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基于质谱的定量蛋白质组学综述:靶向和非依赖性数据采集。

A review on mass spectrometry-based quantitative proteomics: Targeted and data independent acquisition.

机构信息

Masaryk University, Research Centre for Toxic Compounds in the Environment, Kamenice 753/5, 625 00, Brno, Czechia.

Masaryk University, Research Centre for Toxic Compounds in the Environment, Kamenice 753/5, 625 00, Brno, Czechia.

出版信息

Anal Chim Acta. 2017 Apr 29;964:7-23. doi: 10.1016/j.aca.2017.01.059. Epub 2017 Feb 2.

DOI:10.1016/j.aca.2017.01.059
PMID:28351641
Abstract

Mass spectrometry (MS) based proteomics have achieved a near-complete proteome coverage in humans and in several other organisms, producing a wealth of information stored in databases and bioinformatics resources. Recent implementation of selected/multiple reaction monitoring (SRM/MRM) technology in targeted proteomics introduced the possibility of quantitatively follow-up specific protein targets in a hypothesis-driven experiment. In contrast to immunoaffinity-based workflows typically used in biological and clinical research for protein quantification, SRM/MRM is characterized by high selectivity, large capacity for multiplexing (approx. 200 proteins per analysis) and rapid, cost-effective transition from assay development to deployment. The concept of SRM/MRM utilizes triple quadrupole (QqQ) mass analyzer to provide inherent reproducibility, unparalleled sensitivity and selectivity to efficiently differentiate isoforms, post-translational modifications and mutated forms of proteins. SRM-like targeted acquisitions such as parallel reaction monitoring (PRM) are pioneered on high resolution/accurate mass (HR/AM) platforms based on the quadrupole-orbitrap (Q-orbitrap) mass spectrometer. The expansion of HR/AM also caused development in data independent acquisition (DIA). This review presents a step-by-step tutorial on development of SRM/MRM protein assay intended for researchers without prior experience in proteomics. We discus practical aspects of SRM-based quantitative proteomics workflow, summarize milestones in basic biological and medical research as well as recent trends and emerging techniques.

摘要

基于质谱(MS)的蛋白质组学已经在人类和其他几种生物中实现了近乎完整的蛋白质组覆盖,产生了大量存储在数据库和生物信息学资源中的信息。最近,在靶向蛋白质组学中实施的选择/多重反应监测(SRM/MRM)技术为在假设驱动的实验中定量跟踪特定蛋白质靶标提供了可能性。与通常用于生物和临床研究中蛋白质定量的基于免疫亲和的工作流程相比,SRM/MRM 的特点是高选择性、高多重化能力(每个分析约 200 种蛋白质)以及从检测开发到部署的快速、具有成本效益的过渡。SRM/MRM 的概念利用三重四极杆(QqQ)质量分析仪提供固有重现性、无与伦比的灵敏度和选择性,以有效地区分蛋白质的同工型、翻译后修饰和突变形式。基于四极杆-轨道阱(Q-orbitrap)质谱仪的高分辨率/精确质量(HR/AM)平台上开创了类似于 SRM 的靶向采集,如平行反应监测(PRM)。HR/AM 的扩展也推动了数据非依赖性采集(DIA)的发展。本综述为没有蛋白质组学经验的研究人员提供了一个关于开发用于 SRM/MRM 蛋白质分析的逐步教程。我们讨论了基于 SRM 的定量蛋白质组学工作流程的实际方面,总结了基础生物学和医学研究中的里程碑以及最近的趋势和新兴技术。

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