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Improving anticancer activity and reducing systemic toxicity of doxorubicin by self-assembled polymeric micelles

机译:自组装聚合物胶束提高阿霉素的抗癌活性并降低全身毒性

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摘要

In an attempt to improve anticancer activity and reduce systemic toxicity of doxorubicin (Dox), we encapsulated Dox in monomethoxy poly(ethylene glycol)-poly(e-caprolactone) (MPEG-PCL) micelles by a novel self-assembly procedure without using surfactants, organic solvents or vigorous stirring. These Dox encapsulated MPEG-PCL (Dox/MPEG-PCL) micelles with drug loading of 4.2% were monodisperse and ?20 nm in diameter. The Dox can be released from the Dox/MPEG-PCL micelles; the Dox-release at pH 5.5 was faster than that at pH 7.0. Encapsulation of Dox in MPEG-PCL micelles enhanced the cellular uptake and cytotoxicity of Dox on the C-26 colon carcinoma cell in vitro, and slowed the extravasation of Dox in the transgenic zebrafish model. Compared to free Dox, Dox/MPEG-PCL micelles were more effective in inhibiting tumor growth in the subcutaneous C-26 colon carcinoma and Lewis lung carcinoma models, and prolonging survival of mice bearing these tumors. Dox/MPEG-PCL micelles also induced lower systemic toxicity than free Dox. In conclusion, incorporation of Dox in MPEG-PCL micelles enhanced the anticancer activity and decreased the systemic toxicity of Dox; these Dox/MPEG-PCL micelles are an interesting formulation of Dox and may have potential clinical applications in cancer therapy.
机译:为了提高阿霉素(Dox)的抗癌活性并降低其全身毒性,我们通过不使用表面活性剂的新型自组装程序将Dox封装在单甲氧基聚(乙二醇)-聚(ε-己内酯)(MPEG-PCL)胶束中,有机溶剂或剧烈搅拌。这些载药量为4.2%的Dox包封的MPEG-PCL(Dox / MPEG-PCL)胶束是单分散的,直径约为20 nm。 Dox可以从Dox / MPEG-PCL胶束中释放; pH 5.5时Dox释放快于pH 7.0时。 Dox在MPEG-PCL胶束中的封装增强了Dox在体外C-26结肠癌细胞上的细胞摄取和细胞毒性,并减慢了Dox在转基因斑马鱼模型中的外渗。与游离Dox相比,Dox / MPEG-PCL胶束在抑制皮下C-26结肠癌和Lewis肺癌模型中的肿瘤生长方面更有效,并且可以延长携带这些肿瘤的小鼠的生存期。 Dox / MPEG-PCL胶束的全身毒性也比游离Dox低。总之,在MPEG-PCL胶束中掺入Dox可增强Dox的抗癌活性并降低其全身毒性。这些Dox / MPEG-PCL胶束是Dox的有趣配方,在癌症治疗中可能具有潜在的临床应用。

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