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Development of Folate-Functionalized PEGylated Zein Nanoparticles for Ligand-Directed Delivery of Paclitaxel

机译:紫杉醇配体递送的叶酸官能化聚乙二醇化玉米醇纳米粒子的研制

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摘要

In this study, we investigated the active targeted delivery of a hydrophobic drug, paclitaxel (PTX), via receptor-mediated endocytosis by folate receptors expressed on cancer cells using a protein-based nanoparticle system. PTX was loaded on zein nanoparticles and conjugated with folate (PTX/Zein-FA) to estimate its chemotherapeutic efficacy in folate receptor-expressing KB cancer cells. PTX/Zein-FA nanoparticles were successfully developed, with a nanoparticle size of ~180 nm and narrow polydispersity index (~0.22). Accelerated release of PTX in an acidic environment was observed for PTX/Zein-FA. An in vitro cellular study of PTX/Zein-FAs in KB cells suggested that PTX/Zein-FA improved the cytotoxic activity of PTX on folate receptors overexpressed in cancer cells by inducing proapoptotic proteins and inhibiting anti-apoptotic proteins. In addition, PTX/Zein-FA exhibited anti-migratory properties and could alter the cell cycle profile of KB cells. A549 cells, which are folate receptor-negative cancer cells, showed no significant enhancement in the in vitro cellular activities of PTX/Zein-FA. We describe the antitumor efficacy of PTX/Zein-FA in KB tumor-bearing mice with minimum toxicity in healthy organs, and the results were confirmed in comparison with free drug and non-targeted nanoparticles.
机译:在本研究中,我们研究了使用基于蛋白质的纳米粒子系统在癌细胞上表达的叶酸受体通过受体介导的内吞作用,通过受体介导的内吞作用,研究了疏水药物的活性靶向递送。 PTX在ZEIN纳米粒子上装载并与叶酸(PTX / ZEEN-FA)缀合,以估计其在叶酸受体表达的KB癌细胞中的化学治疗效果。成功开发了PTX / ZEIN-FA纳米颗粒,纳米颗粒尺寸为约180nm,窄多分散性指数(〜0.22)。对于PTX / Zein-Fa,观察到酸性环境中PTX的加速释放。 KB细胞中PTX / Zein-Fas的体外细胞研究表明,PTX / Zein-Fa通过诱导促凋亡蛋白并抑制抗凋亡蛋白来改善PTX对癌细胞过表达的叶酸受体的细胞毒性活性。此外,PTX / ZEIN-FA表现出抗迁移性质,可以改变KB细胞的细胞周期谱。 A549细胞,其叶酸受体阴性癌细胞显示出PTX / Zein-Fa的体外细胞活性没有显着增强。我们描述了在KB携带的小鼠中PTX / Zein-Fa的抗肿瘤效果,其具有健康器官的最小毒性,与游离药物和非靶向纳米颗粒相比证实了结果。

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