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跨蛋白质组学分析流水线支持和改进了电子转移解离数据集的分析。

Trans-Proteomic Pipeline supports and improves analysis of electron transfer dissociation data sets.

机构信息

Institute for Systems Biology, Seattle, WA 98103, USA.

出版信息

Proteomics. 2010 Mar;10(6):1190-5. doi: 10.1002/pmic.200900567.

Abstract

Electron transfer dissociation (ETD) is an alternative fragmentation technique to CID that has recently become commercially available. ETD has several advantages over CID. It is less prone to fragmenting amino acid side chains, especially those that are modified, thus yielding fragment ion spectra with more uniform peak intensities. Further, precursor ions of longer peptides and higher charge states can be fragmented and identified. However, analysis of ETD spectra has a few important differences that require the optimization of the software packages used for the analysis of CID data or the development of specialized tools. We have adapted the Trans-Proteomic Pipeline to process ETD data. Specifically, we have added support for fragment ion spectra from high-charge precursors, compatibility with charge-state estimation algorithms, provisions for the use of the Lys-C protease, capabilities for ETD spectrum library building, and updates to the data formats to differentiate CID and ETD spectra. We show the results of processing data sets from several different types of ETD instruments and demonstrate that application of the ETD-enhanced Trans-Proteomic Pipeline can increase the number of spectrum identifications at a fixed false discovery rate by as much as 100% over native output from a single sequence search engine.

摘要

电子转移解离(ETD)是一种替代 CID 的碎片化技术,最近已商业化。ETD 比 CID 具有几个优势。它不太容易使氨基酸侧链碎片化,特别是那些经过修饰的侧链,从而产生具有更均匀峰强度的片段离子谱。此外,可以对更长的肽和更高电荷状态的前体离子进行碎片化和鉴定。然而,分析 ETD 谱图有一些重要的区别,需要优化用于分析 CID 数据的软件包,或者开发专门的工具。我们已经将跨蛋白质组分析管道(Trans-Proteomic Pipeline)用于处理 ETD 数据。具体来说,我们添加了对高电荷前体的片段离子谱的支持,与电荷状态估计算法的兼容性,对 Lys-C 蛋白酶的使用规定,ETD 谱图库构建功能,以及对数据格式的更新以区分 CID 和 ETD 谱图。我们展示了来自几种不同类型的 ETD 仪器的数据处理结果,并证明在固定假阳性率下,应用增强型 ETD 跨蛋白质组分析管道可以比单个序列搜索引擎的原始输出增加多达 100%的谱图鉴定数量。

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