Cyclophosphamide Pharmacokinetics in Mice: A Comparison Between Retro Orbital Sampling Versus Serial Tail Vein Bleeding

R. Said, M. Abdel-Rehim, B. Sadeghi, S. Al-Hashemi, Z. Hassan, Moustapha Hassan
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引用次数: 22

Abstract

Preclinical studies on pharmacokinetics in animals usually require at least 3-5 animals per time point. The use of several animals in each time point may increase the result variation due to individual dosing errors and interand intraindividual variation among animals. Moreover, a large number of animals has to be euthanized in these experiments. In the present paper, the pharmacokinetics of the anticancer drug, cyclophosphamide was investigated using serial bleeding from the tail vein and compared with the kinetics obtained from traditional retro-orbital sinus bleeding in mice. Cyclophosphamide (100 mg/kg) was administered intraperitoneally to two groups of mice. Blood samples were collected at 0, 0.25, 0.5, 1, 2, 3, 4, 5 and 6 hr. In the first group (n=6), 20 L blood samples were collected from the tail-vein by serial bleeding. In the second group, 3 animals were killed at each time point and blood was collected from both tail vein and retro-orbital sinus. Cyclophosphamide analysis in whole blood was carried out using LC-MS/MS with on-line sample preparation utilizing microextraction by packed sorbent (MEPS). Pharmacokinetics including AUC, tmax, Cmax and half – life were estimated using WinNonLin. Cyclophosphamide concentrations in blood obtained after sampling through tail vein were close to those obtained after retro-orbital bleeding within the same animal. No significant differences in estimated pharmacokinetic parameters were found when serial tail vein bleeding was compared to retro-orbital bleeding. Our results indicate that serial sampling using tail vein in mice can be a good alternative to retro-orbital sampling method. The method is reliable, easy and can be used for early preclinical kinetic studies. However, more studies are needed to evaluate different drug categories.
环磷酰胺在小鼠体内的药代动力学:复古眼眶取样与连续尾静脉出血的比较
动物体内药代动力学的临床前研究通常每个时间点至少需要3-5只动物。在每个时间点使用几个动物可能会由于个体给药误差和动物之间的个体间和个体内差异而增加结果的差异。此外,在这些实验中,大量的动物不得不被安乐死。本文采用小鼠尾静脉连续出血的方法研究了抗癌药物环磷酰胺的药代动力学,并与传统的眶后窦出血方法进行了比较。两组小鼠腹腔注射环磷酰胺(100 mg/kg)。于0、0.25、0.5、1、2、3、4、5、6小时采集血样。第一组(n=6)连续出血尾静脉采血20 L。第二组在每个时间点处死3只,分别取尾静脉和眶后窦血。采用液相色谱-串联质谱(LC-MS/MS)对全血中环磷酰胺进行分析,在线制备样品,采用填充吸附剂微萃取(MEPS)。使用WinNonLin估计药物动力学,包括AUC、tmax、Cmax和半衰期。经尾静脉取样后血液中环磷酰胺浓度与同一动物眼眶后出血后血液中环磷酰胺浓度接近。当连续尾静脉出血与眶后出血相比,估计的药代动力学参数没有显著差异。我们的结果表明,小鼠尾静脉连续采样可以替代眶后采样方法。该方法可靠、简便,可用于早期临床前动力学研究。然而,需要更多的研究来评估不同的药物类别。
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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