The effects of renal failure on the hepatic and intestinal extraction of tacrolimus were evaluated to examine the mechanisms for the increased bioavailability of this drug in cisplatin-induced renal failure model rats. Tacrolimus extractions in the liver and intestine were evaluated by intravenous, intraportal and intraintestinal infusion. The intestinal metabolism and absorption rate were estimated by incubating the isolated intestine with drug solution and by an in situ loop method, respectively. Blood concentrations of tacrolimus following the intraintestinal infusion were significantly increased in rats with renal failure compared with those in normal rats. The blood concentration of tacrolimus during intraportal infusion in rats with renal failure showed non-linearity against dose, and was increased as compared with that in normal rats. The intestinal metabolism was not altered, but the absorption rate was significantly increased in the intestine from rats with renal dysfunction. These results suggest that the hepatic metabolism of tacrolimus is impaired in rats with renal failure, and that the accelerated absorption rate in the intestine in renal dysfunction is followed by partial saturation of hepatic extraction, which may be one of the mechanisms of increased bioavailability of tacrolimus.

译文

评估了肾衰竭对他克莫司肝和肠提取的影响,以研究该药物在顺铂诱导的肾衰竭模型大鼠中生物利用度增加的机制。通过静脉内,静脉内和肠内输注评估他克莫司在肝脏和肠道中的提取液。分别通过将分离的肠与药物溶液一起孵育和通过原位循环方法来估算肠的代谢和吸收率。与正常大鼠相比,肾衰竭大鼠在肠内输注后他克莫司的血药浓度显着增加。肾衰竭大鼠在静脉内输注过程中他克莫司的血药浓度显示出对剂量的非线性,并且与正常大鼠相比有所增加。肠道代谢没有改变,但肾功能不全大鼠的肠道吸收率显着增加。这些结果表明,他克莫司的肝代谢在肾功能衰竭大鼠中受损,肾功能不全时肠道吸收速度加快,肝提取部分饱和,这可能是他克莫司生物利用度增加的机制之一。

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