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首页> 外文期刊>Journal of chromatography, B. Analytical technologies in the biomedical and life sciences >Quantitation of phenanthrene dihydrodiols in the urine of smokers and nonsmokers by gas chromatography-negative ion chemical ionization-tandem mass spectrometry
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Quantitation of phenanthrene dihydrodiols in the urine of smokers and nonsmokers by gas chromatography-negative ion chemical ionization-tandem mass spectrometry

机译:通过气相色谱 - 负离子化学离子电离 - 串联质谱法定量吸烟者和非吸烟者尿液中的菲二氢醇的定量

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摘要

Polycyclic aromatic hydrocarbons (PAH) are well-established environmental carcinogens likely to be causative agents for some human cancers. Bay-region diol epoxides are ultimate carcinogenic metabolites of multiple PAH. Dihydrodiols are the important intermediate products of this pathway and can be further oxidized to form diol epoxides. We quantified two dihydrodiol metabolites of phenanthrene (Phe), the simplest PAH with a bayregion, in the 6 h urine of smokers (N = 25) and non-smokers (N = 25) using a newly developed and validated analytical method. After hydrolysis ss-glucuronidase and sulfatase, and solid phase extraction, the sample was silylated and analyzed by gas chromatography-negative ion chemical ionization-tandem mass spectrometry (GC-NICI-MS/MS). Levels (nmol/6h urine) of Phe-1,2-dihydrodiol (Phe-1,2-D) and Phe-3,4-dihydrodiol (Phe-3,4-D) were 2.04 +/- 1.52 and 0.51 +/- 0.35 , respectively, in smokers, significantly higher than those in non-smokers (1.35 +/- 1.11 of Phe-1,2-D, p < 0.05; 0.27 +/- 0.25 of Phe-3,4-D, p < 0.005). Cigarette smoking also influenced the regioselective metabolism of Phe, presenting as a significant difference in the urinary distribution pattern of Phe-1,2-D and Phe-3,4-D between smokers and non-smokers: the ratio Phe-3,4-D: Phe-1,2-D increased from 0.20 in non-smokers to 0.28 in smokers (p < 0.01), which can be explained by the induction of the phenanthrene metabolizing enzymes CYP1A2 and CYP1B1 by cigarette smoke. The method described here is the first example of facile quantitation of an intact human dihydrodiol metabolite of any PAH with three or more aromatic rings and will be applicable in clinical and molecular epidemiology studies of PAH metabolism and cancer susceptibility.
机译:多环芳烃(PAH)是良好的环境致癌物质,可能是一些人类癌症的致病药物。海湾区二醇环氧化物是多个PAH的最终致癌代谢物。二氢醇是该途径的重要中间产物,可以进一步氧化以形成二醇环氧化物。我们量化了两种二氢醇代谢物,菲丙烯(PHE),最简单的PAH与BayRegion,在吸烟者(n = 25)和非吸烟者(n = 25)中使用新开发和经过验证的分析方法。水解SS-葡糖醛酸酶和硫酸酶和固相萃取后,将样品甲硅烷基化并通过气相色谱 - 负离子化学电离 - 串联质谱法(GC-Nici-MS / MS)分析。 PHE-1,2-二水二醇(PHE-1,2-D)和PHE-3,4-二氢醇(PHE-3,4-D)的水平(Nmol / 6h尿液)为2.04 +/- 1.52和0.51 + / - 0.35分别在吸烟者中,显着高于非吸烟者(1.35 +/- 1.11的PHE-1,2-D,P <0.05; 0.27 +/- 0.25,PHE-3,4-D, P <0.005)。吸烟也影响了PHE的区域选择性代谢,呈现为吸烟者和非吸烟者之间PHE-1,2-D和PHE-3,4-D的尿发分布模式的显着差异:PHE-3,4的比例-D:PHE-1,2-D在吸烟者中从0.20增加到0.28(P <0.01),可以通过香烟烟雾诱导菲施菲代谢酶CYP1A2和CYP1B1的诱导来解释。这里描述的方法是具有三种或更多种芳环的任何PAH的完整的人二水二醇代谢物的容易定量的第一例,并且适用于PAH代谢和癌症易感性的临床和分子流行病学研究。

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