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基于介孔 ZSM-5/KIT-6 和 ZSM-5/SBA-15 聚合物纳米复合材料的维拉帕米递药系统作为克服癌细胞多药耐药性的潜在工具。

Verapamil delivery systems on the basis of mesoporous ZSM-5/KIT-6 and ZSM-5/SBA-15 polymer nanocomposites as a potential tool to overcome MDR in cancer cells.

机构信息

Institute of Organic Chemistry with Centre of Phytochemistry, Bulgarian Academy of Sciences, 1113 Sofia, Bulgaria.

Faculty of Pharmacy, Medical University Sofia, Bulgaria.

出版信息

Eur J Pharm Biopharm. 2019 Sep;142:460-472. doi: 10.1016/j.ejpb.2019.07.021. Epub 2019 Jul 20.

DOI:10.1016/j.ejpb.2019.07.021
PMID:31336182
Abstract

ZSM-5/KIT-6 and ZSM-5/SBA-15 nanoparticles were synthesized and further modified by a post-synthesis method with (CH)SOH and (CH)NHCO(CH)COOH groups to optimize their drug loading and release kinetic profiles. The verapamil cargo drug was loaded by incipient wetness impregnation both on the parent and modified nanoporous supports. Nanocarriers were then coated with a three-layer polymeric shell composed of chitosan-k-carrageenan-chitosan with grafted polysulfobetaine chains. The parent and drug loaded formulations were characterized by powder XRD, N physisorption, thermal analysis, AFM, DLS, TEM, ATR-FT-IR and solid state NMR spectroscopies. Loading of verapamil on such nanoporous carriers and their subsequent polymer coating resulted in a prolonged in vitro release of the drug molecules. Quantum-chemical calculations were performed to investigate the strength of the interaction between the specific functional groups of the drug molecule and (CH)SOH and CH)NHCO(CH)COOH groups of the drug carrier. Furthermore, the ability of the developed nanocomposites to positively modulate the intracellular internalization and thereby augment the antitumor activity of the p-gp substrate drug doxorubicin was investigated in a comparative manner vs. free drug in a panel of MDR positive (HL-60/Dox, HT-29) and MDR negative (HL-60) human cancer cell lines using the Chou-Talalay method.

摘要

ZSM-5/KIT-6 和 ZSM-5/SBA-15 纳米粒子通过后合成方法用 (CH)SOH 和 (CH)NHCO(CH)COOH 基团进行修饰,以优化其药物负载和释放动力学特性。维拉帕米货物药物通过初始湿浸渍法同时负载在母体和修饰的纳米多孔载体上。然后,纳米载体用由壳聚糖-卡拉胶-壳聚糖组成的三层聚合壳进行涂覆,其中接枝了聚磺丁基甜菜碱链。母体和负载药物的制剂通过粉末 XRD、N 物理吸附、热分析、AFM、DLS、TEM、ATR-FT-IR 和固态 NMR 光谱进行表征。维拉帕米在这种纳米多孔载体上的负载及其随后的聚合物涂层导致药物分子的体外释放时间延长。进行量子化学计算以研究药物分子的特定功能基团与药物载体的 (CH)SOH 和 (CH)NHCO(CH)COOH 基团之间相互作用的强度。此外,通过使用 Chou-Talalay 方法在一组多药耐药阳性(HL-60/Dox、HT-29)和多药耐药阴性(HL-60)人癌细胞系中与游离药物进行比较,研究了开发的纳米复合材料在正向调节细胞内内化方面的能力,从而增强 p-糖蛋白底物药物阿霉素的抗肿瘤活性。

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