首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >Development of a pharmacokinetic/pharmacodynamic (PK/PD)-simulation system for doxorubicin in long circulating liposomes in mice using peritoneal P388.
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Development of a pharmacokinetic/pharmacodynamic (PK/PD)-simulation system for doxorubicin in long circulating liposomes in mice using peritoneal P388.

机译:使用腹膜P388在小鼠长循环脂质体中阿霉素的药代动力学/药效学(PK / PD)模拟系统的开发。

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摘要

The objective of this study was to develop a simulation system that optimizes the pharmacokinetic parameters of drug carriers for anticancer agents in order to maximize their anticancer effects. The pharmacokinetic/pharmacodynamic (PK/PD) model of doxorubicin (DOX) encapsulated into liposomes has been developed for mice and each parameter required for simulations was obtained in the peritoneally inoculated P388 leukemia model in mice. PK parameters, which describe the dispositions of free and liposomally encapsulated DOX, were obtained by kinetic analysis of experimental data in this study, as well as from literature. PD parameters, which describe the growth and death rate of cancer cells in vivo, were also determined. The PK/PD model developed in this study is capable of simulating the time course of the number of cancer cells quantitatively and evaluating the significance of each parameter on the carrier system for DOX. Simulations based on the PK/PD model predict the optimum rate of drug release from long circulating liposomes as 0.06 h(-1) for maximum anticancer effect. Thus, this simulation system provides useful information relative to the optimization of drug carriers for DOX.
机译:这项研究的目的是开发一种模拟系统,该系统可以优化用于抗癌药的药物载体的药代动力学参数,以最大程度地发挥其抗癌作用。已经为小鼠开发了封装在脂质体中的阿霉素(DOX)的药代动力学/药效学(PK / PD)模型,并且在小鼠的腹膜接种P388白血病模型中获得了模拟所需的每个参数。 PK参数描述了游离和脂质体包裹的DOX的位置,该参数通过本研究以及从文献中对实验数据进行动力学分析获得。还确定了PD参数,其描述了体内癌细胞的生长和死亡率。在这项研究中开发的PK / PD模型能够定量模拟癌细胞数量的时程并评估DOX载体系统上每个参数的重要性。基于PK / PD模型的模拟预测从长循环脂质体释放药物的最佳速率为0.06 h(-1),以实现最大的抗癌效果。因此,该模拟系统提供了有关优化DOX药物载体的有用信息。

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