首页> 外文期刊>Journal of Pharmaceutical and Biomedical Analysis: An International Journal on All Drug-Related Topics in Pharmaceutical, Biomedical and Clinical Analysis >Progress toward automated metabolic profiling of human serum: Comparison of CPMG and gradient-filtered NMR analytical methods
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Progress toward automated metabolic profiling of human serum: Comparison of CPMG and gradient-filtered NMR analytical methods

机译:人血清自动代谢谱分析的进展:CPMG与梯度过滤NMR分析方法的比较

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摘要

The investigation of drug delivery and metabolism requires the analysis of molecules in complicated biological matrices such as human serum. In NMR-based metabonomic analysis, T_2 relaxation editing with a CPMG filter is commonly used to suppress background signals from proteins and other endogenous components. Radio frequency pulse imperfections and incomplete irradiation across the spectral bandwidth can cause phase and baseline distortions in CPMG spectra. These distortions are exacerbated by water suppression techniques. Baseline correction methods included in commercially available data processing software packages may be incapable of producing artifact-free spectra. To increase the analytical precision of metabolic profiling, one NMR spectroscopist may be responsible for manually phasing and baseline correcting hundreds of spectra individually to remove operator-dependent variations, significantly reducing throughput. For metabonomic analysis of human serum, it was observed that the application of a pulsed field gradient filter produced H NMR spectra well suited to automatic phasing routines. Superior baseline characteristics, an increased tolerance to radio frequency pulse imperfections, and improved water suppression were achieved, A concomitant reduction in signal intensity compared with the CPMG method was easily recovered by increasing the number of scans. Principal component analysis (PCA) of spectra, acquired under a variety of experimental conditions, revealed the improved teproducibility and robustness of 'H NMR pulsed field gradient-filtered metabonomic analyses of serum compared to the CPMG method.
机译:药物输送和代谢研究需要分析复杂的生物基质(例如人血清)中的分子。在基于NMR的代谢组学分析中,通常使用CPMG滤镜进行T_2弛豫编辑来抑制蛋白质和其他内源性成分的背景信号。射频脉冲缺陷和整个频谱带宽的不完全照射会导致CPMG频谱出现相位和基线失真。用水抑制技术会加剧这些变形。市售数据处理软件包中包含的基线校正方法可能无法生成无伪影的光谱。为了提高代谢图谱的分析精度,一位NMR光谱学家可能负责手动定相和基线校正数百个光谱,以消除操作员相关的变化,从而显着降低了通量。对于人血清的代谢组学分析,观察到脉冲场梯度滤波器的应用产生了非常适合自动定相程序的1 H NMR光谱。实现了出色的基线特性,增加了对射频脉冲缺陷的耐受性,并改善了水抑制性能。与CPMG方法相比,信号强度的降低可通过增加扫描次数轻松恢复。在各种实验条件下获得的光谱主成分分析(PCA)显示,与CPMG方法相比,1 H NMR脉冲场梯度过滤的血清代谢组学分析具有更高的重复性和鲁棒性。

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