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Liquid chromatography-mass spectrometry in metabolomics research: Mass analyzers in ultra high pressure liquid chromatography coupling(Review)

机译:代谢组学中的液相色谱-质谱联用:超高压液相色谱联用中的质谱分析仪(综述)

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The present review gives an introduction into the concept of metabolomics and provides an overview of the analytical tools applied in non-targeted metabolomics with a focus on liquid chromatography (LC). LC is a powerful analytical tool in the study of complex sample matrices. A further development and configuration employing Ultra-High Pressure Liquid Chromatography (UHPLC) is optimized to provide the largest known liquid chromatographic resolution and peak capacity. Reasonably UHPLC plays an important role in separation and consequent metabolite identification of complex molecular mixtures such as bio-fluids. The most sensitive detectors for these purposes are mass spectrometers. Almost any mass analyzer can be optimized to identify and quantify small pre-defined sets of targets; however, the number of analytes in metabolomics is far greater. Optimized protocols for quantification of large sets of targets may be rendered inapplicable. Results on small target set analyses on different sample matrices are easily comparable with each other. In non-targeted metabolomics there is almost no analytical method which is applicable to all different matrices due to limitations pertaining to mass analyzers and chromatographic tools. The specifications of the most important interfaces and mass analyzers are discussed. We additionally provide an exemplary application in order to demonstrate the level of complexity which remains intractable up to date. The potential of coupling a high field Fourier Transform Ion Cyclotron Resonance Mass Spectrometer (ICR-FT/MS), the mass analyzer with the largest known mass resolving power, to UHPLC is given with an example of one human pre-treated plasma sample. This experimental example illustrates one way of overcoming the necessity of faster scanning rates in the coupling with UHPLC. The experiment enabled the extraction of thousands of features (analytical signals). A small subset of this compositional space could be mapped into a mass difference network whose topology shows specificity toward putative metabolite classes and retention time.
机译:本综述介绍了代谢组学的概念,并概述了应用于非目标代谢组学的分析工具,重点是液相色谱法(LC)。 LC是研究复杂样品基质的有力分析工具。优化了采用超高压液相色谱(UHPLC)的进一步开发和配置,以提供最大的已知液相色谱分辨率和峰容量。合理地,UHPLC在分离和随后的代谢物鉴定复杂分子混合物(例如生物流体)中起着重要作用。用于这些目的的最灵敏的检测器是质谱仪。几乎所有质量分析仪都可以进行优化,以识别和量化小的预定义目标集;但是,代谢组学中的分析物数量要多得多。用于量化大量靶标的优化方案可能不适用。在不同样品基质上进行小目标集分析的结果很容易相互比较。在非靶向代谢组学中,由于质量分析仪和色谱分析工具的局限性,几乎没有适用于所有不同基质的分析方法。讨论了最重要的接口和质量分析器的规格。我们另外提供了一个示例性应用程序,以演示迄今为止仍然难以解决的复杂性水平。以一个人类预处理血浆样品为例,给出了将高场傅立叶变换离子回旋共振质谱仪(ICR-FT / MS)(具有最大已知质量分辨能力的质量分析仪)与UHPLC耦合的潜力。该实验示例说明了一种克服与UHPLC耦合使用更快扫描速率的必要性的方法。实验能够提取数千个特征(分析信号)。该组成空间的一小部分可以映射到质量差异网络中,该质量差异网络的拓扑结构显示出对假定的代谢物类别和保留时间的特异性。

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