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Expanding the Limits of Human Blood Metabolite Quantitation Using NMR Spectroscopy

机译:使用NMR光谱扩大人类血液代谢物定量的范围

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A current challenge in metabolomics is the reliable quantitation of many metabolites. Limited resolution and sensitivity combined with the challenges associated with unknown metabolite identification have restricted both the number and the quantitative accuracy of blood metabolites. Focused on alleviating this bottleneck in NMR-based metabolomics, investigations of pooled human serum combining an array of 1D/2D NMR experiments at 800 MHz, database searches, and spiking with authentic compounds enabled the identification of 67 blood metabolites. Many of these (similar to 1/3) are new compared with those reported previously as a part of the Human Serum Metabolome Database. In addition, considering both the high reproducibility and quantitative nature of NMR as well as the sensitivity of NMR chemical shifts to altered sample conditions, experimental protocols and comprehensive peak annotations are provided here as a guide for identification and quantitation of the new pool of blood metabolites for routine applications. Further, investigations focused on the evaluation of quantitation using organic solvents revealed a surprisingly poor performance for protein precipitation using acetonitrile. One-third of the detected metabolites were attenuated by 10-67% compared with methanol precipitation at the same solvent-to-serum ratio of 2:1 (v/v). Nearly 2/3 of the metabolites were further attenuated by up to 65% upon increasing the acetonitrile-to-serum ratio to 4:1 (v/v). These results, combined with the newly established identity for many unknown metabolites in the NMR spectrum, offer new avenues for human serum/plasma-based metabolomics. Further, the ability to quantitatively evaluate nearly 70 blood metabolites that represent numerous classes, including amino acids, organic acids, carbohydrates, and heterocyclic compounds, using a simple and highly reproducible analytical method such as NMR may potentially guide the evaluation of samples for analysis using mass spectrometry.
机译:代谢组学当前面临的挑战是对许多代谢物的可靠定量。有限的分辨率和灵敏度以及与未知代谢物鉴定相关的挑战限制了血液代谢物的数量和定量准确性。致力于减轻基于NMR的代谢组学中的瓶颈,对合并的人血清进行的研究结合了800 MHz处的一系列1D / 2D NMR实验,数据库搜索以及掺入可靠的化合物,从而可以鉴定67种血液代谢物。与以前作为人类血清代谢组数据库的一部分报道的那些相比,其中许多(类似于1/3)是新的。此外,考虑到NMR的高重现性和定量性质以及NMR化学位移对改变的样品条件的敏感性,此处提供实验方案和全面的峰注释,作为鉴定和定量新的血液代谢物池的指南用于常规应用。此外,针对使用有机溶剂进行定量评估的研究表明,使用乙腈进行蛋白质沉淀的性能出乎意料地差。在相同的溶剂与血清比率为2:1(v / v)的情况下,与甲醇沉淀相比,检测到的代谢物的三分之一衰减了10-67%。将乙腈与血清的比例提高至4:1(v / v)后,近2/3的代谢产物进一步减弱了多达65%。这些结果与NMR光谱中许多未知代谢物的新建立身份相结合,为基于人血清/血浆的代谢组学提供了新途径。此外,使用简单且高度可重复的分析方法(例如NMR)对包括氨基酸,有机酸,碳水化合物和杂环化合物在内的近70种血液代谢产物(包括氨基酸,有机酸,碳水化合物和杂环化合物)进行定量评估的能力可能会指导使用以下方法对样品进行评估:质谱。

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