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采用保留时间锁定气相色谱/质谱选择离子监测技术将非靶向代谢物分析方法转化为伪靶向方法的新方法。

A novel approach to transforming a non-targeted metabolic profiling method to a pseudo-targeted method using the retention time locking gas chromatography/mass spectrometry-selected ions monitoring.

机构信息

CAS Key Laboratory of Separation Science for Analytical Chemistry, Dalian Institute of Chemical Physics, Chinese Academy of Sciences, Dalian 116023, China.

出版信息

J Chromatogr A. 2012 Sep 14;1255:228-36. doi: 10.1016/j.chroma.2012.01.076. Epub 2012 Feb 2.

Abstract

Non-targeted metabolic profiling is the most widely used method for metabolomics. In this paper, a novel approach was established to transform a non-targeted metabolic profiling method to a pseudo-targeted method using the retention time locking gas chromatography/mass spectrometry-selected ion monitoring (RTL-GC/MS-SIM). To achieve this transformation, an algorithm based on the automated mass spectral deconvolution and identification system (AMDIS), GC/MS raw data and a bi-Gaussian chromatographic peak model was developed. The established GC/MS-SIM method was compared with GC/MS-full scan (the total ion current and extracted ion current, TIC and EIC) methods, it was found that for a typical tobacco leaf extract, 93% components had their relative standard deviations (RSDs) of relative peak areas less than 20% by the SIM method, while 88% by the EIC method and 81% by the TIC method. 47.3% components had their linear correlation coefficient higher than 0.99, compared with 5.0% by the EIC and 6.2% by TIC methods. Multivariate analysis showed the pooled quality control samples clustered more tightly using the developed method than using GC/MS-full scan methods, indicating a better data quality. With the analysis of the variance of the tobacco samples from three different planting regions, 167 differential components (p<0.05) were screened out using the RTL-GC/MS-SIM method, but 151 and 131 by the EIC and TIC methods, respectively. The results show that the developed method not only has a higher sensitivity, better linearity and data quality, but also does not need complicated peak alignment among different samples. It is especially suitable for the screening of differential components in the metabolic profiling investigation.

摘要

非靶向代谢组学分析是代谢组学中最常用的方法。本文建立了一种新方法,通过使用保留时间锁定气相色谱/质谱选择离子监测(RTL-GC/MS-SIM)将非靶向代谢组学方法转化为伪靶向方法。为了实现这种转变,开发了一种基于自动质谱解卷积和识别系统(AMDIS)、GC/MS 原始数据和双高斯色谱峰模型的算法。将建立的 GC/MS-SIM 方法与 GC/MS-全扫描(总离子流和提取离子流,TIC 和 EIC)方法进行比较,结果发现对于典型的烟叶提取物,SIM 方法中 93%的成分的相对峰面积的相对标准偏差(RSD)小于 20%,EIC 方法为 88%,TIC 方法为 81%。与 EIC 方法的 5.0%和 TIC 方法的 6.2%相比,47.3%的成分具有更高的线性相关系数(R>0.99)。多元分析表明,与 GC/MS-全扫描方法相比,使用该方法时,合并的质量控制样品聚类更紧密,表明数据质量更好。通过对来自三个不同种植区的烟叶样品进行方差分析,使用 RTL-GC/MS-SIM 方法筛选出 167 个差异成分(p<0.05),而 EIC 和 TIC 方法分别筛选出 151 个和 131 个差异成分。结果表明,该方法不仅具有更高的灵敏度、更好的线性和数据质量,而且不需要在不同样品之间进行复杂的峰对齐。它特别适用于代谢组学研究中差异成分的筛选。

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