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丙酮醛双脒腙(甲基-GAG)的药代动力学研究。

Pharmacokinetic study of methyl glyoxal-bis-guanylhydrazone (methyl-GAG).

作者信息

Slavik M, Clouse T, Wood A, Blanc O, Eschbach R C

出版信息

Invest New Drugs. 1983;1(3):219-24. doi: 10.1007/BF00208893.

Abstract

Using a paired ion exchange high pressure liquid chromatographic assay, pharmacokinetic evaluation of methyl glyoxal bis guanylhydrazone (methyl-GAG) was performed in nine male New Zealand albino rabbits following administration of a single intravenous bolus dose of 50 mg/kg B.W (550 mg/m2 BSA). Blood samples were collected before and at intervals of 5, 10, 15, 30 min and 1, 2, 3, 4, 6, 8, 12, 18, and 24 h after administration of the drug. The analysis of experimental data indicates a three compartment open model with first order elimination from the central compartment described by the equation Cpt = A.e-alpha t + B.e-beta t + C.e-gamma t, where A, B, C, are 107.985, 4.785, and 0.763 micrograms/ml, respectively. alpha, beta, gamma, are 5.466, 0.487, and 0.030 h-1, respectively, and T1/2 alpha, beta, gamma are 7.6, 85.3 min and 23.1 h, respectively. The mean volume of distribution in the central compartment Vc was 0.44 liters (1)/kg, volume of distribution Vdarea 30.326 1/kg, and the total body clearance 0.9097 1/kg/h. The existence of a long terminal plasma half life of methyl-GAG reported previously in human studies was also confirmed in experimental animals and may explain the cumulative toxicity of this drug.

摘要

采用配对离子交换高压液相色谱分析法,对9只雄性新西兰白化兔单次静脉推注50mg/kg体重(550mg/m²体表面积)的甲基乙二醛双脒腙(methyl-GAG)后进行了药代动力学评估。给药前及给药后5、10、15、30分钟以及1、2、3、4、6、8、12、18和24小时采集血样。实验数据分析表明,该药物符合三室开放模型,从中央室以一级速率消除,其方程为Cpt = A.e-αt + B.e-βt + C.e-γt,其中A、B、C分别为107.985、4.785和0.763微克/毫升。α、β、γ分别为5.466、0.487和0.030 h⁻¹,T1/2α、β、γ分别为7.6、85.3分钟和23.1小时。中央室的平均分布容积Vc为0.44升(1)/千克,分布容积Vdarea为30.326升/千克,总体清除率为0.9097升/千克/小时。先前在人体研究中报道的methyl-GAG具有较长的终末血浆半衰期,在实验动物中也得到了证实,这可能解释了该药物的累积毒性。

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