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载紫杉醇的聚电解质纳米粒作为被动靶向药物载体的有前途的候选物。

Pegylated polyelectrolyte nanoparticles containing paclitaxel as a promising candidate for drug carriers for passive targeting.

机构信息

Jerzy Haber Institute of Catalysis and Surface Chemistry Polish Academy of Sciences, Niezapominajek 8, 30-239 Kraków, Poland.

Department of Cell Biochemistry, Faculty of Biochemistry, Biophysics and Biotechnology, Jagiellonian University, 30-348 Kraków, Poland.

出版信息

Colloids Surf B Biointerfaces. 2016 Jul 1;143:463-471. doi: 10.1016/j.colsurfb.2016.03.064. Epub 2016 Mar 23.

DOI:10.1016/j.colsurfb.2016.03.064
PMID:27037784
Abstract

Targeted drug delivery systems are of special importance in cancer therapies, since serious side effects resulting from unspecific accumulation of highly toxic chemotherapeutics in healthy tissues can restrict effectiveness of the therapy. In this work we present the method of preparing biocompatible, polyelectrolyte nanoparticles containing the anticancer drug that may serve as a vehicle for passive tumor targeting. The nanoparticles were prepared via direct encapsulation of emulsion droplets in a polyelectrolyte multilayer shell. The oil cores that contained paclitaxel were stabilized by docusate sodium salt/poly-l-lysine surface complex (AOT/PLL) and were encapsulated in shells formed by the LbL adsorption of biocompatible polyelectrolytes, poly-L-glutamic acid (PGA) and PLL up to 5 or 6 layers. The surface of the nanoparticles was pegylated through the adsorption of the pegylated polyelectrolyte (PGA-g-PEG) as the outer layer to prolong the persistence of the nanocarriers in the circulation. The synthesized nanoparticles were stable in cell culture medium containing serum and their average size was 100nm, which makes them promising candidates for passive targeted drug delivery. This notion was further confirmed by the results of studying the biological effects of nanoformulations on two tumor cell lines: mouse colon carcinoma cell line CT26-CEA and the mouse mammary carcinoma cell line 4T1. The empty polyelectrolyte nanoparticles did not affect the viability of the tested cells, whereas encapsulated paclitaxel retained its strong cytotoxic/cytostatic activity.

摘要

靶向药物递送系统在癌症治疗中具有特殊意义,因为高度毒性化疗药物在健康组织中的非特异性积累导致的严重副作用可能会限制治疗的效果。在这项工作中,我们提出了一种制备含有抗癌药物的生物相容的聚电解质纳米粒子的方法,该纳米粒子可以作为被动肿瘤靶向的载体。通过将乳液液滴直接包封在聚电解质多层壳中来制备纳米粒子。含有紫杉醇的油核由十二烷基硫酸钠/聚-L-赖氨酸表面复合物(AOT/PLL)稳定,并通过生物相容的聚电解质聚-L-谷氨酸(PGA)和 PLL 的 LbL 吸附被包封在壳中,达到 5 或 6 层。纳米粒子的表面通过吸附聚乙二醇化的聚电解质(PGA-g-PEG)作为外层进行聚乙二醇化,以延长纳米载体在循环中的持久性。在含有血清的细胞培养基中,合成的纳米粒子稳定,平均粒径为 100nm,这使它们成为被动靶向药物递送的有前途的候选物。这一概念通过研究纳米制剂对两种肿瘤细胞系(小鼠结肠癌细胞系 CT26-CEA 和小鼠乳腺癌细胞系 4T1)的生物学效应得到了进一步证实。空的聚电解质纳米粒子不会影响测试细胞的活力,而包封的紫杉醇保留了其强烈的细胞毒性/细胞抑制活性。

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