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Effects of Peritoneal Dialysis on Pharmacotherapy: A Deductive Pharmacokinetic-model Approach to Predict Drug Concentration Profiles in Plasma and Peritoneal Fluid

机译:腹膜透析对药物治疗的影响:一种推导的药代动力学模型方法,可预测血浆和腹膜液中的药物浓度

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The aim of this study was to present a deductive compartment pharmacokinetic (PK) model to predict the concentration profiles of drugs in plasma and peritoneal fluid in peritoneal dialysis (PD) rats. PK parameters of model drugs in normal and experimentally induced acute renal failure (ARF) rats not undergoing PD were obtained inductively in a common regression manner with a two-compartment model. In PD normal and ARF rats, PK parameters relating to the transfer of drugs to the peritoneal dialysate and the progress of renal failure were deductively modified to simulate the drug concentration-time profiles in plasma and in the peritoneal fluid in PD rats. The deductively introduced modifiers were the volume of distribution in the peripheral compartment, plasma protein binding, and solvent movement factor to the peritoneal fluid. Predicted profiles of tolbutamide, propranolol and cefazolin in PD normal and ARF rats were compared with the corresponding observed data. This minimal deductive approach yielded satisfactory accuracy in the prediction of both the plasma and peritoneal fluid concentrations of tolbutamide and propranolol.
机译:这项研究的目的是提出一个演绎室药代动力学(PK)模型,以预测腹膜透析(PD)大鼠血浆和腹膜液中药物的浓度分布。用两室模型以通用回归方式归纳获得正常和实验诱发的急性肾衰竭(ARF)大鼠中未经历PD的模型药物的PK参数。在PD正常和ARF大鼠中,演绎地修改了与药物向腹膜透析液转移和肾衰竭进展有关的PK参数,以模拟PD大鼠血浆和腹膜液中的药物浓度-时间曲线。演绎地引入的修饰剂是外周区室中的分布体积,血浆蛋白结合以及溶剂对腹膜液的运动因子。将PD正常和ARF大鼠中甲苯磺丁酰胺,普萘洛尔和头孢唑林的预测特征与相应的观察数据进行比较。这种最小的演绎方法在预测甲苯磺丁酰胺和普萘洛尔的血浆和腹膜液浓度方面均获得了令人满意的准确性。

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