Kao Mark L, Ruoff Bruce, Bower Nancy, Aoki Toyohiko, Smart Clair, Mannens Geert
Janssen R&D, Drug Safety Sciences, Raritan, NJ 08869, USA.
Xenobiotica. 2012 Apr;42(4):389-97. doi: 10.3109/00498254.2011.627478. Epub 2011 Nov 4.
The pharmacokinetics, metabolism and excretion of monoethyl phthalate (MEP) and diethyl phthalate (DEP) were compared after intravenous or oral administration of [(14)C]MEP or [(14)C]DEP in juvenile beagle dogs. Four male juvenile beagle dogs were treated with a single oral or bolus intravenous dose of either [(14)C]MEP or [(14)C]DEP (164 μg/kg). The absorption, metabolism, excretion and pharmacokinetics of [(14)C]MEP and [(14)C]DEP were nearly identical. [(14)C]DEP was rapidly and nearly completely metabolized to [(14)C]MEP following either intravenous or oral administration. [(14)C]MEP and[(14)C]DEP were rapidly absorbed, the elimination half-life was estimated to be 1 hour. Approximately 90%-96% of the dose was excreted in urine with 2%-3% of the dose in faeces. MEP accounted for the majority of the dose in plasma and urine; in addition, three minor metabolites (M1, M2 and M3) were detected. The minor metabolites were neither phthalic acid nor glucuronide/sulfate conjugates. The nearly identical metabolism and pharmacokinetics of MEP and DEP in juvenile dogs justifies the use of DEP toxicity data in the risk assessment of MEP exposure.
在幼年比格犬静脉注射或口服[(14)C]单乙基邻苯二甲酸酯(MEP)或[(14)C]二乙基邻苯二甲酸酯(DEP)后,对比了MEP和DEP的药代动力学、代谢及排泄情况。给4只雄性幼年比格犬单次口服或静脉推注[(14)C]MEP或[(14)C]DEP(164μg/kg)。[(14)C]MEP和[(14)C]DEP的吸收、代谢、排泄及药代动力学情况几乎相同。静脉注射或口服[(14)C]DEP后,其迅速且几乎完全代谢为[(14)C]MEP。[(14)C]MEP和[(14)C]DEP吸收迅速,消除半衰期估计为1小时。约90%-96%的剂量经尿液排泄,2%-3%经粪便排泄。MEP占血浆和尿液中剂量的大部分;此外,还检测到三种次要代谢物(M1、M2和M3)。这些次要代谢物既不是邻苯二甲酸,也不是葡糖醛酸/硫酸盐结合物。幼年犬中MEP和DEP几乎相同的代谢及药代动力学情况证明在MEP暴露风险评估中可使用DEP的毒性数据。
