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对一般人群中多环芳烃和 ET 的暴露进行环境和生物监测。

Environmental and biological monitoring of exposures to PAHs and ETS in the general population.

机构信息

Division of Environmental Health & Risk Management, School of Geography, Earth & Environmental Sciences, University of Birmingham, Edgbaston, Birmingham B15 2TT, United Kingdom.

出版信息

Environ Int. 2010 Oct;36(7):763-71. doi: 10.1016/j.envint.2010.05.015. Epub 2010 Jun 29.

Abstract

The objective of this study was to analyse environmental tobacco smoke (ETS) and PAH metabolites in urine samples of non-occupationally exposed non-smoker adult subjects and to establish relationships between airborne exposures and urinary concentrations in order to (a) assess the suitability of the studied metabolites as biomarkers of PAH and ETS, (b) study the use of 3-ethenypyridine as ETS tracer and (c) link ETS scenarios with exposures to carcinogenic PAH and VOC. Urine samples from 100 subjects were collected and concentrations of monophenolic metabolites of naphthalene, fluorene, phenanthrene, and pyrene and the nicotine metabolites cotinine and trans-3'-hydroxycotinine were measured using liquid chromatography-tandem mass spectrometry (LC-MS/MS) to assess PAH and ETS exposures. Airborne exposures were measured using personal exposure samplers and analysed using GC-MS. These included 1,3-butadiene (BUT), 3-ethenylpyridine (3-EP) (a tobacco-specific tracer derived from nicotine pyrolysis) and PAHs. ETS was reported by the subjects in 30-min time-activity questionnaires and specific comments were collected in an ETS questionnaire each time ETS exposure occurred. The values of 3-EP (>0.25 microg/m(3) for ETS) were used to confirm the ETS exposure status of the subject. Concentrations as geometric mean, GM, and standard deviation (GSD) of personal exposures were 0.16 (5.50)microg/m(3) for 3-EP, 0.22 (4.28)microg/m(3) for BUT and 0.09 (3.03)ng/m(3) for benzo(a)pyrene. Concentrations of urinary metabolites were 0.44 (1.70)ng/mL for 1-hydroxypyrene and 0.88 (5.28)ng/mL for cotinine. Concentrations of urinary metabolites of nicotine were lower than in most previous studies, suggesting very low exposures in the ETS-exposed group. Nonetheless, concentrations were higher in the ETS population for cotinine, trans-3'hydroxycotinine, 3-EP, BUT and most high molecular weight PAH, whilst 2-hydroxyphenanthrene, 3+4-hydroxyphenanthrene and 1-hydroxyphenanthrene were only higher in the high-ETS subpopulation. There were not many significant correlations between either personal exposures to PAH and their urinary metabolites, or of the latter with ETS markers. However, it was found that the urinary log cotinine concentration showed significant correlation with log concentrations of 3-EP (R=0.75), BUT (R=0.47), and high molecular weight PAHs (MW>200), especially chrysene (R=0.55) at the p=0.01 level. On the other hand, low correlation was observed between the PAH metabolite 2-naphthol and the parent PAH, gas-phase naphthalene. These results suggest that (1) ETS is a significant source of inhalation exposure to the carcinogen 1,3-butadiene and high molecular weight PAHs, many of which are carcinogenic, and (2) that for lower molecular weight PAHs such as naphthalene, exposure by routes other than inhalation predominate, since metabolite levels correlated poorly with personal exposure air sampling.

摘要

本研究旨在分析非职业性暴露非吸烟者的尿液样本中的环境烟草烟雾(ETS)和多环芳烃(PAH)代谢物,并建立空气暴露与尿液浓度之间的关系,以(a)评估所研究代谢物作为 PAH 和 ETS 生物标志物的适用性,(b)研究 3-乙烯基吡啶作为 ETS 示踪剂的用途,以及(c)将 ETS 情况与致癌性 PAH 和 VOC 的暴露联系起来。收集了 100 名受试者的尿液样本,并使用液相色谱-串联质谱法(LC-MS/MS)测量了萘、芴、菲和芘的单酚代谢物以及尼古丁代谢物可替宁和反式-3'-羟基可替宁的浓度,以评估 PAH 和 ETS 暴露情况。使用个人暴露采样器测量空气暴露情况,并使用 GC-MS 进行分析。这些包括 1,3-丁二烯(BUT)、3-乙烯基吡啶(3-EP)(一种源自尼古丁热解的烟草特异性示踪剂)和 PAHs。受试者在 30 分钟的时间活动问卷中报告 ETS,并在每次发生 ETS 暴露时在 ETS 问卷中收集具体意见。3-EP(>0.25 μg/m3 用于 ETS)的值用于确认受试者的 ETS 暴露状态。个人暴露的浓度为几何平均值 GM 和标准差(GSD),3-EP 为 0.16(5.50)μg/m3,BUT 为 0.22(4.28)μg/m3,苯并(a)芘为 0.09(3.03)ng/m3。尿代谢物浓度为 1-羟基芘为 0.44(1.70)ng/mL,可替宁为 0.88(5.28)ng/mL。尼古丁尿代谢物的浓度低于大多数先前的研究,这表明 ETS 暴露组的暴露水平非常低。尽管如此,在 ETS 人群中,可替宁、反式-3'-羟基可替宁、3-EP、BUT 和大多数高分子量 PAH 的浓度更高,而 2-羟基菲、3+4-羟基菲和 1-羟基菲仅在高 ETS 亚群中更高。PAH 及其尿代谢物的个人暴露与尿代谢物之间,或与 ETS 标志物之间,并没有很多显著的相关性。然而,发现尿可替宁浓度的对数与 3-EP(R=0.75)、BUT(R=0.47)和高分子量 PAHs(MW>200)的对数浓度呈显著相关性,尤其是苊(R=0.55),p=0.01。另一方面,2-萘酚与母体 PAH、气相萘的相关性较低。这些结果表明,(1)ETS 是吸入 1,3-丁二烯和高分子量 PAHs(其中许多是致癌物质)的重要致癌源,(2)对于萘等低分子量 PAH,吸入以外的途径是主要暴露途径,因为代谢物水平与个人暴露空气采样相关性较差。

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