A facile synthesis of uniform hollow MIL-125 titanium-based nanoplatform for endosomal esacpe and intracellular drug delivery

生物相容性 纳米材料 药物输送 表面改性 阿霉素 体内 纳米技术 药品 材料科学 纳米颗粒 纳米载体 化学 药理学 医学 冶金 生物技术 物理化学 外科 化疗 生物
作者
Jun‐Ling Song,Zhao‐Qian Huang,Jing Mao,Weijun Chen,Bin Wang,Fuwei Yang,Shen-Huan Liu,Huijie Zhang,Lipeng Qiu,Jinghua Chen
出处
期刊:Chemical Engineering Journal [Elsevier]
卷期号:396: 125246-125246 被引量:53
标识
DOI:10.1016/j.cej.2020.125246
摘要

Metal-organic-frameworks (MOFs) have been widely used for drug delivery systems due to their high drug loading content and easy modification. But it remains the biggest challenge to exploring biocompatible MOFs with uniform small sizes and well-defined surface chemistry for tumor therapy. Especially, the hollow-structured MIL-125 Titanium (Ti) nano-MOFs have not been prepared for drug carriers. Therefore, we studied a facile approach to synthesize hollow-structured Ti-based nano-MOF via surfactant coordination modulation. The as-prepared nanomaterials exhibited uniform size of ~200 nm and large BET surface area of 1134 m2·g−1. And then, by simple mechanical grinding, we prepared this hyaluronic acid (HA) modified Ti-based MOFs. Moreover, the amount of HA modification on the MOFs surface for the drug delivery systems was systematically investigated. The doxorubicin (DOX) loaded nano-MOFs ([email protected]) and HA modified nanomaterials ([email protected]) possessed high doxorubicin loading content (~25.0–35.0%) due to their hollow structures and π-π stacking interaction. Especially, In vitro and in vivo safety assessments proved that the Ti-based nano MOF was non-toxic and biocompatibility. Besides, [email protected] could escape from lysosomes to improve intracellular drug accumulations resulting in the enhanced the anticancer efficacy. In vivo antitumor results demonstrated that [email protected] could not only enhance targeted tumor therapy but also lower the side effect of DOX. Therefore, the novel hollow [email protected] as a promising nanoplatform could be applied to targeted tumor therapy.
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