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Integrated Algorithms for High-Throughput Examination of Covalently Labeled Biomolecules by Structural Mass Spectrometry

机译:通过结构质谱法对共价标记生物分子进行高通量检验的集成算法

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摘要

Mass spectrometry based structural proteomics approaches for probing protein structures are increasingly gaining in popularity. The potential for such studies is limited because of the lack of analytical techniques for the automated interpretation of resulting data. In this article, a suite of algorithms called ProtMapMS is developed, integrated, and implemented specifically for the comprehensive automatic analysis of mass spectrometry data obtained for protein structure studies using covalent labeling. The functions include data format conversion, mass spectrum interpretation, detection, and verification of all peptide species, confirmation of the modified peptide products, and quantification of the extent of peptide modification. The results thus obtained provide valuable data for use in combination with computational approaches for protein structure modeling. The structures of both monomeric and hexameric forms of insulin were investigated by oxidative protein footprinting followed by high-resolution mass spectrometry. The resultant data was analyzed both manually and using ProtMapMS without any manual intervention. The results obtained using the two methods were found to be in close agreement and overall were consistent with predictions from the crystallographic structure.
机译:用于探测蛋白质结构的基于质谱的结构蛋白质组学方法越来越受欢迎。由于缺乏自动解释结果数据的分析技术,因此此类研究的潜力受到限制。在本文中,专门开发,集成和实现了一套称为ProtMapMS的算法,用于对使用共价标记进行蛋白质结构研究而获得的质谱数据进行全面的自动分析。功能包括数据格式转换,质谱解释,所有肽种类的检测和验证,修饰肽产物的确认以及肽修饰范围的定量。如此获得的结果提供了有价值的数据,可与蛋白质结构建模的计算方法结合使用。胰岛素的单体和六聚体形式的结构均通过氧化蛋白质足迹法和高分辨率质谱法进行了研究。手动和使用ProtMapMS分析所得数据,无需任何人工干预。发现使用两种方法获得的结果非常一致,并且总体上与晶体结构的预测一致。

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