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首页> 外文期刊>Journal of Bioactive and Compatible Polymers >Specific gene delivery mediated by poly(ethylene glycol)-grafted polyamidoamine dendrimer modified with a novel HER2-targeting nanobody
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Specific gene delivery mediated by poly(ethylene glycol)-grafted polyamidoamine dendrimer modified with a novel HER2-targeting nanobody

机译:新型靶向HER2的纳米抗体修饰的聚乙二醇接枝聚酰胺胺树枝状大分子介导的特定基因传递

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摘要

As compared to other nanobiopolymers used in gene delivery applications, polyamidoamine dendrimers possess significantly improved physical and chemical properties such as monodispersity, well-defined size and shape, and biocompatibility, which make them ideal vectors for biomedical purposes. The aim of this study was fine-tuning of an anti-human epidermal growth factor receptor 2 (HER2) nanobody-polyethylene glycol (PEG)-G5 polyamidoamine gene delivery vector for potential in vivo applications. Polyethylene glycol was conjugated to polyamidoamine dendrimers at three different molar ratios of 10, 20, and 30 (polyethylene glycol: polyamidoamine). Anti-HER2 nanobody was chosen as our targeting agents and attached to polyethylene glycol-polyamidoamine conjugates. Cytotoxicity assays and transfection studies were carried out to find the most efficient conjugate in terms of both low cytotoxicity and high transfection rate. Our data indicated that PEGylation decreased the cytotoxicity of dendrimers alone and when complexed with DNA (dendriplexes). Among all of the polyethylene glycol-polyamidoamine dendrimers, polyethylene glycol(10)-polyamidoamine resulted in the most efficient gene transfection vector in both BT-474 and MCF-10A cell lines. Incorporation of anti-HER2 nanobodies could further increase their cellular uptake up to 1.7-fold compared to native dendrimers in HER2-overexpressing BT-474 cells but not in HER2-negative MCF-10A cells. It can be concluded from our results that nanobody-polyethylene glycol-polyamidoamine conjugates might be a promising new bioconjugate for the targeted gene delivery to HER2-positive tumor cells in vivo.
机译:与基因递送应用中使用的其他纳米生物聚合物相比,聚酰胺酰胺树状聚合物具有显着改善的物理和化学特性,例如单分散性,明确定义的大小和形状以及生物相容性,使其成为用于生物医学目的的理想载体。这项研究的目的是为潜在的体内应用微调抗人类表皮生长因子受体2(HER2)纳米抗体-聚乙二醇(PEG)-G5聚酰胺酰胺基因传递载体。聚乙二醇以三种不同的摩尔比10、20和30(聚乙二醇:聚酰胺型胺)与聚酰胺型胺树枝状聚合物结合。选择抗-HER2纳米抗体作为我们的靶向剂,并将其连接到聚乙二醇-聚酰胺基共轭物上。进行了细胞毒性测定和转染研究,以发现在低细胞毒性和高转染率方面最有效的缀合物。我们的数据表明,聚乙二醇化降低了单独的树状聚合物以及与DNA复合时(树状复合物)的细胞毒性。在所有聚乙二醇-聚酰胺酰胺树状聚合物中,聚乙二醇(10)-聚酰胺酰胺导致BT-474和MCF-10A细胞系中最有效的基因转染载体。与HER2过表达的BT-474细胞中的天然树状大分子相比,抗HER2纳米抗体的掺入可进一步将其细胞摄取提高至1.7倍,而在HER2阴性MCF-10A细胞中则没有。从我们的结果可以得出结论,纳米抗体-聚乙二醇-聚酰胺酰胺偶联物可能是一种有前途的新生物偶联物,可用于体内靶向基因递送至HER2阳性肿瘤细胞。

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