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Effects of Water Deprivation on the Pharmacokinetics of Metformin in Rats

机译:缺水对大鼠二甲双胍药代动力学的影响

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摘要

It was reported that metformin was mainly metabolized via hepatic CYP2C11, 2D1 and 3A1/2 in rats, and in a rat model of dehydration, the expressions of hepatic CYP2C11 and 3A1/ 2 were not changed. Hence, it could be expected that the Cl_nr of metformin is comparable between two groups of rats if the contribution of CYP2D1 in the rat model of dehydration is not considerable. It was also reported that the timed-interval renal clearance of metformin was dependent on the urine flow rate in rats. In the rat model of dehydration, the 24 h urine output was significantly smaller than in the controls. Hence, the urinary excretion of metformin was expected to be smaller than the controls. The above expectations were proven as follows. After intravenous administration of metformin (100 mg/kg) to the rat model of dehydration, the Cl_(nr) were comparable between the two groups of rats. After both intravenous and oral administration of metformin (both 100 mg/kg) to the rat model of dehydration, the 24 h urinary excretion of the drug was significantly smaller than in the controls. After oral administration of metformin to the rat model of dehydration, the AUC was significantly greater (99.2% increase) than the controls.
机译:据报道,二甲双胍主要通过大鼠肝脏CYP2C11、2D1和3A1 / 2代谢,在脱水模型中,肝脏CYP2C11和3A1 / 2的表达没有改变。因此,如果在大鼠脱水模型中CYP2D1的贡献不大,则可以预期二甲双胍的Cl_nr在两组大鼠之间具有可比性。也有报道说,二甲双胍的定时间隔肾脏清除率取决于大鼠的尿流率。在脱水的大鼠模型中,24小时尿量显着小于对照组。因此,预期二甲双胍的尿排泄量小于对照。以上期望被证明如下。在对大鼠脱水模型静脉注射二甲双胍(100 mg / kg)后,Cl_(nr)在两组大鼠之间具有可比性。在大鼠脱水模型中静脉和口服给予二甲双胍(均为100 mg / kg)后,该药物在24小时内的尿排泄量明显小于对照组。在大鼠脱水模型中口服二甲双胍后,AUC明显高于对照组(增加了99.2%)。

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