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Predictable 'individual differences' in uptake and excretion of gases and lipid soluble vapours simulation study.

机译:可预测的“个体差异”在气体和脂溶性气体的吸收和排泄模拟研究中。

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摘要

A five-compartment pharmacokinetic model with two excretory pathways, exhalation and metabolism, based on first order kinetics is used to outline the effect of body build, pulmonary ventilation, and lipid content in blood on uptake, distribution, and clearance of low solubility gases and lipid soluble vapours during and after exposure. The model shows the extent that individual differences have on altering uptake and distribution, with consequent changes in blood concentration, rate of excretion, and toxicity, even when variations in these parameters are within physiological ranges. The model is also used to describe the concentration variation of inhaled substances in tissues of subjects exposed to concentrations with permitted excursions. During the same course of exposure, the tissue concentrations of low solubility gases fluctuate much more than tissue concentrations of lipid soluble vapours. The fluctuation is reduced by metabolism of inhaled substance. These conclusions are recommended for consideration whenever evaluating the effect of excursions above the threshold limit values used in the control of industrial exposures (by excursion factors).
机译:基于一阶动力学的五室药动学模型,具有两个排泄途径,即呼气和代谢,用于概述健美,肺通气和血液中脂质含量对低溶解度气体和脂肪的吸收,分布和清除的影响。暴露期间和之后的脂溶性蒸气。该模型显示出个体差异改变摄取和分布的程度,从而导致血液浓度,排泄速率和毒性的变化,即使这些参数的变化在生理范围内。该模型还用于描述暴露在允许偏移范围内的受试者的组织中吸入物质的浓度变化。在相同的暴露过程中,低溶解度气体的组织浓度波动要比脂溶性蒸气的组织浓度波动大得多。吸入物质的新陈代谢可减少这种波动。建议在评估超出工业控制中使用的阈值极限值(由偏移因子)引起的偏移的影响时考虑这些结论。

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