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Methodologies for the quantitative estimation of toxicant dose to cigarette smokers using physical chemical and bioanalytical data

机译:使用物理化学和生物分析数据定量估算吸烟者有毒物质剂量的方法

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摘要

Methodologies have been developed, described and demonstrated that convert mouth exposure estimates of cigarette smoke constituents to dose by accounting for smoke spilled from the mouth prior to inhalation (mouth-spill (MS)) and the respiratory retention (RR) during the inhalation cycle. The methodologies are applicable to just about any chemical compound in cigarette smoke that can be measured analytically and can be used with ambulatory population studies. Conversion of exposure to dose improves the relevancy for risk assessment paradigms. Except for urinary nicotine plus metabolites, biomarkers generally do not provide quantitative exposure or dose estimates. In addition, many smoke constituents have no reliable biomarkers. We describe methods to estimate the RR of chemical compounds in smoke based on their vapor pressure (VP) and to estimate the MS for a given subject. Data from two clinical studies were used to demonstrate dose estimation for 13 compounds, of which only 3 have urinary biomarkers. Compounds with VP > 10−5 Pa generally have RRs of 88% or greater, which do not vary appreciably with inhalation volume (IV). Compounds with VP < 10−7 Pa generally have RRs dependent on IV and lung exposure time. For MS, mean subject values from both studies were slightly greater than 30%. For constituents with urinary biomarkers, correlations with the calculated dose were significantly improved over correlations with mouth exposure. Of toxicological importance is that the dose correlations provide an estimate of the metabolic conversion of a constituent to its respective biomarker.
机译:已经开发,描述和证明了通过考虑吸入之前从嘴中溢出的烟雾(口溢(MS))和吸入周期中的呼吸保持力(RR),将香烟烟雾成分的口腔暴露估计值转换为剂量的方法。该方法学适用于卷烟烟雾中的几乎所有化合物,这些化合物可以进行分析测量并可以用于非流动人口研究。暴露量转换为剂量可以改善风险评估范式的相关性。除了尿中的尼古丁加代谢物外,生物标志物通常不提供定量暴露或剂量估计。此外,许多烟雾成分没有可靠的生物标记。我们介绍了根据烟雾的蒸气压(VP)估算化学物质的RR并估算给定对象的MS的方法。来自两项临床研究的数据用于证明13种化合物的剂量估算,其中只有3种具有尿液生物标志物。 VP> 10 −5 Pa的化合物的RR通常为88%或更高,并且随吸入量(IV)的变化不大。 VP <10 −7 Pa的化合物通常具有取决于IV和肺部暴露时间的RR。对于MS,两项研究的平均受试者价值均略高于30%。对于具有尿液生物标志物的成分,与计算剂量的相关性明显优于与口腔暴露的相关性。毒理学重要性在于剂量相关性提供了组分向其相应生物标记物代谢转化的估计。

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