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大鼠吸入甲苯急性行为效应的剂量学分析。

A dosimetric analysis of the acute behavioral effects of inhaled toluene in rats.

作者信息

Bushnell Philip J, Oshiro Wendy M, Samsam Tracey E, Benignus Vernon A, Krantz Quentin Todd, Kenyon Elaina M

机构信息

Neurotoxicology Division, National Health and Environmental Effects Research Laboratory, U.S. Environmental Protection Agency, Research Triangle Park, NC 27711, USA.

出版信息

Toxicol Sci. 2007 Sep;99(1):181-9. doi: 10.1093/toxsci/kfm146. Epub 2007 Jun 4.

Abstract

Knowledge of the appropriate metric of dose for a toxic chemical facilitates quantitative extrapolation of toxicity observed in the laboratory to the risk of adverse effects in the human population. Here, we utilize a physiologically based toxicokinetic (PBTK) model for toluene, a common volatile organic compound (VOC), to illustrate that its acute behavioral effects in rats can be quantitatively predicted on the basis of its concentration in the brain. Rats previously trained to perform a visual signal detection task for food reward performed the task while inhaling toluene (0, 1200, 1600, 2000, and 2400 ppm in different test sessions). Accuracy and speed of responding were both decreased by toluene; the magnitude of these effects increased with increasing concentration of the vapor and with increasing duration of exposure. Converting the exposure conditions to brain toluene concentration using the PBTK model yielded a family of overlapping curves for each end point, illustrating that the effects of toluene can be described quantitatively by its internal dose at the time of behavioral assessment. No other dose metric, including inhaled toluene concentration, duration of exposure, the area under the curve of either exposure (ppm h), or modeled brain toluene concentration (mg-h/kg), provided unambiguous predictions of effect. Thus, the acute behavioral effects of toluene (and of other VOCs with a similar mode of action) can be predicted for complex exposure scenarios by simulations that estimate the concentration of the VOC in the brain from the exposure scenario.

摘要

了解有毒化学物质的适当剂量指标有助于将实验室观察到的毒性定量外推至人群中不良反应的风险。在此,我们利用一种基于生理学的甲苯毒代动力学(PBTK)模型,甲苯是一种常见的挥发性有机化合物(VOC),以说明其在大鼠中的急性行为效应可根据其在大脑中的浓度进行定量预测。先前经过训练以执行视觉信号检测任务以获取食物奖励的大鼠,在吸入甲苯(在不同测试时段分别为0、1200、1600、2000和2400 ppm)时执行该任务。甲苯降低了反应的准确性和速度;这些效应的程度随着蒸汽浓度的增加和暴露时间的延长而增加。使用PBTK模型将暴露条件转换为大脑甲苯浓度,对于每个终点都产生了一组重叠曲线,说明甲苯的效应可通过行为评估时的内剂量进行定量描述。没有其他剂量指标,包括吸入甲苯浓度、暴露持续时间、任何一种暴露的曲线下面积(ppm·h)或模拟的大脑甲苯浓度(mg·h/kg),能提供明确的效应预测。因此,对于复杂的暴露场景,通过根据暴露场景估算VOC在大脑中的浓度的模拟,可以预测甲苯(以及具有类似作用模式的其他VOC)的急性行为效应。

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