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基于离子淌度的无标定量采集(MSE)为噬菌体结构蛋白质组学分析提供了一种系统的方法。

Data-independent acquisition (MSE) with ion mobility provides a systematic method for analysis of a bacteriophage structural proteome.

机构信息

Cabrini College, Department of Science, 610 King of Prussia Road, Radnor, PA 19087, United States.

出版信息

J Virol Methods. 2014 Jan;195:9-17. doi: 10.1016/j.jviromet.2013.10.007. Epub 2013 Oct 12.

Abstract

In this work, a method was developed to study the structural proteome of mycobacteriophage Marvin, a recent isolate from soil with 107 predicted coding sequences. This prototype method was applied for semi-quantitative analysis of the composition of this mycobacteriophage virion using ion mobility spectrometry and data-independent acquisition (MS(E)-IMS). MS(E)-IMS was compared to a more conventional proteomics technique employing mass spectrometry with a data-dependent acquisition strategy. MS(E)-IMS provided broad coverage of the virion proteome and high sequence coverage for individual proteins. This shotgun method does not depend on the limited sensitivity of visualization of protein bands by staining reagents inherent in gel-based methods. The method is comprehensive, provides high sequence coverage and is proposed as a particularly efficient method for the study of bacteriophage proteomes.

摘要

在这项工作中,开发了一种方法来研究 Marvin 分枝杆菌噬菌体的结构蛋白质组,Marvin 是一种最近从土壤中分离出来的噬菌体,有 107 个预测的编码序列。该原型方法应用于使用离子淌度谱和非依赖性数据获取(MS(E)-IMS)对半定量分析这种分枝杆菌噬菌体病毒粒子的组成。MS(E)-IMS 与更传统的依赖于数据的采集策略的质谱蛋白质组学技术进行了比较。MS(E)-IMS 提供了病毒粒子蛋白质组的广泛覆盖范围和单个蛋白质的高序列覆盖范围。这种鸟枪法方法不依赖于基于凝胶的方法中染色试剂固有地对蛋白质条带进行可视化的有限灵敏度。该方法是全面的,提供了高的序列覆盖范围,并被提议作为研究噬菌体蛋白质组的一种特别有效的方法。

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