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基于气体摄取研究的吸入药代动力学。V. 大鼠体内乙烯和1,3 - 丁二烯的比较药代动力学。

Inhalation pharmacokinetics based on gas uptake studies. V. Comparative pharmacokinetics of ethylene and 1,3-butadiene in rats.

作者信息

Bolt H M, Filser J G, Störmer F

出版信息

Arch Toxicol. 1984 Oct;55(4):213-8. doi: 10.1007/BF00341013.

Abstract

The pharmacokinetics of ethylene and 1,3-butadiene were studied in male Sprague-Dawley rats by use of a closed inhalation chamber system. Both compounds showed saturable metabolism when untreated rats were used. "Linear" pharmacokinetics applied at exposure concentrations below 800 ppm ethylene and below 1,000 ppm 1,3-butadiene. A constant elimination rate, indicative of metabolic saturation, occurred at concentrations higher than 1,000 ppm ethylene or 1,500 ppm 1,3-butadiene. Pretreatment with aroclor 1254 (polychlorinated biphenyls) increased Vmax for both compounds. For 1,3-butadiene, no saturation of metabolic capacity was observed with exposure concentrations up to 12,000 ppm when the rats were pretreated with aroclor 1254. A comparison with previous studies on ethane and n-pentane suggested that introduction of a double bond into a saturated aliphatic hydrocarbon increased the rate of metabolism under conditions in vivo.

摘要

利用密闭吸入舱系统,在雄性斯普拉格-道利大鼠中研究了乙烯和1,3-丁二烯的药代动力学。当使用未处理的大鼠时,这两种化合物均表现出饱和代谢。在乙烯浓度低于800 ppm和1,3-丁二烯浓度低于1,000 ppm时,呈现“线性”药代动力学。当乙烯浓度高于1,000 ppm或1,3-丁二烯浓度高于1,500 ppm时,出现恒定消除率,这表明存在代谢饱和。用多氯联苯混合物Aroclor 1254预处理可提高这两种化合物的最大反应速率(Vmax)。对于1,3-丁二烯,当用Aroclor 1254预处理大鼠时,在高达12,000 ppm的暴露浓度下未观察到代谢能力饱和。与先前关于乙烷和正戊烷的研究比较表明,在体内条件下,在饱和脂肪烃中引入双键会提高代谢速率。

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