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The Effect of Liver and Kidney Disease on the Pharmacokinetics of Clozapine and Sildenafil: A Physiologically Based Pharmacokinetic Modeling

机译:肝肾疾病对氯氮平和西地那非药代动力学的影响:一种生理基础的药代动力学建模

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Background and Objectives: Physiologically based pharmacokinetic (PBPK) modeling permits clinical scientists to reduce practical constraints for clinical trials on patients with special diseases. In this study, simulations were carried out to validate the pharmacokinetic parameters of clozapine and sildenafil using Simcypsup?/sup simulator in young male adults and compare the effect of renal or hepatic impairment on the pharmacokinetic parameters of clozapine and sildenafil. Also, the effect of age on pharmacokinetic parameters of both drugs was investigated in healthy population and in patients with renal and hepatic impairment. Methods: A full PBPK model was built in the simulator for clozapine and sildenafil based on physicochemical properties and observed clinical results. The model used was Advanced, Dissolution, Absorption and Metabolism (ADAM) for both drugs. Results: The PBPK model adequately predicted the pharmacokinetic parameters of clozapine and sildenafil for the healthy adult population. In the simulation results, the bioavailability of both drugs was remarkably raised in both renal and hepatic impairment in young and elderly populations. Conclusion: PBPK modeling could be helpful in the investigation and comparison of the pharmacokinetics in populations with specific disease conditions.
机译:背景和目标:基于生理学的药代动力学(PBPK)建模允许临床科学家减少对特殊疾病患者的临床试验的实际限制。在该研究中,进行了仿真以验证氯氮平和西地那非的药代动力学参数使用辛型β-β-β-αs模拟器,并比较肾脏或肝损伤对氯氮平和西地那非的药代动力学参数的影响。此外,在健康人口和肾病患者中,研究了两种药物的年龄对药代动力学参数的影响。方法:基于物理化学特性,在氯氮平和西地那非的模拟器中建立了完整的PBPK模型,并观察到临床结果。使用的模型是两种药物的先进,溶解,吸收和代谢(ADAM)。结果:PBPK模型充分预测了氯氮平和西地那非为健康成年人群的药代动力学参数。在仿真结果中,两种药物的生物利用度在年轻和老年人口中的肾病和肝障碍中显着提高。结论:PBPK建模可能有助于调查和比较具有特定疾病病症的群体中的药代动力学。

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