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采用 SPE-prepLC-MS-LC-MS-NMR 法从黑茶消费者尿液中分离得到的共轭缬草酸代谢物的全氢和碳 NMR 谱分配

Full H and C NMR spectral assignment of conjugated valerolactone metabolites isolated from urine of black tea consumers by means of SPE-prepLC-MS-LC-MS-NMR.

机构信息

Spectroscopy & Imaging, Unilever Research and Development Vlaardingen, Vlaardingen, The Netherlands.

Laboratory of Biophysics, Wageningen University and Research, Wageningen, The Netherlands.

出版信息

Magn Reson Chem. 2019 Sep;57(9):548-557. doi: 10.1002/mrc.4833. Epub 2019 Mar 19.

DOI:10.1002/mrc.4833
PMID:30658005
Abstract

The health benefits of black tea have been linked to polyphenol metabolites that target specific modes of action in the human body. A major bottleneck in unravelling the underlying mechanisms is the preparative isolation of these metabolites, which hampers their structural elucidation and assessment of in vitro bioactivity. A solid phase extraction (SPE)-preparative liquid chromatography (prepLC)-MS-LC-MS-NMR workflow was implemented for preparative isolation of conjugated valerolactone metabolites of catechin-based polyphenols from urine of black tea consumers. First, the urine was cleaned and preconcentrated using an SPE method. Subsequently, the clean urine concentrate was injected on a preparative LC column, and conjugated valerolactones were obtained by MS-guided collection. Reconstituted fractions were further separated on an analytical LC column, and valerolactone fractions were collected in an MS-guided manner. These were reconstituted in methanol-d and identified and quantified using 1D and 2D homo- and hetereonuclear NMR experiments (at a field strength of 14.1 T), in combination with mass spectrometry. This resulted in the full spectral H and C NMR assignments of five conjugated valerolactones. These metabolites were collected in quantities of 8-160 μg and purities of 70-91%. The SPE-prepLC-MS-LC-MS-NMR workflow is suitable for isolating metabolites that occur at sub-μM concentrations in a complex biofluid such as urine. The workflow also provides an alternative for cumbersome and expensive de novo synthesis of tea metabolites for testing in bioactivity assays or for use as authentic analytical standards for quantification by mass spectrometry.

摘要

红茶对健康的益处与多酚代谢物有关,这些代谢物针对人体的特定作用模式。阐明其潜在机制的主要瓶颈是这些代谢物的制备性分离,这阻碍了它们的结构阐明和体外生物活性评估。我们实施了固相萃取 (SPE)-制备液相色谱 (prepLC)-MS-LC-MS-NMR 工作流程,从红茶消费者的尿液中分离儿茶素基多酚的共轭缬草酸内酯代谢物。首先,使用 SPE 方法对尿液进行清洗和预浓缩。随后,将清洁的尿液浓缩物注入制备 LC 柱,通过 MS 引导收集共轭缬草酸内酯。重组馏分在分析 LC 柱上进一步分离,以 MS 引导方式收集缬草酸内酯馏分。这些在甲醇-d 中重建,并使用 1D 和 2D 同核和异核 NMR 实验(场强为 14.1 T)进行鉴定和定量,结合质谱。这导致了五个共轭缬草酸内酯的全谱 H 和 C NMR 分配。这些代谢物的收集量为 8-160 μg,纯度为 70-91%。SPE-prepLC-MS-LC-MS-NMR 工作流程适用于从尿液等复杂生物流体中以亚 μM 浓度存在的代谢物的分离。该工作流程还为茶代谢物的繁琐和昂贵的从头合成提供了替代方法,用于生物活性测定的测试,或用作通过质谱定量的真实分析标准。

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