首页> 外文期刊>Journal of drug targeting >Paclitaxel-loaded PLGA nanoparticles surface modified with transferrin and Pluronic((R))P85, an in vitro cell line and in vivo biodistribution studies on rat model.
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Paclitaxel-loaded PLGA nanoparticles surface modified with transferrin and Pluronic((R))P85, an in vitro cell line and in vivo biodistribution studies on rat model.

机译:用转铁蛋白和Pluronic(R)P85表面修饰的紫杉醇载PLGA纳米颗粒,在大鼠模型上进行了体外细胞系和体内生物分布研究。

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摘要

The development of multidrug resistance (due to drug efflux by P-glycoproteins) is a major drawback with the use of paclitaxel (PTX) in the treatment of cancer. The rationale behind this study is to prepare PTX nanoparticles (NPs) for the reversal of multidrug resistance based on the fact that PTX loaded into NPs is not recognized by P-glycoproteins and hence is not effluxed out of the cell. Also, the intracellular penetration of the NPs could be enhanced by anchoring transferrin (Tf) on the PTX-PLGA-NPs. PTX-loaded PLGA NPs (PTX-PLGA-NPs), Pluronic((R))P85-coated PLGA NPs (P85-PTX-PLGA-NPs), and Tf-anchored PLGA NPs (Tf-PTX-PLGA-NPs) were prepared and evaluted for cytotoxicity and intracellular uptake using C6 rat glioma cell line. A significant increase in cytotoxicity was observed in the order of Tf-PTX-PLGA-NPs > P85-PTX-PLGA-NPs > PTX-PLGA-NPs in comparison to drug solution. In vivo biodistribution on male Sprague-Dawley rats bearing C6 glioma (subcutaneous) showed higher tumor PTX concentrations in animals administered with PTX-NPs compared to drug solution.
机译:使用紫杉醇(PTX)治疗癌症时,多药耐药性的发展(由于P-糖蛋白的药物外排)是一个主要缺点。这项研究的基本原理是基于P-糖蛋白无法识别加载到NPs中的PTX并因此不将其释放出细胞这一事实,为逆转多药耐药性制备PTX纳米颗粒(NP)。而且,可以通过将转铁蛋白(Tf)锚定在PTX-PLGA-NP上来增强NP的细胞内渗透。装有PTX的PLGA NP(PTX-PLGA-NP),Pluronic(R)P85涂层的PLGA NP(P85-PTX-PLGA-NP)和Tf固定PLGA NP(Tf-PTX-PLGA-NP)是用C6大鼠神经胶质瘤细胞系制备并评估其细胞毒性和细胞内摄取。与药物溶液相比,观察到Tf-PTX-PLGA-NPs> P85-PTX-PLGA-NPs> PTX-PLGA-NPs的细胞毒性显着增加。与药物溶液相比,在接受C6胶质瘤(皮下)的雄性Sprague-Dawley大鼠中,其体内生物分布显示较高的肿瘤PTX浓度。

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