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Ultra-small lipid-polymer hybrid nanoparticles for tumor-penetrating drug delivery

机译:超薄lipid-polymer混合纳米颗粒tumor-penetrating药物输送

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摘要

Lipid-polymer hybrid nanoparticles, consisting of a polymeric core coated by a layer of lipids, are a class of highly scalable, biodegradable nanocarriers that have shown great promise in drug delivery applications. Here, we demonstrate the facile synthesis of ultra-small, sub-25 nm lipid-polymer hybrid nanoparticles using an adapted nanoprecipitation approach and explore their utility for targeted delivery of a model chemotherapeutic. The fabrication process is first optimized to produce a monodisperse population of particles that are stable under physiological conditions. It is shown that these ultra-small hybrid nanoparticles can be functionalized with a targeting ligand on the surface and loaded with drug inside the polymeric matrix. Further, the in vivo fate of the nanoparticles after intravenous injection is characterized by examining the blood circulation and biodistribution. In a final proof-of-concept study, targeted ultrasmall hybrid nanoparticles loaded with the cancer drug docetaxel are used to treat a mouse tumor model and demonstrate improved efficacy compared to a clinically available formulation of the drug. The ability to synthesize a significantly smaller version of the established lipid-polymer hybrid platform can ultimately enhance its applicability across a wider range of applications.
机译:Lipid-polymer混合纳米颗粒组成的聚合物核心涂布一层脂质,一类高度可伸缩的、可生物降解的人们有很大的承诺药的应用程序。超薄的简单合成,sub-25 nm使用一个lipid-polymer混合纳米颗粒适应nanoprecipitation方法和探索他们的效用目标提供一个模型化疗。第一次优化的生产单分散的人口稳定的粒子生理条件。混合纳米颗粒可以超小携带一个靶向配体在聚合物表面和装载药物矩阵。静脉注射后的纳米粒子通过检查血液循环特点和biodistribution。研究中,针对超混合纳米颗粒与抗癌药物紫杉醇用于加载治疗小鼠肿瘤模型和演示改善临床疗效相比配方的药物可用。合成的小得多的版本lipid-polymer混合平台可以建立最终在增强其适用性广泛的应用。

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