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通过统计全相关(核磁共振)光谱法在分子流行病学研究中检测尿液药物代谢物(外源代谢组)特征。

Detection of urinary drug metabolite (xenometabolome) signatures in molecular epidemiology studies via statistical total correlation (NMR) spectroscopy.

作者信息

Holmes Elaine, Loo Ruey Leng, Cloarec Olivier, Coen Muireann, Tang Huiru, Maibaum Elaine, Bruce Stephen, Chan Queenie, Elliott Paul, Stamler Jeremiah, Wilson Ian D, Lindon John C, Nicholson Jeremy K

机构信息

Biomolecular Medicine, Division of Surgery, Oncology, Reproductive Biology and Anaesthetics (SORA), Faculty of Medicine, Imperial College London, SW7 2AZ, UK.

出版信息

Anal Chem. 2007 Apr 1;79(7):2629-40. doi: 10.1021/ac062305n. Epub 2007 Feb 27.

Abstract

Western populations use prescription and nonprescription drugs extensively, but large-scale population usage is rarely assessed objectively in epidemiological studies. Here we apply statistical methods to characterize structural pathway connectivities of metabolites of commonly used drugs detected routinely in 1H NMR spectra of urine in a human population study. 1H NMR spectra were measured for two groups of urine samples obtained from U.S. participants in a known population study. The novel application of a statistical total correlation spectroscopy (STOCSY) approach enabled rapid identification of the major and certain minor drug metabolites in common use in the population, in particular, from acetaminophen and ibuprofen metabolites. This work shows that statistical connectivities between drug metabolites can be established in routine "high-throughput" NMR screening of human samples from participants who have randomly self-administered drugs. This approach should be of value in considering interpopulation patterns of drug metabolism in epidemiological and pharmacogenetic studies.

摘要

西方人群广泛使用处方药和非处方药,但在流行病学研究中,很少对大规模人群的用药情况进行客观评估。在此,我们运用统计方法,在一项人群研究中,对尿液1H NMR谱中常规检测到的常用药物代谢物的结构途径连接性进行表征。对从一项已知人群研究中的美国参与者获取的两组尿液样本进行了1H NMR谱测量。统计全相关谱(STOCSY)方法的新应用能够快速识别该人群中常用的主要和某些次要药物代谢物,特别是对乙酰氨基酚和布洛芬的代谢物。这项工作表明,在对随机自行用药的参与者的人类样本进行常规“高通量”NMR筛查时,可以建立药物代谢物之间的统计连接性。这种方法在考虑流行病学和药物遗传学研究中的人群间药物代谢模式时应具有价值。

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