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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >The research background for risk assessment of ethylene oxide: aspects of dose.
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The research background for risk assessment of ethylene oxide: aspects of dose.

机译:环氧乙烷风险评估的研究背景:剂量方面。

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摘要

Data for relationships between in vivo doses inferred from levels of hemoglobin (Hb) or DNA adducts and administered (by inhalation or injection) doses of ethylene oxide (EO) in mice, rats and humans are reviewed. At low absorbed doses or dose rates these relationships appear to be linear, whereas at higher dose rates deviations from linearity due to saturation kinetics of detoxification and of DNA repair as well as certain toxic effects have to be allowed for. If these factors are taken into consideration, a rather consistent picture is obtained for animal studies, with a variation by less than a factor 2 between estimates of adduct level increments or in vivo dose increments per unit of administered dose. Although the value for in vivo dose per unit of exposure dose (ppm-hour) in humans is uncertain because of unreliable data for the time-weighted average exposure level, the most likely value for this relationship, supported by data for ethene, agrees with data for the rodents. In the animal species testis doses are approximately one-half of the blood doses inferred from Hb adducts.
机译:审查了从血红蛋白(Hb)或DNA加合物的水平推断出的体内剂量与(通过吸入或注射)环氧乙烷(EO)的剂量在小鼠,大鼠和人类中的体内剂量之间的关系的数据。在低吸收剂量或剂量率下,这些关系似乎是线性的,而在较高剂量率下,由于排毒和DNA修复的饱和动力学以及某些毒性作用,会偏离线性。如果考虑到这些因素,则对于动物研究可获得相当一致的图像,每加单位剂量的加合物水平增量或体内剂量增量估算值之间的差异小于2。尽管由于时间加权平均暴露水平的数据不可靠,人体中单位暴露剂量(ppm小时)的体内剂量值尚不确定,但乙烯数据支持的这种关系的最可能值与啮齿动物的数据。在动物物种中,睾丸的剂量约为Hb加合物推断的血液剂量的一半。

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