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肽段的基于质量的分类(MBC):高精度的前体离子质量值可用于直接识别肽段磷酸化。

Mass-based classification (MBC) of peptides: highly accurate precursor ion mass values can be used to directly recognize peptide phosphorylation.

作者信息

Spengler Bernhard, Hester Alfons

机构信息

Institute of Inorganic and Analytical Chemistry, Justus Liebig University Giessen, Giessen, Germany.

出版信息

J Am Soc Mass Spectrom. 2008 Dec;19(12):1808-12. doi: 10.1016/j.jasms.2008.08.005. Epub 2008 Aug 15.

DOI:10.1016/j.jasms.2008.08.005
PMID:18804385
Abstract

Accurate mass values as obtainable by Fourier transform ion cyclotron resonance mass spectrometry (FTICR-MS) were employed in a theoretical study to differentiate between nonmodified and phosphorylated peptides. It was found that for peptide masses up to 1,000 u more than 98% of all theoretical monophosphorylated peptides (all possible combinations of proteinogenic amino acids having one phosphorylation on S, T, or Y) can be distinguished from nonphosphorylated peptides directly by their mass, if mass values are determined with an accuracy of better than +/-0.1 ppm. At a peptide mass of 1,500 u still 70% of all possible monophosphorylated peptides are distinguishable from nonmodified peptides by their accurate mass alone. In contrast to established techniques of data-dependent multidimensional mass spectrometry, only the mass of the precursor ion is necessary to decide upon subsequent fragment ion analysis of a peptide for sequence analysis in an LC-MS/MS investigation of a complex sample, when using a precalculated mass distribution table of theoretical peptides. A mass distribution table of nonphosphorylated and monophosphorylated peptides with a bin width of 0.1 mu was made available via the open web site www.peptidecomposer.com.

摘要

在一项理论研究中,采用了傅里叶变换离子回旋共振质谱法(FTICR-MS)可获得的精确质量值来区分未修饰肽和磷酸化肽。研究发现,对于质量高达1000 u的肽,如果质量值的测定精度优于±0.1 ppm,超过98%的所有理论单磷酸化肽(蛋白质氨基酸在丝氨酸、苏氨酸或酪氨酸上有一个磷酸化的所有可能组合)可以直接通过其质量与未磷酸化肽区分开来。在肽质量为1500 u时,仍有70%的所有可能的单磷酸化肽仅通过其精确质量就可与未修饰肽区分开来。与已建立的数据依赖型多维质谱技术不同,在对复杂样品进行液相色谱-串联质谱(LC-MS/MS)分析以进行序列分析时,当使用预先计算的理论肽质量分布表时,仅需前体离子的质量就可决定对肽进行后续的碎片离子分析。通过开放网站www.peptidecomposer.com提供了一个箱宽为0.1 mu的未磷酸化和单磷酸化肽的质量分布表。

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