首页> 外文期刊>The Journal of toxicological sciences >Species differences in toxicokinetic parameters of glycidol after a single dose of glycidol or glycidol linoleate in rats and monkeys.
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Species differences in toxicokinetic parameters of glycidol after a single dose of glycidol or glycidol linoleate in rats and monkeys.

机译:在大鼠和猴子中单次服用缩水甘油或亚油酸亚麻油酸酯后缩水甘油的毒物动力学参数的物种差异。

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Glycidol fatty acid esters (GEs) have been identified as contaminants in refined edible oils. Although the possible release of glycidol (G) from GEs is a concern, little is known about the conversion of GEs to G in the human body. This study addressed the toxicokinetics of glycidol linoleate (GL) and G in male Crl:CD(SD) rats and cynomolgus monkeys. Equimolar amounts of GL (341 mg/kg) or G (75 mg/kg) were administered by gavage to each animal. G was found in both species after the G and GL administration, while plasma GL concentrations were below the lower limit of quantification (5 ng/ml) in both species. In rats, the administration of GL or G produced similar concentration-time profiles for G. In monkeys, the C(max) and AUC values after GL administration were significantly lower than those after G administration. The oral bioavailability of G in monkeys (34.3%) was remarkably lower than that in rats (68.8%) at 75 mg/kg G administration. In addition, plasma G concentrations after oral administration at three lower doses of GL or G were measured in both species. In monkeys, G was detected only at the highest dose of G. In contrast, the rats exhibited similar plasma G concentration-time profiles after GL or G administration with significantly higher G levels than those in monkeys. In conclusion, these results indicate that there are remarkable species differences in the toxicokinetics of GEs and G between rodents and primates, findings that should be considered when assessing the human risk of GEs.
机译:缩水甘油脂肪酸酯(GEs)已被确定为精制食用油中的污染物。尽管人们可能担心缩水甘油(G)从GEs释放出来,但人们对GEs向G的转化了解甚少。这项研究解决了雄性Crl:CD(SD)大鼠和食蟹猴中亚油酸缩水甘油酯(GL)和G的毒代动力学。通过管饲法向每只动物施用等摩尔量的GL(341 mg / kg)或G(75 mg / kg)。施用G和GL后,两个物种中均发现G,而两个物种的血浆GL浓度均低于定量下限(5 ng / ml)。在大鼠中,GL或G的施用产生了类似的G浓度-时间曲线。在猴子中,GL施用后的C(max)和AUC值显着低于G施用后的。施用75 mg / kg的G后,猴子的G口服生物利用度(34.3%)明显低于大鼠(68.8%)。另外,在两个物种中都测量了口服三种较低剂量的GL或G后血浆G的浓度。在猴子中,仅在最高剂量的G时才检测到G。相比之下,在GL或G施用后,大鼠表现出相似的血浆G浓度-时间曲线,G水平明显高于猴子。总之,这些结果表明,啮齿动物和灵长类动物之间在GEs和G的毒代动力学上存在显着的物种差异,在评估人类对GEs的风险时应考虑这些发现。

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