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Fast Multi-blind Modification Search through Tandem Mass Spectrometry

机译:通过串联质谱快速进行多盲修饰搜索

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摘要

With great biological interest in post-translational modifications (PTMs), various approaches have been introduced to identify PTMs using MS/MS. Recent developments for PTM identification have focused on an unrestrictive approach that searches MS/MS spectra for all known and possibly even unknown types of PTMs at once. However, the resulting expanded search space requires much longer search time and also increases the number of false positives (incorrect identifications) and false negatives (missed true identifications), thus creating a bottleneck in high throughput analysis. Here we introduce MODa, a novel “multi-blind” spectral alignment algorithm that allows for fast unrestrictive PTM searches with no limitation on the number of modifications per peptide while featuring over an order of magnitude speedup in relation to existing approaches. We demonstrate the sensitivity of MODa on human shotgun proteomics data where it reveals multiple mutations, a wide range of modifications (including glycosylation), and evidence for several putative novel modifications. Based on the reported findings, we argue that the efficiency and sensitivity of MODa make it the first unrestrictive search tool with the potential to fully replace conventional restrictive identification of proteomics mass spectrometry data.
机译:随着对翻译后修饰(PTM)的极大生物学兴趣,已引入各种方法来使用MS / MS识别PTM。 PTM识别的最新发展集中在一种非限制性方法上,该方法可以一次搜索MS / MS频谱以查找所有已知甚至可能甚至未知的PTM类型。但是,所得到的扩展搜索空间需要更长的搜索时间,并且还会增加误报(错误的标识)和误报(缺少正确的标识)的数量,从而在高吞吐量分析中造成瓶颈。在这里,我们介绍MODA,这是一种新颖的“多盲”光谱比对算法,它可以进行快速无限制的PTM搜索,而对每个肽的修饰数量没有限制,同时相对于现有方法而言,具有超过一个数量级的加速比。我们证明了MODa对人类shot弹枪蛋白质组学数据的敏感性,它揭示了多个突变,广泛的修饰(包括糖基化)以及几种推定的新颖修饰的证据。根据报告的发现,我们认为MODa的效率和灵敏度使其成为第一个无限制搜索工具,有可能完全替代蛋白质组学质谱数据的常规限制性鉴定。

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