Identification of toxic cyclopeptides based on mass spectral library matching

Boris L. Milman , Inna K. Zhurkovich
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引用次数: 6

Abstract

To gain perspective on the use of tandem mass spectral libraries for identification of toxic cyclic peptides, the new library was built from 263 mass spectra (mainly MS2 spectra) of 59 compounds of that group, such as microcystins, amatoxins, and some related compounds. Mass spectra were extracted from the literature or specially acquired on ESI-Q-ToF and MALDI-ToF/ToF tandem instruments. ESI-MS2 product-ion mass spectra appeared to be rather close to MALDI-ToF/ToF fragment spectra which are uncommon for mass spectral libraries. Testing of the library was based on searches where reference spectra were in turn cross-compared. The percentage of 1st rank correct identifications (true positives) was 70% in a general case and 88–91% without including knowingly defective (‘one-dimension’) spectra as test ones. The percentage of 88–91% is the principal estimate for the overall performance of this library that can be used in a method of choice for identification of individual cyclopeptides and also for group recognition of individual classes of such peptides. The approach to identification of cyclopeptides based on mass spectral library matching proved to be the most effective for abundant toxins. That was confirmed by analysis of extracts from two cyanobacterial strains.

基于质谱库匹配的有毒环肽鉴定
为了进一步研究串联质谱文库在毒性环肽鉴定中的应用,本文利用微囊藻毒素(microcystiins)、阿马特毒素(amatoxins)及其相关化合物的263个质谱(主要为MS2谱)建立了串联质谱文库。质谱由ESI-Q-ToF和MALDI-ToF/ToF串联仪器提取或专门获取。ESI-MS2产物离子质谱与MALDI-ToF/ToF片段质谱相当接近,这在质谱库中并不常见。文库的测试是基于参考光谱依次交叉比较的搜索。在一般情况下,一级正确鉴定(真阳性)的百分比为70%,在不包括故意缺陷(“一维”)光谱作为测试的情况下,这一比例为88-91%。88-91%的百分比是该文库总体性能的主要估计,可用于识别单个环肽的选择方法,也可用于此类肽的单个类别的基团识别。结果表明,基于质谱库匹配的环肽鉴定方法对丰富的毒素是最有效的。对两种蓝藻菌株提取物的分析证实了这一点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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