Comparison of in vitro and in vivo developmental toxicity and pharmacokinetics of phenytoin in the rat.

M E Beekhuijzen, A Verhoef, R Klaassen, C J Rompelberg, A H Piersma
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引用次数: 4

Abstract

The rat whole embryo culture was compared to an in vivo experiment with regard to embryotoxicity as well as exposure characteristics, using phenytoin as a model compound. Intra-embryonic concentrations and their embryotoxic effects were determined on gestation day 11 after in vitro administration of 50-150 microg/ml or in vivo gavage of 500-1500 mg/kg body-weight on gestation day 10. In addition, exposure kinetics were studied in vivo after a single oral dose on gestation day 10, and developmental defects on gestation day 21 were scored. The embryotoxic effects observed on gestation day 11 were more pronounced after in vitro exposure in comparison to in vivo exposure at similar intra-embryonic concentrations. Exposure of phenytoin on gestation day 10 in vitro via the culture medium resulted in general embryotoxicity on gestation day 11, whereas in vivo effects as determined on gestation day 11 were minimal. Plasma concentrations of phenytoin increased and plateaued around 35 microg/ml during the 48 hr monitoring period. Plasma concentration curves and pharmacokinetic parameters did not show remarkable differences between the dose groups, indicating that absorption is the limiting factor at the dose range used. Although the developmental effects were minimal as observed in vivo on gestation day 11, specific malformations (defects encompassing the urogenital. craniofacial and skeletal systems) were observed on gestation day 21. These findings show that with similar intra-embryonic concentrations of phenytoin the embryotoxicity in rat whole embryo culture was not comparable with the in vivo embryotoxicity as determined on gestation day 11. This discrepancy may at least partly be explained by differences in exposure characteristics.

苯妥英在大鼠体内外发育毒性及药代动力学比较。
以苯妥英为模型化合物,对大鼠全胚胎培养与体内实验的胚胎毒性及暴露特性进行了比较。在妊娠第10天体外给药50 ~ 150 mg/ ml或体内灌胃500 ~ 1500 mg/kg体重,于妊娠第11天测定胚胎内浓度及其胚胎毒性作用。此外,研究了妊娠第10天单次口服剂量后的体内暴露动力学,并对妊娠第21天的发育缺陷进行了评分。在妊娠第11天观察到的胚胎毒性作用在体外暴露后比在体内暴露在相似的胚胎内浓度下更为明显。在体外妊娠第10天通过培养基暴露于苯妥英导致妊娠第11天的一般胚胎毒性,而在体内妊娠第11天的影响最小。在48小时的监测期间,苯妥英的血浆浓度升高并稳定在35微克/毫升左右。血浆浓度曲线和药代动力学参数在剂量组间无显著差异,说明在剂量范围内,吸收是限制因素。尽管在妊娠第11天体内观察到的发育影响很小,但包括泌尿生殖器官在内的特定畸形(缺陷)。妊娠第21天观察颅面和骨骼系统。这些结果表明,在胚胎内苯妥英浓度相似的情况下,大鼠全胚胎培养的胚胎毒性与妊娠第11天测定的体内胚胎毒性不具有可比性。这种差异至少部分可以用暴露特征的不同来解释。
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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