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Quantitative Profiling of Polar Cationic Metabolites in Human Cerebrospinal Fluid by Reversed-Phase Nanoliquid Chromatography/Mass Spectrometry

机译:反相纳米液相色谱/质谱法定量分析人脑脊髓液中极性阳离子代谢产物

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Reversed-phase (RP) nanoliquid chromatography (LC)/mass spectrometry (MS) is widely used for proteome analysis, but hydrophilic metabolites are poorly retained on RP columns. We describe here the development and application of an efficient, robust, and quantitative nano-LC/MS method for cationic metabolome analysis in the positive ionization mode without any derivatization of analytes. Various stationary phases for nano-LC, coating of the internal wall of the capillary column, and various mobile phases were evaluated in terms of separation and peak shapes for 33 hydrophilic metabolites, including nonderivatized amino acids. Polar cationic compounds were strongly bound to mixed-functional RP with cation exchange mode resin, and the best separation was obtained with hydrophilic internal wall coating and a two-step trifluoroacetic acid (TFA) gradient in methanol as the mobile phase. Simple, but optimized, sample processing and the use of a high content of methanol allowed robust nano-LC/MS analysis. Our developed method was applied for biomarker discovery in Alzheimer's disease (AD). Several hundred peaks were detected from 10 (mu)L of cerebrospinal fluid (CSF). In a principal component analysis (PCA) plot using peak intensities without normalization, peak separation depended on the experimental date, not disease state. Therefore, constant amounts of two stable isotope-labeled amino acids, Val and Lys, were added as internal standards (ISs) to each sample before processing. These ISs were eluted in different gradient slopes in the two-step gradient, and the normalized peak ratios using the corresponding ISs gave a unique group of PCA scores which could distinguish AD CSF samples from age-matched control CSF samples.
机译:反相(RP)纳米液相色谱(LC)/质谱(MS)被广泛用于蛋白质组分析,但是亲水性代谢物很少保留在RP色谱柱上。我们在这里描述了在阳离子电离模式下无需任何分析物衍生化的高效,稳健和定量的纳米LC / MS方法的发展和应用,用于阳离子代谢组学分析。根据33种亲水性代谢物(包括未衍生化的氨基酸)的分离和峰形,评估了纳米LC的各种固定相,毛细管柱内壁的涂层以及各种流动相。极性阳离子化合物与阳离子交换模式树脂牢固地结合在混合功能RP上,使用亲水性内壁涂层和​​甲醇中的两步三氟乙酸(TFA)梯度作为流动相可获得最佳分离效果。简单但经过优化的样品处理过程以及高含量甲醇的使用使得纳米LC / MS的分析更为可靠。我们开发的方法用于阿尔茨海默氏病(AD)中的生物标记物发现。从10μL脑脊液(CSF)中检测到数百个峰。在使用峰强度而不进行归一化的主成分分析(PCA)图中,峰分离取决于实验日期,而不取决于疾病状态。因此,在处理之前,将恒定量的两个稳定同位素标记的氨基酸Val和Lys作为内标(IS)添加到每个样品中。这些IS在两步梯度中以不同的梯度斜率洗脱,并且使用相应IS的归一化峰比率给出了一组独特的PCA评分,可以区分AD CSF样品和年龄匹配的对照CSF样品。

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