25年来对呼吸道和其他病毒的质谱反应

Q3 Physics and Astronomy Mass spectrometry Pub Date : 2023-01-01 DOI:10.5702/massspectrometry.a0136
Kevin M. Downard
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引用次数: 0

摘要

本文综述了作者实验室在过去25年中开发的质谱(MS)方法的发展和应用,用于检测;特征、类型和亚型;区分流感、SARS-CoV-2等呼吸道病毒的主要变异和亚变异。所有特征都利用基质辅助激光解吸电离(MALDI)质量图,记录单个病毒蛋白或整个病毒消化。一种基于MALDI的免疫分析方法,将抗体-肽复合物保存在传统MALDI靶标上,而不固定它们,从而使它们能够间接检测。结合位点,从而确定病毒的分子抗原性。同样的方法被用于研究抗病毒药物与其靶病毒蛋白的结合、结合残基的性质和相对结合亲和力。高分辨率质谱的优势被用于检测整个病毒和单个蛋白质消化的独特质量的序列保守的特征肽。这使得病毒能够被分型、分亚型、确定它们的谱系、区分变异和亚变异。它们的检测使用选定的离子监测提高了分析灵敏度限制,以帮助鉴定临床标本中的病毒。相同的高分辨率海量地图数据,用于广泛的病毒株,被输入到一个专门构建的算法(masstreet)中,以便绘制和询问病毒的进化。不需要基因或蛋白质序列,也不需要任何序列比对,这种系统数量学方法还可以在单树构建步骤中确定和显示与病毒蛋白质进化相关的单点突变。
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25 Years Responding to Respiratory and Other Viruses with Mass Spectrometry
This review article presents the development and application of mass spectrometry (MS) approaches, developed in the author’s laboratory over the past 25 years, to detect; characterise, type and subtype; and distinguish major variants and subvariants of respiratory viruses such as influenza and severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). All features make use of matrix-assisted laser desorption ionisation (MALDI) mass maps, recorded for individual viral proteins or whole virus digests. A MALDI-based immunoassay in which antibody–peptide complexes were preserved on conventional MALDI targets without their immobilisation led to an approach that enabled their indirect detection. The site of binding, and thus the molecular antigenicity of viruses, could be determined. The same approach was employed to study antivirals bound to their target viral protein, the nature of the binding residues, and relative binding affinities. The benefits of high-resolution MS were exploited to detect sequence-conserved signature peptides of unique mass within whole virus and single protein digests. These enabled viruses to be typed, subtyped, their lineage determined, and variants and subvariants to be distinguished. Their detection using selected ion monitoring improved analytical sensitivity limits to aid the identification of viruses in clinical specimens. The same high-resolution mass map data, for a wide range of viral strains, were input into a purpose-built algorithm (MassTree) in order to both chart and interrogate viral evolution. Without the need for gene or protein sequences, or any sequence alignment, this phylonumerics approach also determines and displays single-point mutations associated with viral protein evolution in a single-tree building step.
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来源期刊
Mass spectrometry
Mass spectrometry Physics and Astronomy-Instrumentation
CiteScore
1.90
自引率
0.00%
发文量
3
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