首页> 美国卫生研究院文献>International Journal of Nanomedicine >Fabrication of cRGD-modified reduction-sensitive nanocapsule via Pickering emulsion route to facilitate tumor-targeted delivery
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Fabrication of cRGD-modified reduction-sensitive nanocapsule via Pickering emulsion route to facilitate tumor-targeted delivery

机译:通过Pickering乳液路线制备cRGD修饰的还原敏感性纳米胶囊以促进肿瘤靶向递送

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摘要

>Purpose: To fabricate multifunctional nanocapsule via Pickering emulsion route to facilitate tumor-targeted delivery.>Methods: Poly(N-isopropylacrylamide-co-acrylic acid) nanoparticles (PNA) stabilized nanocapsules were fabricated by Pickering emulsion (PE) technology. For controllable drug-release and enhancing targeted antitumor effects, the nanocapsules were crosslinked with cystamine and coupled on cell-surface molecule markers (cRGDfK) to achieve on-demand drug release and targeted delivery.>Results: The fabricated PE and nanocapsules with average particle sizes (250 and 150 nm) were obtained. Encapsulation efficiency of hydrophobic anticancer drug (DOX) was determined as >90%. Release kinetic profiles for encapsulated nanocapsules displayed circulation stability and redox-sensitive releasing behavior with the supposed increase bioavailability. Both cytotoxicity assay, cellular uptake analysis and anticancer efficacy in B16F10 murine model demonstrated these redox-responsive drug-release and active targeted delivery.>Conclusion: The results clearly demonstrated nanocapsule via PE route as promising candidate to provide an effective platform for incorporating hydrophobic drug for targeted cancer chemotherapy.
机译:>目的:通过Pickering乳液路线制造多功能纳米胶囊,以促进肿瘤靶向递送。>方法:聚(N-异丙基丙烯酰胺-丙烯酸)纳米粒子(PNA)稳定的纳米胶囊由Pickering乳液(PE)技术制成。为了控制药物的释放并增强靶向抗肿瘤作用,将纳米胶囊与胱胺交联并偶联在细胞表面分子标记(cRGDfK)上,以实现按需释放和靶向递送。>结果:获得具有平均粒径(250和150 nm)的PE和纳米胶囊。疏水抗癌药(DOX)的包封效率确定为> 90%。封装的纳米胶囊的释放动力学曲线显示出循环稳定性和氧化还原敏感释放行为,并具有增加的生物利用度。 B16F10小鼠模型的细胞毒性测定,细胞摄取分析和抗癌功效均证明了这些氧化还原反应性药物释放和主动靶向递送。将疏水性药物用于靶向癌症化疗的有效平台。

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