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首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Use of a pharmacokinetic model to assess chlorpyrifos exposure and dose in children, based on urinary biomarker measurements.
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Use of a pharmacokinetic model to assess chlorpyrifos exposure and dose in children, based on urinary biomarker measurements.

机译:根据尿液生物标志物的测量,使用药代动力学模型评估儿童的毒死rif暴露量和剂量。

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Chlorpyrifos is a common agricultural insecticide and has been used residentially in the United States until the year 2000 when this use was restricted by the U.S. Environmental Protection Agency (U.S. EPA). A chlorpyrifos metabolite, 3,5,6-trichloro-2-pyridinol (TCPy) has been found in urine samples collected during exposure field studies. In this work, we use urinary biomarker data and the inverse solution of a simple pharmacokinetic (PK) model for chlorpyrifos to estimate the magnitude and timing of doses. Three urine samples were collected on separate days from each of 15 children (ages 3-12) who were participants in the Minnesota Children's Pesticide Exposure Study (MNCPES). The total volume of urine was noted and samples analyzed for TCPY: The urinary data was used along with constraints imposed on dose timing, based on responses of the individuals to pesticide-use surveys. We predicted the time and magnitude of multiple "event" exposures characterized by short-term, relatively high doses superimposed over a continuous background exposure. The average dose of chlorpyrifos predicted by the model was 1.61 microg/kg per reported event. Average background dose rate for these children that reported exposure events was 0.0062 microg/kg/h, or 0.15 microg/kg/day. In addition to predicting the total dose of chlorpyrifos received by an individual from urinary biomarker measurements, the model can then be run in a forward manner once the exposure regime is determined. This will allow the prediction of the total amount of TCPy eliminated in the urine over any time period of interest.
机译:毒死rif是一种常见的农业杀虫剂,直到2000年受到美国环境保护署(U.S. EPA)的限制在美国一直在居民使用。在接触场研究期间收集的尿液样本中发现了毒死rif代谢产物3,5,6-三氯-2-吡啶醇(TCPy)。在这项工作中,我们使用尿液生物标志物数据和毒死rif的简单药代动力学(PK)模型的逆解来估计剂量的大小和时间安排。分别从15名儿童(3-12岁)中分别收集了三个尿液样本,他们是明尼苏达州儿童农药暴露研究(MNCPES)的参与者。记录尿液总量并分析TCPY样品:根据个体对农药使用调查的反应,使用尿液数据以及对剂量时间的限制。我们预测了多次“事件”暴露的时间和强度,其特征是短期,相对高剂量叠加在连续的背景暴露上。该模型预测的毒死rif平均剂量为每个报告事件1.61微克/千克。这些报告有暴露事件的儿童的平均背景剂量率为0.0062微克/千克/小时,或0.15微克/千克/天。除了从尿液生物标志物测量值预测个人所接收的毒死dose总剂量外,一旦确定了暴露方式,该模型就可以向前运行。这将允许预测在任何感兴趣的时间段内尿液中消除的TCPy总量。

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