Doxorubicin-Loaded Core–Shell UiO-66@SiO2 Metal–Organic Frameworks for Targeted Cellular Uptake and Cancer Treatment

生物相容性 药物输送 叶酸受体 阿霉素 材料科学 泊洛沙姆 纳米颗粒 纳米技术 介孔二氧化硅 癌细胞 毒品携带者 化学 生物物理学 生物医学工程 介孔材料 癌症 有机化学 聚合物 化疗 医学 外科 共聚物 内科学 催化作用 生物
作者
Daria B. Trushina,Anastasiia Yu. Sapach,Olga A. Burachevskaia,P. V. Medvedev,Д. Н. Хмеленин,Tatyana N. Bоrodinа,Mikhail A. Soldatov,Vera V. Butova
出处
期刊:Pharmaceutics [MDPI AG]
卷期号:14 (7): 1325-1325 被引量:30
标识
DOI:10.3390/pharmaceutics14071325
摘要

Beneficial features of biocompatible high-capacity UiO-66 nanoparticles, mesoporous SiO2, and folate-conjugated pluronic F127 were combined to prepare the core-shell UiO-66@SiO2/F127-FA drug delivery carrier for targeted cellular uptake in cancer treatment. UiO-66 and UiO-66-NH2 nanoparticles with a narrow size and shape distribution were used to form a series of core-shell MOF@SiO2 structures. The duration of silanization was varied to change the thickness of the SiO2 shell, revealing a nonlinear dependence that was attributed to silicon penetration into the porous MOF structure. Doxorubicin encapsulation showed a similar final loading of 5.6 wt % for both uncoated and silica-coated particles, demonstrating the potential of the nanocomposite's application in small molecule delivery. Silica coating improved the colloidal stability of the composites in a number of model physiological media, enabled grafting of target molecules to the surface, and prevented an uncontrolled release of their cargo, with the drawback of decreased overall porosity. Further modification of the particles with the conjugate of pluronic and folic acid was performed to improve the biocompatibility, prolong the blood circulation time, and target the encapsulated drug to the folate-expressing cancer cells. The final DOX-loaded UiO-66@SiO2/F127-FA nanoparticles were subjected to properties characterization and in vitro evaluation, including studies of internalization into cells and antitumor activity. Two cell lines were used: MCF-7 breast cancer cells, which have overexpressed folate receptors on the cell membranes, and RAW 264.7 macrophages without folate overexpression. These findings will provide a potential delivery system for DOX and increase the practical value of MOFs.
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