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Dendrimer-Functionalized Laponite Nanodisks as a Platform for Anticancer Drug Delivery

机译:树状大分子功能化的皂石纳米盘作为抗癌药物传递的平台。

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摘要

In this study, we synthesized dendrimer-functionalized laponite (LAP) nanodisks for loading and delivery of anticancer drug doxorubicin (DOX). Firstly, LAP was modified with silane coupling agents and succinic anhydride to render abundant carboxyl groups on the surface of LAP. Then, poly(amidoamine) (PAMAM) dendrimer of generation 2 (G2) were conjugated to form LM-G2 nanodisks. Anticancer drug DOX was then loaded on the LM-G2 with an impressively high drug loading efficiency of 98.4% and could be released in a pH-sensitive and sustained manner. Moreover, cell viability assay results indicate that LM-G2/DOX complexes could more effectively inhibit the proliferation of KB cells (a human epithelial carcinoma cell line) than free DOX at the same drug concentration. Flow cytometry analysis and confocal laser scanning microscope demonstrated that LM-G2/DOX could be uptaken by KB cells more effectively than free DOX. Considering the exceptional high drug loading efficiency and the abundant dendrimer amine groups on the surface that can be further modified, the developed LM-G2 nanodisks may hold a great promise to be used as a novel platform for anticancer drug delivery.
机译:在这项研究中,我们合成了树状大分子官能化的皂石(LAP)纳米盘,用于装载和输送抗癌药阿霉素(DOX)。首先,用硅烷偶联剂和琥珀酸酐对LAP进行改性,以在LAP的表面上形成丰富的羧基。然后,第2代(G2)的聚(酰胺基胺)(PAMAM)树状大分子共轭形成LM-G2纳米盘。然后将抗癌药物DOX装载到LM-G2上,其载药效率高达98.4%,令人印象深刻,并且可以以pH敏感且持续的方式释放。此外,细胞活力测定结果表明,在相同药物浓度下,LM-G2 / DOX复合物比游离DOX更有效地抑制KB细胞(人上皮癌细胞系)的增殖。流式细胞仪分析和共聚焦激光扫描显微镜表明,KB-细胞可以比游离的DOX更有效地摄取LM-G2 / DOX。考虑到非凡的高载药效率和表面上丰富的树枝状大分子胺基团可以进一步修饰,因此开发的LM-G2纳米圆片有望成为一种新型的抗癌药物平台。

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