosis biomarker discovery.

机构信息

Centro Studi sull'Invecchiamento (Ce.S.I.), Fondazione G. d'Annunizio, Chieti, Italy.

出版信息

J Proteomics. 2010 Jan 3;73(3):579-92. doi: 10.1016/j.jprot.2009.07.014. Epub 2009 Aug 8.

DOI:10.1016/j.jprot.2009.07.014
PMID:19666151
Abstract

Serum proteome investigations have raised an incredible interest in the research of novel molecular biomarker, nevertheless few of the proposed evidences have been translated to the clinical practice. One of the limiting factors has been the lack of generally accepted guidelines for clinical proteomics studies and the lack of a robust analytical and pre-analytical ground for the proposed classification models. Pre-analytical issues may results in a deep impact for biomarker discovery campaign. In this study we present a systematic evaluation of sample storage and sampling conditions for clinical proteomics investigations. We have developed and validated a linear MALDI-TOF-MS protein profiling method to explore the low protein molecular weight region (5-20 kDa) of serum samples. Data normalization and processing was performed using optimise peak detection routine (LIMPIC) able to describe each group under investigation. Data were acquired either from healthy volunteers and from multiple sclerosis patients in order to highlight ex vivo protein profile alteration related to different physio-pathological conditions. Our data showed critical conditions for serum protein profiles depending on storage times and temperatures: 23 degrees C, 4 degrees C, -20 degrees C and -80 degrees C. We demonstrated that upon a -20 degrees C short term storage, characteristic degradation profiles are associated with different clinical groups. Protein signals were further identified after preparative HPLC separation by peptide sequencing on a nanoLC-Q-TOF TANDEM mass spectrometer. Apolipoprotein A-IV and complement C3 protein fragments, transthyretin and the oxidized isoforms in different apolipoprotein species represent the major molecular features of such a degradation pattern.

摘要

血清蛋白质组学研究引起了人们对新型分子生物标志物的极大兴趣,但提出的证据很少转化为临床实践。其中一个限制因素是缺乏普遍接受的临床蛋白质组学研究指南,以及缺乏用于提出的分类模型的稳健分析和预分析基础。预分析问题可能会对生物标志物发现研究产生深远的影响。在这项研究中,我们对临床蛋白质组学研究的样品储存和采样条件进行了系统评估。我们开发并验证了一种线性 MALDI-TOF-MS 蛋白质分析方法,用于探索血清样品的低分子量蛋白质区域(5-20 kDa)。使用能够描述每个研究组的优化峰检测例程(LIMPIC)对数据进行归一化和处理。数据来自健康志愿者和多发性硬化症患者,以突出与不同生理病理条件相关的体外蛋白质谱改变。我们的数据显示,血清蛋白质谱取决于储存时间和温度的关键条件:23°C、4°C、-20°C 和-80°C。我们证明,在-20°C 的短期储存下,不同临床组与特征性降解谱相关。在通过纳升 LC-Q-TOF TANDEM 质谱仪进行肽测序进行制备性 HPLC 分离后,进一步鉴定了蛋白质信号。载脂蛋白 A-IV 和补体 C3 蛋白片段、转甲状腺素蛋白以及不同载脂蛋白物种中的氧化同工型代表了这种降解模式的主要分子特征。

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