首页> 美国卫生研究院文献>Environmental Health Perspectives >Physiologically based toxicokinetic modeling of 13-butadiene lung metabolism in mice becomes more important at low doses.
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Physiologically based toxicokinetic modeling of 13-butadiene lung metabolism in mice becomes more important at low doses.

机译:低剂量时小鼠13丁二烯肺部代谢的基于生理的毒代动力学模型变得更加重要。

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摘要

This paper describes a physiologically based toxicokinetic model for 1,3-butadiene uptake, distribution, and metabolic clearance in mice. Model parameters for metabolic activity were estimated from the correspondence between computer simulation studies and experimental results as published in the literature. The parameterized model was validated with independent literature data. With the resulting model, the relative importance of lung metabolism as compared to metabolism in the liver increased with decreasing ambient air concentrations. This was due to saturation of metabolism in the alveolar area of the lung, which occurred in the simulations at ambient air concentrations well below current threshold limit values. At higher air concentration, liver metabolism became relatively more important. The tendency toward increased importance of lung metabolism at low doses indicates the necessity of careful extrapolation of in vivo results to low doses. Moreover, this trend may also contribute to species difference in susceptibility to the carcinogenic activity of butadiene.
机译:这篇论文描述了小鼠中1,3-丁二烯摄取,分布和代谢清除的基于生理学的毒物动力学模型。代谢活性的模型参数是根据计算机模拟研究与实验结果之间的对应关系(如文献中所述)估算的。参数化模型已通过独立文献数据验证。使用生成的模型,与肝脏中的代谢相比,肺部代谢的相对重要性随环境空气浓度的降低而增加。这是由于肺的肺泡区域中的新陈代谢饱和所致,该饱和在模拟中发生在环境空气浓度远低于当前阈值极限值的情况下。在较高的空气浓度下,肝脏代谢变得相对更重要。低剂量时肺代谢重要性越来越高的趋势表明,必须将体内结果小心地外推至低剂量。而且,这种趋势也可能导致对丁二烯致癌活性的敏感性差异。

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