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Non-targeted LC-MS and CE-MS for biomarker discovery in bioreactors: Influence of separation, mass spectrometry and data processing tools

机译:用于生物反应器中的生物标志物发现的非靶向LC-MS和CE-MS:分离,质谱和数据处理工具的影响

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摘要

Liquid separation coupled to mass spectrometry is often used for non-targeted analyses in various fields, such as metabolomics. However, the combination of non-standardized methods, various mass spectrometers (MS) and processing tools for data evaluation affect biomarker discovery potentially. Here, we present a comprehensive study of these factors based on non-targeted liquid chromatography coupled to time-of-flight (TOF) and Orbitrap MS and capillary zone electrophoresis to Orbitrap analyses of the same bioreactor samples, describing the correlation of its gas yield with changing feature signal intensity. The three datasets were processed with MZmine 2 and XCMS online and subsequential Partial Least Square Regression (PLSR) with Variable Importance in Projection (VIP) ranking for feature prioritization. The six feature tables were compared to evaluate their overlap of shared features and the influence of the processing software and MS instrument on the VIP values and fold changes. The overlaps, defined as a fraction of one feature table found in the comparative table, were from 27% to 57% for the comparison of MZmine and XCMS and from 15% to 50% between Orbitrap and TOF data sets, respectively. Considering the most relevant features only (VIP >1.5), the overlaps were increased significantly in all cases from 26% to 95%. For the same data set, both VIP values and fold changes were well correlated, however, varied significantly between TOF and Orbitrap. CE-MS showed higher total feature numbers compared to LC-MS, most likely due to its more appropriate selectivity, different sample preparation, and/or the sensitive nano-ESI interface. Since only less than 10% of MS/MS data overlapped, CE-MS provided complementary information to LC-MS. Overall, our systematic study proves the benefits of using different separation techniques and processing tools but also indicates a significant influence of mass spectrometry on comprehensive biomarker discovery.
机译:偶联至质谱法的液体分离通常用于各种领域的非靶向分析,例如代谢组。然而,非标准化方法的组合,各种质谱仪(MS)和用于数据评估的处理工具可能影响生物标志物发现。在这里,我们对基于非靶向液相色谱的这些因素进行了综合研究,这些因子耦合到飞行时间(TOF)和氧化物MS和毛细管区电泳与相同生物反应器样本的orbitrap分析,描述其天然气产量的相关性随着改变特征信号强度。使用Mzmine 2和XCMS在线和后续部分最小二乘回归(PLSR)处理三个数据集,在投影(VIP)排名中具有可变重要性的特征优先级。比较六个特征表以评估它们对共享特征的重叠和处理软件和MS仪器对VIP值的影响和折叠变化。定义为比较表中发现的一个特征表的一部分的重叠为27%至57%,用于比较MZMINE和XCMS,分别在orbitrap和TOF数据集之间的15%至50%。考虑到最相关的特征(VIP> 1.5),在所有情况下,重叠在26%至95%的情况下显着增加。对于相同的数据集,vip值和折叠变化都很好地相关,但ToF和orbitrap之间有显着变化。 CE-MS与LC-MS相比显示出更高的总特征数字,最有可能是由于其更适当的选择性,不同的样品制备和/或敏感的纳米ESI界面。由于只有不到10%的MS / MS数据重叠,因此CE-MS为LC-MS提供了互补信息。总体而言,我们的系统研究证明了使用不同的分离技术和加工工具的益处,但也表明了质谱对综合生物标志物发现的显着影响。

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