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Carboxy group derivatization for enhanced electron-transfer dissociation mass spectrometric analysis of phosphopeptides

机译:羧基衍生化可增强磷酸肽的电子转移解离质谱分析

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摘要

A novel strategy based on carboxy group derivatization is presented for specific characterization of phosphopeptides. By tagging the carboxy group with 1-(2-pyrimidyl) piperazine (PP), the ion charge states of phosphopeptides can be largely enhanced, showing great advantages for sequencing phosphorylated peptides with electron-transfer dissociation MS. Besides, after PP-derivatization, most non-specific bindings can be avoided by eliminating the interaction between the carboxy group and TiO 2, greatly improving the specificity of TiO 2-based phosphopeptide enrichment strategy. Moreover, being tagged with a hydrophobic group, the retention time of phosphopeptides in RPLC can be prolonged, overcoming the difficulty of separating phosphopeptides in RPLC-based approach. Together with several other advantages, such as ease of handling, rapid reaction time, broad applicability and good reproducibility, this PP-derivatization method is promising for high-throughput phosphoproteome research.
机译:提出了一种基于羧基衍生化的新策略,用于磷酸肽的特异性表征。通过用1-(2-嘧啶基)哌嗪(PP)标记羧基,可以大大提高磷酸肽的离子电荷状态,显示出用电子转移解离MS对磷酸化肽进行测序的巨大优势。此外,PP衍生化后,通过消除羧基与TiO 2之间的相互作用,可以避免大多数非特异性结合,从而大大提高了基于TiO 2的磷酸肽富集策略的特异性。此外,通过疏水基团的标记,磷酸肽在RPLC中的保留时间可以延长,克服了基于RPLC的方法分离磷酸肽的困难。加上易于操作,反应时间短,适用范围广和重现性好等其他优点,这种PP衍生化方法有望用于高通量磷酸化蛋白质组学研究。

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