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用于甲氨蝶呤协同自靶向癌症治疗及双模式成像的载药/染料多功能聚乙二醇-壳聚糖-氧化铁纳米复合材料

Drug/Dye-Loaded, Multifunctional PEG-Chitosan-Iron Oxide Nanocomposites for Methotraxate Synergistically Self-Targeted Cancer Therapy and Dual Model Imaging.

作者信息

Lin Jinyan, Li Yang, Li Yanxiu, Wu Hongjie, Yu Fei, Zhou Shuifan, Xie Liya, Luo Fanghong, Lin Changjian, Hou Zhenqing

机构信息

§Department of Pharmacy, School of Pharmaceutical Science, Xiamen University, Xiamen 361102, China.

⊥The First Affiliated Hospital of Xiamen University, Xiamen 361002, China.

出版信息

ACS Appl Mater Interfaces. 2015 Jun 10;7(22):11908-20. doi: 10.1021/acsami.5b01685. Epub 2015 May 28.

DOI:10.1021/acsami.5b01685
PMID:25978458
Abstract

Multifunctional nanocomposites hold great potential to integrate therapeutic and diagnostic functions into a single nanoscale structure. In this paper, we prepared the MTX-PEG-CS-IONPs-Cy5.5 nanocomposites by functionalizing the surface of chitosan-decorated iron oxide nanoparticles (CS-IONPs) with polyethylene glycolated methotraxate (MTX-PEG) and near-infrared fluorescent cyanin dye (Cy5.5). A clinically useful PEGylated anticancer prodrug, MTX-PEG, was also developed as a tumor cell-specific targeting ligand for self-targeted cancer treatment. In such nanocomposites, the advantage was that the orthogonally functionalized, self-targeted MTX-PEG-CS-IONPs-Cy5.5 can synergistically combine an early phase selective tumor-targeting efficacy with a late-phase cancer-killing effect, which was also confirmed by dual model (magnetic resonance and fluorescence) imaging. Furthermore, with the aids of the folate (FA) receptor-mediated endocytosis (able to turn cellular uptake "off" in normal cells and "on" in cancer cells) and pH/intracellular protease-mediated hydrolyzing peptide bonds (able to turn drug release "off" in systemic circulation and "on" inside endo/lysosomes), the MTX-PEG-CS-IONPs-Cy5.5 could deliver MTX to FA receptors-overexpressed cancer cells, showing the improved anticancer activity with the reduced side effects. Together, the MTX-PEG-CS-IONPs-Cy5.5 could act as a highly convergent, flexible, and simplified system for dual model imaging and synergistically self-targeted cancer therapy, holding great promise for versatile biomedical applications in future.

摘要

多功能纳米复合材料在将治疗和诊断功能整合到单个纳米级结构方面具有巨大潜力。在本文中,我们通过用聚乙二醇化甲氨蝶呤(MTX-PEG)和近红外荧光菁染料(Cy5.5)对壳聚糖修饰的氧化铁纳米颗粒(CS-IONPs)表面进行功能化,制备了MTX-PEG-CS-IONPs-Cy5.5纳米复合材料。一种临床上有用的聚乙二醇化抗癌前药MTX-PEG也被开发为用于自靶向癌症治疗的肿瘤细胞特异性靶向配体。在这种纳米复合材料中,优势在于正交功能化的自靶向MTX-PEG-CS-IONPs-Cy5.5可以将早期阶段的选择性肿瘤靶向功效与晚期阶段的癌症杀伤作用协同结合,这也通过双模态(磁共振和荧光)成像得到了证实。此外,借助叶酸(FA)受体介导的内吞作用(能够使正常细胞中的细胞摄取“关闭”,癌细胞中的细胞摄取“开启”)以及pH/细胞内蛋白酶介导的肽键水解(能够使全身循环中的药物释放“关闭”,在内体/溶酶体内“开启”),MTX-PEG-CS-IONPs-Cy5.5可以将MTX递送至FA受体过表达的癌细胞,显示出抗癌活性提高且副作用减少。总之,MTX-PEG-CS-IONPs-Cy5.5可以作为一种高度整合、灵活且简化的双模态成像和协同自靶向癌症治疗系统,在未来的多功能生物医学应用中具有巨大前景。

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