Pharmacokinetics of intracerebroventricular tBuOOH in young adult and mature mice.

M L Chang, J D Adams
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引用次数: 8

Abstract

This in vivo study compared the pharmacokinetics of intracerebroventricularly administered tertiary butylhydroperoxide (tBuOOH) (109.7 mg/kg) among six different brain regions in two age groups of mice (2- and 8-mo-old mice). Brains were dissected at 11 time-points ranging from 0.5-60 min. Pharmacokinetics parameters did not differ between the two age groups. This demonstrates that previously reported age-related differences in tBuOOH toxicity may not be owing to pharmacokinetic differences between the two age groups. Differences were found when comparing the pharmacokinetics of tBuOOH among the various brain regions. Area under the curve (AUC) values were highest in the striatum and thalamus, and lowest in the cerebellum. The half-life of tBuOOH varied widely among the regions with the longest half-lives in the cortex and hippocampus, and the shortest in the striatum and cerebellum. The oxidation of glutathione and the induction of DNA damage are critical aspects of tBuOOH toxicity. These data show that region-dependent differences in toxicity reported previously may result from factors, such as tBuOOH-induced glutathione oxidation and DNA damage.

青壮年和成年小鼠脑室内buooh的药动学。
这项体内研究比较了脑室内给药叔丁基过氧化氢(tBuOOH) (109.7 mg/kg)在两个年龄组小鼠(2岁和8岁小鼠)6个不同脑区中的药代动力学。在0.5-60分钟的11个时间点解剖大脑。两个年龄组的药代动力学参数没有差异。这表明,先前报道的年龄相关的tBuOOH毒性差异可能不是由于两个年龄组之间的药代动力学差异。当比较不同脑区中buooh的药代动力学时,发现了差异。曲线下面积(AUC)在纹状体和丘脑中最高,在小脑中最低。脑皮层和海马的半衰期最长,纹状体和小脑的半衰期最短。谷胱甘肽的氧化和DNA损伤的诱导是丁烯ooh毒性的关键方面。这些数据表明,先前报道的区域依赖性毒性差异可能是由buooh诱导的谷胱甘肽氧化和DNA损伤等因素造成的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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