首页> 外文期刊>Inhalation toxicology >A hybrid computational fluid dynamics and physiologically based pharmacokinetic model for comparison of predicted tissue concentrations of acrylic acid and other vapors in the rat and human nasal cavities following inhalation exposure.
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A hybrid computational fluid dynamics and physiologically based pharmacokinetic model for comparison of predicted tissue concentrations of acrylic acid and other vapors in the rat and human nasal cavities following inhalation exposure.

机译:混合计算流体动力学和基于生理学的药代动力学模型,用于比较吸入暴露后大鼠和人鼻腔中丙烯酸和其他蒸气的预测组织浓度。

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摘要

To assist in interspecies dosimetry comparisons for risk assessment of the nasal effects of organic acids, a hybrid computational fluid dynamics (CFD) and physiologically based pharmacokinetic (PBPK) dosimetry model was constructed to estimate the regional tissue dose of inhaled vapors in the rat and human nasal cavity. Application to a specific vapor would involve the incorporation of the chemical-specific reactivity, metabolism, partition coefficients, and diffusivity (in both air and tissue phases) of the vapor. This report describes the structure of the CFD-PBPK model and its application to a representative acidic vapor, acrylic acid, for interspecies tissue concentration comparisons to assist in risk assessment. By using the results from a series of short-term in vivo studies combined with computer modeling, regional nasal tissue dose estimates were developed and comparisons of tissue doses between species were conducted. To make these comparisons, the assumption was made that the susceptibilities of human and rat olfactory epithelium to the cytotoxic effects of organic acids were similar, based on similar histological structure and common mode of action considerations. Interspecies differences in response were therefore assumed to be driven primarily by differences in nasal tissue concentrations that result from regional differences in nasal air flow patterns relative to the species-specific distribution of olfactory epithelium in the nasal cavity. The results of simulations with the seven-compartment CFD-PBPK model suggested that the olfactory epithelium of the human nasal cavity would be exposed to tissue concentrations of acrylic acid similar to that of the rat nasal cavity when the exposure conditions are the same. Similar analysis of CFD data and CFD-PBPK model simulations with a simpler one-compartment model of the whole nasal cavities of rats and humans provides comparable results to averaging over the compartments of the seven-compartment model. These results indicate that the general structure of the hybrid CFD-PBPK model applied in this assessment would be useful for target tissue dosimetry and interspecies dose comparisons for a wide variety of vapors. Because of its flexibility, this CFD-PBPK model is envisioned to be a platform for the construction of case-specific inhalation dosimetry models to simulate in vivo exposures that do not involve significant histopathological damage to the nasal cavity.
机译:为了协助进行种间剂量学比较以评估有机酸对鼻腔的影响,建立了混合计算流体动力学(CFD)和基于生理学的药代动力学(PBPK)剂量学模型,以估计大鼠和人体吸入蒸气的区域组织剂量鼻腔。施加到特定的蒸气上将涉及该蒸气的化学特异性反应性,新陈代谢,分配系数和扩散率(在空气和组织相中)的结合。本报告介绍了CFD-PBPK模型的结构及其在代表性酸性蒸气(丙烯酸)中的应用,以进行种间组织浓度比较,以帮助进行风险评估。通过使用一系列短期体内研究的结果并结合计算机建模,开发了鼻区域组织剂量估计值,并进行了物种间组织剂量的比较。为了进行这些比较,基于相似的组织学结构和共同的作用方式考虑,假设人类和大鼠嗅觉上皮对有机酸的细胞毒性作用的敏感性相似。因此,假定种间反应的差异主要是由鼻组织浓度的差异引起的,鼻组织浓度的差异是由鼻气流模式的区域差异(相对于鼻腔中嗅觉上皮的物种特异性分布)引起的。七室CFD-PBPK模型的模拟结果表明,当暴露条件相同时,人鼻腔的嗅觉上皮将暴露于类似于大鼠鼻腔的丙烯酸组织浓度。用更简单的大鼠和人类整个鼻腔的一室模型对CFD数据和CFD-PBPK模型进行的类似分析,可提供与七室模型的各个室平均相比的可比结果。这些结果表明,此评估中使用的混合CFD-PBPK模型的一般结构将可用于各种蒸汽的目标组织剂量测定和种间剂量比较。由于其灵活性,该CFD-PBPK模型可望成为构建特定病例的吸入剂量模型的平台,以模拟不涉及对鼻腔重大病理损害的体内暴露。

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