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Assessing the impact of the duration and intensity of inhalation exposure on the magnitude of the variability of internal dose metrics in children and adults

机译:评估吸入暴露的持续时间和强度对儿童和成人内部剂量指标变化幅度的影响

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摘要

The objective of this study was to assess the impact of the exposure duration and intensity on the human kinetic adjustment factor (HKAF). A physiologically based pharmacokinetic model was used to compute target dose metrics (i.e. maximum blood concentration (C max) and amount metabolized/L liver/24h (Amet)) in adults, neonates (0-30 days), toddlers (13 years), and pregnant women following inhalation exposure to benzene, styrene, 1,1,1-trichloroethane and 1,4-dioxane. Exposure scenarios simulated involved various concentrations based on the chemical's reference concentration (low) and six of U.S. EPA's Acute Exposure Guideline Levels (AEGLs) (high), for durations of 10min, 60min, 8h, and 24h, as well as at steady-state. Distributions for body weight (BW), height (H), and hepatic CYP2E1 content were obtained from the literature or from P3M software, whereas blood flows and tissue volumes were calculated from BW and H. The HKAF was computed based on distributions of dose metrics obtained by Monte Carlo simulations [95th percentile in each subpopulation/median in adults]. At low levels of exposure, ranges of C max -based HKAF were 1-6.8 depending on the chemical, with 1,4-dioxane exhibiting the greatest values. At high levels of exposure, this range was 1.1-5.2, with styrene exhibiting the greatest value. Neonates were always the most sensitive subpopulation based on C max, and pregnant women were most sensitive based on Amet in the majority of the cases (1.3-2.1). These results have shown that the chemical-specific HKAF varies as a function of exposure duration and intensity of inhalation exposures, and sometimes exceeds the default value used in risk assessments.
机译:这项研究的目的是评估暴露时间和强度对人体动力学调节因子(HKAF)的影响。使用基于生理学的药代动力学模型来计算成人,新生儿(0-30天),学步儿童(13岁),和孕妇吸入苯,苯乙烯,1,1,1-三氯乙烷和1,4-二恶烷后。模拟的暴露场景涉及基于化学物质的参考浓度(低)和美国EPA急性暴露指导水平(AEGL)中的六种(高)的各种浓度,持续时间分别为10min,60min,8h和24h,并且处于稳态。体重(BW),身高(H)和肝CYP2E1含量的分布是从文献或P3M软件获得的,而血流量和组织体积是从体重和H来计算的.HKAF是根据剂量指标的分布计算的通过蒙特卡洛模拟获得的数据[成人每个亚群/中位数的95%百分位数]。在低暴露水平下,基于C max的HKAF范围取决于化学物质,为1-6.8,其中1,4-二恶烷显示出最大值。在高暴露水平下,该范围为1.1-5.2,其中苯乙烯表现出最大值。基于C max,新生儿始终是最敏感的亚群,在大多数情况下,孕妇基于Amet最为敏感(1.3-2.1)。这些结果表明,特定于化学品的HKAF随暴露时间和吸入暴露强度而变化,有时超过风险评估中使用的默认值。

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