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首页> 外文期刊>Journal of the American Society for Mass Spectrometry >Manipulating the fragmentation patterns of phosphopeptides via gas-phase boron derivatization: Determining phosphorylation sites in peptides with multiple serines
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Manipulating the fragmentation patterns of phosphopeptides via gas-phase boron derivatization: Determining phosphorylation sites in peptides with multiple serines

机译:通过气相硼衍生化处理磷酸肽的片段化模式:确定具有多个丝氨酸的肽中的磷酸化位点

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摘要

Trivalent boron species readily react with protonated phosphopeptides to give addition products with the loss of boron ligands. In the present study, trimethoxyborane (TMB), diisopropoxymethylborane (DIPM), and diethylmethoxyborane (DEMB) were allowed to react with four phosphopeptides, VsSF, LSsF, LsGASA, and VSGAsA (lower-case s indicates phosphoserine). Each of the phosphopeptides contains one serine that is phosphorylated and one that is not. Under collision-activated dissociation (CAD) conditions, the boron-derivatized peptides give fragmentation patterns that differ significantly from that of the protonated phosphopeptide. The patterns vary, depending on the number of labile (i.e., alkoxy) ligands on the boron. In general, boron derivatization increases the yield of phosphate-containing sequence ions, but dramatic effects are only seen with certain reagent/peptide combinations. However, the suite of reagents provides a means of altering and increasing the information content of phosphopeptide CAD spectra.
机译:三价硼物质很容易与质子化的磷酸肽反应生成加成产物,但硼配体丢失。在本研究中,使三甲氧基硼烷(TMB),二异丙氧基甲基硼烷(DIPM)和二乙基甲氧基硼烷(DEMB)与四种磷酸肽VsSF,LSsF,LsGASA和VSGAsA反应(小写字母s表示磷酸丝氨酸)。每种磷酸肽均含有一个丝氨酸被磷酸化而另一个未被磷酸化。在碰撞激活解离(CAD)条件下,硼衍生的肽的片段化模式与质子化磷酸肽的片段显着不同。图案根据硼上不稳定的(即烷氧基)配体的数量而变化。通常,硼衍生化可增加含磷酸盐的序列离子的产量,但仅在某些试剂/肽组合下才能看到显着效果。但是,试剂套件提供了一种改变和增加磷酸肽CAD光谱信息含量的方法。

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