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Chitosan-based nanoparticles for controlled release of hydrophobic and hydrophilic drugs

机译:基于壳聚糖的纳米粒子,用于控释疏水和亲水药物

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摘要

Nanoparticles encapsulating different kinds of therapeutic drugs are promising drug delivery systems for controlling release and targeting tumor cells. Chitosan nanoparticles made by polyelectrolyte complexation were designed as drug carriers using doxorubicin (DOX)/5-fluorouracil (5-FU) as hydrophobic/hydrophilic model drugs. The sizes of nanoparticles were 235 ± 13 and 177 ± 7 nm with narrow distributions. The effects of the initial drug amount and pH of the medium on drug-controlled release properties were evaluated, the model-fitting results and release mechanisms were analyzed as well. For 5-FU-loaded chitosan nanoparticles, the controlled-release effect was superior to that of DOX, indicating that the polyelectrolyte complex nanoparticles were more suitable for hydrophilic drugs, particularly for negatively charged or electrically neutral drugs. Moreover, the release behaviors conformed with the first-order kinetic model, indicating that the nanoparticles were mainly released by diffusion during the drug release process; the system could also be fitted using the Higuchi model, showing that the entire drug release process was dominated by diffusion and supplemented by gradual dissolution. In all, the results suggested that chitosan nanoparticles made by polyelectrolyte complexation can be launched as a smart drug delivery system for cancer treatments.
机译:包封不同种类治疗药物的纳米颗粒是用于控制释放和靶向肿瘤细胞的药物递送系统。通过聚电解质络合制备的壳聚糖纳米颗粒被设计为使用多柔比星(DOX)/ 5-氟尿嘧啶(5-FU)作为疏水/亲水模型药物的药物载体。纳米颗粒的尺寸为235±13和177±7nm,分布窄。评价初始药物量和培养基对药物控制释放性能的效果,也分析了模型拟合结果和释放机制。对于5-FU负载的壳聚糖纳米粒子,受控释放效果优于DOX的,表明聚电解质复合纳米颗粒更适合亲水药物,特别是对于带负电或电中性药物。此外,释放行为与一阶动力学模型符合,表明纳米颗粒主要通过扩散在药物释放过程中释放;该系统也可以使用HIGUCHI模型配合,表明整个药物释放过程通过扩散来支配并通过逐渐溶解补充。总而言之,结果表明,通过聚电解质络合制备的壳聚糖纳米粒子可作为癌症治疗的智能药物输送系统发射。

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