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采用 13C-/12C-同位素Dansyl 标记结合液相色谱傅里叶变换离子回旋共振质谱联用技术对人脑脊液进行定性代谢组学分析。

Qualitative metabolome analysis of human cerebrospinal fluid by 13C-/12C-isotope dansylation labeling combined with liquid chromatography Fourier transform ion cyclotron resonance mass spectrometry.

机构信息

Department of Chemistry, University of Alberta, Edmonton, Alberta, T6G 2G2, Canada.

出版信息

J Am Soc Mass Spectrom. 2011 Feb;22(2):339-47. doi: 10.1007/s13361-010-0033-4. Epub 2011 Jan 27.

Abstract

Metabolome analysis of human cerebrospinal fluid (CSF) is challenging because of low abundance of metabolites present in a small volume of sample. We describe and apply a sensitive isotope labeling LC-MS technique for qualitative analysis of the CSF metabolome. After a CSF sample is divided into two aliquots, they are labeled by (13)C-dansyl and (12)C-dansyl chloride, respectively. The differentially labeled aliquots are then mixed and subjected to LC-MS using Fourier-transform ion cyclotron resonance mass spectrometry (FTICR MS). Dansylation offers significant improvement in the performance of chromatography separation and detection sensitivity. Moreover, peaks detected in the mass spectra can be readily analyzed for ion pair recognition and database search based on accurate mass and/or retention time information. It is shown that about 14,000 features can be detected in a 25-min LC-FTICR MS run of a dansyl-labeled CSF sample, from which about 500 metabolites can be profiled. Results from four CSF samples are compared to gauge the detectability of metabolites by this method. About 261 metabolites are commonly detected in replicate runs of four samples. In total, 1132 unique metabolite ion pairs are detected and 347 pairs (31%) matched with at least one metabolite in the Human Metabolome Database. We also report a dansylation library of 220 standard compounds and, using this library, about 85 metabolites can be positively identified. Among them, 21 metabolites have never been reported to be associated with CSF. These results illustrate that the dansylation LC-FTICR MS method can be used to analyze the CSF metabolome in a more comprehensive manner.

摘要

对人脑脊液 (CSF) 的代谢组学分析具有挑战性,因为存在于小体积样本中的代谢物丰度低。我们描述并应用了一种灵敏的同位素标记 LC-MS 技术,用于 CSF 代谢组的定性分析。CSF 样品分为两份后,分别用 (13)C-丹磺酰氯和 (12)C-丹磺酰氯进行标记。然后将标记的两份 CSF 混合,使用傅里叶变换离子回旋共振质谱(FTICR MS)进行 LC-MS 分析。丹磺酰化可显著提高色谱分离和检测灵敏度。此外,基于精确质量和/或保留时间信息,可以轻松分析质谱中检测到的峰,以进行离子对识别和数据库搜索。结果表明,对丹磺酰化 CSF 样品进行 25 分钟的 LC-FTICR MS 运行,可检测到约 14000 个特征峰,其中约 500 个代谢物可进行谱图分析。对四个 CSF 样品的结果进行比较,以评估该方法对代谢物的检测能力。四个样本的重复运行中共同检测到约 261 种代谢物。总共检测到 1132 个独特的代谢物离子对,其中 347 对(31%)与人类代谢组数据库中至少一种代谢物匹配。我们还报告了一个包含 220 种标准化合物的丹磺酰化文库,使用该文库可以对约 85 种代谢物进行阳性鉴定。其中,21 种代谢物从未被报道与 CSF 有关。这些结果表明,丹磺酰化 LC-FTICR MS 方法可用于更全面地分析 CSF 代谢组。

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