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EGF-coated nano-dendriplexes for tumor-targeted nucleic acid delivery in vivo

机译:EGF涂层的纳米树状复合物用于体内靶向肿瘤的核酸递送

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Abstract The clinical success of therapeutic DNA is still hindered due to the lack of effective delivery carriers. Here, we designed a tumor-targeted gene nano delivery system based on EGFR targeting strategy. Epidermal growth factor (EGF) was introduced to nano-complexes of PAMAM dendrimer and DNA via electrostatic interactions to form self-assembled PAMAM/DNA/EGF nano-complexes. The properties of self-assembled complexes were characterized by gel retardation assay and particle size and zeta potential analysis. Meanwhile, the toxicity of EGF-dendriplexes was evaluated by the MTT assay, which indicated that the complexes exhibited decreased cytotoxicity with the incorporation of EGF. We labeled polyamidoamine (PAMAM) dendrimers with FITC or a near-infrared (NIR) dye Lss670 and tested the cellular uptake in vitro and biodistribution in xenograft mouse tumor models. As compared to dendriplexes, the ternary EGF-dendriplexes showed a significantly higher cellular uptake into HepG2 cells due to the specific binding between EGF and EGF receptor (EGFR) over expressed on HepG2 cells, which resulted in the enhanced gene transfection efficiency. The biodistribution of EGF-dendriplexes in vivo was monitored with in vivo imaging technique, which indicated that EGF-dendriplexes enhanced EGFR-positive tumor-targeted biodistribution. These findings indicate that this novel nano-vector realized efficiently tumor-targeting gene delivery and high efficient gene expression in vivo, and it may possess a potential targeting gene delivery system in cancer therapy.
机译:摘要由于缺乏有效的递送载体,治疗性DNA的临床成功仍然受到阻碍。在这里,我们设计了基于EGFR靶向策略的肿瘤靶向基因纳米递送系统。通过静电相互作用将表皮生长因子(EGF)引入PAMAM树枝状大分子和DNA的纳米复合物中,形成自组装的PAMAM / DNA / EGF纳米复合物。自组装复合物的性质通过凝胶阻滞分析,粒度和ζ电势分析来表征。同时,MTT法评价了EGF-树突状复合物的毒性,表明该复合物随着EGF的掺入而显示出降低的细胞毒性。我们用FITC或近红外(NIR)染料Lss670标记了聚酰胺酰胺(PAMAM)树状大分子,并测试了异种移植小鼠肿瘤模型中的细胞摄取体外和生物分布。与树状复合体相比,三价EGF-树状复合体显示出显着更高的细胞摄取到HepG2细胞中,这是由于EGF和EGF受体(EGFR)之间的特异性结合超过了HepG2细胞上的表达,从而提高了基因转染效率。用体内成像技术监测EGF-树突状体在体内的生物分布,这表明EGF-树突状复合物增强了EGFR阳性肿瘤靶向的生物分布。这些发现表明,这种新颖的纳米载体在体内实现了有效的靶向肿瘤的基因递送和高效的基因表达,并且在癌症治疗中可能具有潜在的靶向基因递送系统。

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