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Solution-phase and solid-phase sequential selective modification of side chains in KDYWEC and KDYWE as models for usage in single-molecule protein sequencing

机译:KDYWEC和KDYWE中侧链的溶液相和固相顺序选择性修饰可作为单分子蛋白质测序中的模型

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摘要

Single-molecule protein sequencing is regarded as a promising new method in the field of proteomics. It potentially offers orders of magnitude improvements in sensitivitiy and throughput for protein detection when compared to mass spectrometry. However, the development of such a technology faces significant barriers, especially in the need to chemically derivatize specific amino-acid types with unique labels. For example, fluorescent dyes would be suitable for single-molecule microscopy or nanopore-based sequencing. These emerging single-molecule protein-sequencing technologies suggests a need to develop an amino acid side chain-selective modification scheme that could target several side chains of interest. Current work for modifying residues focuses mainly on one or two side chains. The need to label many side chains, as recent computational modeling suggests, is required for high protein, sequencing coverage of the human proteome. Herein, we report our stragety for modifying two model peptides KYDWEC and KDYWE containing the most reactive residues, using highly opitmized mass labels in a sequential and selective fashion both using solution-phase and solid-phase chemistries, respectively. This will serve as a step towards a modification scheme appropriate for single-molecule studies.
机译:在蛋白质组学领域,单分子蛋白质测序被认为是一种有前途的新方法。与质谱法相比,它有可能在蛋白质检测的灵敏度和通量方面提高几个数量级。但是,这种技术的发展面临重大障碍,特别是在需要使用独特标记对特定氨基酸类型进行化学衍生化的过程中。例如,荧光染料将适合于单分子显微镜或基于纳米孔的测序。这些新兴的单分子蛋白质测序技术表明需要开发一种氨基酸侧链选择性修饰方案,该方案可以靶向多个目标侧链。当前用于修饰残基的工作主要集中在一个或两个侧链上。正如最近的计算模型所表明的那样,人类蛋白质组的高蛋白测序覆盖范围需要标记许多侧链。在本文中,我们报告了我们使用修饰度最高的质量标记,分别采用溶液相和固相化学方法依次和选择性地修饰高度反应性残基的两个模型肽KYDWEC和KDYWE的策略。这将是朝着适用于单分子研究的修饰方案迈出的一步。

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