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Exopeptidase Assisted N- and C-Terminal Proteome Sequencing

机译:Exopeptivease辅助N-和C末端蛋白酶序列测序

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摘要

Due to mechanisms such as proteolytic processing or alternative translation starts, in vivo proteoforms do not necessarily correspond directly to those encoded in the genome. Therefore, the knowledge of protein termini is an indispensable prerequisite to understand protein functions. So far, sequencing of protein N- and C-termini has been limited to single purified protein species, while the proteome-wide identification of N- and C-termini relies on the generation of single, terminal proteotypic peptides followed by chemical enrichment or depletion strategies to facilitate their detection via mass spectrometry (MS). To overcome the numerous limitations in such approaches, we present an alternative concept that readily enables unbiased ladder sequencing of protein N- and C-termini. The approach combines exopeptidase digestions of the proteome with two-dimensional chromatographic separation and tandem-MS. We demonstrate the potential of the methodology by analyzing the N- and Cterminome of S. cerevisiae, identifying 2190 N-termini and 1562 C-termini. In conclusion, the presented method largely expands the proteomics toolbox enabling N- and C-terminal sequential characterization of entire proteomes.
机译:由于诸如蛋白水解加工或替代翻译的机制,在体内蛋白质常规中不一定直接对应于基因组中编码的那些。因此,蛋白质末端的知识是了解蛋白质功能的不可或缺的先决条件。到目前为止,蛋白质N-和C-Termini的测序仅限于单一纯化的蛋白质物种,而N-和C-Termini的蛋白质综合鉴定依赖于单一,终端蛋白质肽的产生,然后是化学富集或耗尽促进通过质谱(MS)检测的策略。为了克服这些方法的许多限制,我们提出了一种替代概念,即易于实现蛋白质N-和C-Termini的梯形梯形测序。该方法将蛋白质组的外肽酶消化与二维色谱分离和串联 - MS结合在一起。我们通过分析酿酒酵母的N-和柔粉,鉴定2190 N-Termini和1562 C-Termini,证明了方法的潜力。总之,所提出的方法在很大程度上扩展了蛋白质组学工具箱,从而实现了整个蛋白质组的N-和C末端顺序表征。

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  • 来源
    《Analytical chemistry》 |2020年第7期|共10页
  • 作者单位

    Christian Albrechts Univ Kiel Inst Expt Med Systemat Proteome Res &

    Bioanalyt Kiel Germany;

    Christian Albrechts Univ Kiel Inst Expt Med Systemat Proteome Res &

    Bioanalyt Kiel Germany;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分析化学;
  • 关键词

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