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与职业暴露相关的环氧乙烷风险评估及肿瘤动力学

Risk assessment and oncodynamics of ethylene oxide as related to occupational exposure.

作者信息

Beliles R P, Parker J C

机构信息

U.S. Environmental Protection Agency, Washington, D.C.

出版信息

Toxicol Ind Health. 1987 Sep;3(3):371-82. doi: 10.1177/074823378700300309.

Abstract

Two rat inhalation bioassays have been integrated into the risk assessment on the carcinogenicity of ethylene oxide (EO). The carcinogenic findings as well as relevant metabolism and pharmacokinetic data are reviewed. Brain tumors were selected as the endpoint for the assessment of risk because of the indication that adverse effects on the nervous system, related to EO exposure, were consistent across species. Two methods, time-exposure concentration product and area under the plasma concentration-time curve (AUC) are used as a basis for calculating effective dose. Scaling of the dose to man from both rat and dog is explored based on pharmacokinetic studies. Two different mathematical risk extrapolation models, the probit and the multi-stage, are used to estimate the cancer risk for daily exposures to EO of 1.8 microgram/liter over a working lifetime. The use of AUC as a basis for dose from a daily exposure of 1.8 microgram/liter over a working lifetime gives the higher risk rates (90-142/10,000 workers). The implication of the simulated dose using plasma concentrations versus the time-concentration product approach is discussed in relation to threshold effects.

摘要

两项大鼠吸入生物测定已纳入环氧乙烷(EO)致癌性的风险评估中。对致癌研究结果以及相关代谢和药代动力学数据进行了综述。由于有迹象表明,与环氧乙烷暴露相关的对神经系统的不良反应在不同物种中是一致的,因此选择脑肿瘤作为风险评估的终点。两种方法,即时间-暴露浓度乘积和血浆浓度-时间曲线下面积(AUC),被用作计算有效剂量的基础。基于药代动力学研究,探讨了从大鼠和狗向人类的剂量换算。两种不同的数学风险外推模型,即概率单位模型和多阶段模型,用于估计在整个工作寿命期间每天暴露于1.8微克/升环氧乙烷的癌症风险。以AUC作为在整个工作寿命期间每天暴露于1.8微克/升的剂量基础,得出的风险率更高(90-142/10000名工人)。讨论了使用血浆浓度模拟剂量与时间-浓度乘积方法相对于阈值效应的含义。

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