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首页> 外文期刊>Journal of proteomics >Comprehensive identification of protein disulfide bonds with pepsin/trypsin digestion, Orbitrap HCD and Spectrum Identification Machine
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Comprehensive identification of protein disulfide bonds with pepsin/trypsin digestion, Orbitrap HCD and Spectrum Identification Machine

机译:用胃蛋白酶/胰蛋白酶消化,锻造HCD和谱识别机综合鉴定蛋白质二硫键。

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摘要

Disulfide bonds (SS) are post-translational modifications important for the proper folding and stabilization of many cellular proteins with therapeutic uses, including antibodies and other biologics. With budding advances of biologics and biosimilars, there is a mounting need for a robust method for accurate identification of SS. Even though several mass spectrometry methods have emerged for this task, their practical use rests on the broad effectiveness of both sample preparation methods and bioinformatics tools. Here we present a new protocol tailored toward mapping SS; it uses readily available reagents, instruments, and software. For sample preparation, a 4-h pepsin digestion at pH 1.3 followed by an overnight trypsin digestion at pH 6.5 can maximize the release of SS-containing peptides from non-reduced proteins, while minimizing SS scrambling. For LC/MS/MS analysis, SS-containing peptides can be efficiently fragmented with HCD in a Q Exactive Orbitrap mass spectrometer, preserving SS for subsequent identification. Our bioinformatics protocol describes how we tailored our freely downloadable and easy-to-use software, Spectrum Identification Machine for Cross-Linked Peptides (SIM-XL), to minimize false identification and facilitate manual validation of SS-peptide mass spectra. To substantiate this optimized method, we've comprehensively identified 14 out of 17 known SS in BSA.
机译:二硫键(SS)是翻译后修饰对于具有治疗用途的许多细胞蛋白的适当折叠和稳定,包括抗体和其他生物学。随着生物学和生物纤维单模的萌芽进步,有一种用于精确识别SS的鲁棒方法的安装需求。尽管为此任务出现了几种质谱方法,但它们的实际用途也可以依赖于样品制备方法和生物信息学工具的广泛有效性。在这里,我们提出了一种针对映射SS量身定制的新协议;它使用易于获得的试剂,仪器和软件。对于样品制备,在pH 1.3的pH 1.3下进行4-H百长蛋白酶消化,然后在pH 6.5下消化,可以最大化来自非减少蛋白质的含Ss的肽的释放,同时最小化SS扰扰。对于LC / MS / MS分析,含SS的肽可以用HCD在Q辐射的横射质谱仪中用HCD有效地将SS进行有效地碎片,以随后鉴定。我们的生物信息学协议描述了我们如何根据交联肽(SIM-XL)量身定制我们自由可下载和易于使用的软件,频谱识别机,以最大限度地减少假识别并促进SS-肽质谱的手工验证。为了证实这一优化方法,我们在BSA中全面地识别了17个已知的SS中的14个。

著录项

  • 来源
    《Journal of proteomics》 |2019年第2019期|共9页
  • 作者单位

    Rutgers State Univ Ctr Adv Prote Res New Jersey Med Sch Newark NJ 07103 USA;

    Rutgers State Univ Ctr Adv Prote Res New Jersey Med Sch Newark NJ 07103 USA;

    Rutgers State Univ Ctr Adv Prote Res New Jersey Med Sch Newark NJ 07103 USA;

    Rutgers State Univ Ctr Adv Prote Res New Jersey Med Sch Newark NJ 07103 USA;

    Rutgers State Univ Ctr Adv Prote Res New Jersey Med Sch Newark NJ 07103 USA;

    Inst Pasteur CNRS USR 2000 Mass Spectrometry Biol Unit Paris France;

    Fiocruz Parana Lab Struct &

    Computat Prote Carlos Chagas Inst Curitiba Parana Brazil;

    Rutgers State Univ New Jersey Med Sch Dept Pharmacol Physiol &

    Neurosci Newark NJ 07103 USA;

    Rutgers State Univ Ctr Adv Prote Res New Jersey Med Sch Newark NJ 07103 USA;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 蛋白质;
  • 关键词

    Tandem mass spectrometry; Protein disulfide bond; Pepsin; Trypsin; HCD; SIM-XL;

    机译:串联质谱;蛋白质二硫键;胃蛋白酶;胰蛋白酶;HCD;SIM-XL;

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