使用靶向和非靶向数据非依赖型采集技术的定量蛋白质组学的临床应用
Clinical applications of quantitative proteomics using targeted and untargeted data-independent acquisition techniques.
作者信息
Meyer Jesse G, Schilling Birgit
机构信息
a Mass Spectrometry Core , Buck Institute for Research on Aging , Novato , CA , USA.
出版信息
Expert Rev Proteomics. 2017 May;14(5):419-429. doi: 10.1080/14789450.2017.1322904.
Abstract
While selected/multiple-reaction monitoring (SRM or MRM) is considered the gold standard for quantitative protein measurement, emerging data-independent acquisition (DIA) using high-resolution scans have opened a new dimension of high-throughput, comprehensive quantitative proteomics. These newer methodologies are particularly well suited for discovery of biomarker candidates from human disease samples, and for investigating and understanding human disease pathways. Areas covered: This article reviews the current state of targeted and untargeted DIA mass spectrometry-based proteomic workflows, including SRM, parallel-reaction monitoring (PRM) and untargeted DIA (e.g., SWATH). Corresponding bioinformatics strategies, as well as application in biological and clinical studies are presented. Expert commentary: Nascent application of highly-multiplexed untargeted DIA, such as SWATH, for accurate protein quantification from clinically relevant and disease-related samples shows great potential to comprehensively investigate biomarker candidates and understand disease.
摘要
虽然选择反应监测/多反应监测(SRM或MRM)被认为是蛋白质定量测量的金标准,但使用高分辨率扫描的新兴数据非依赖型采集(DIA)开启了高通量、全面定量蛋白质组学的新篇章。这些更新的方法特别适合从人类疾病样本中发现生物标志物候选物,以及研究和理解人类疾病途径。涵盖领域:本文综述了基于靶向和非靶向DIA质谱的蛋白质组学工作流程的现状,包括SRM、平行反应监测(PRM)和非靶向DIA(如SWATH)。介绍了相应的生物信息学策略以及在生物学和临床研究中的应用。专家评论:高度多重非靶向DIA(如SWATH)在从临床相关和疾病相关样本中进行准确蛋白质定量方面的新兴应用,在全面研究生物标志物候选物和理解疾病方面显示出巨大潜力。
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