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Chemo-biologic combinatorial drug delivery using folate receptor-targeted dendrimer nanoparticles for lung cancer treatment

机译:使用叶酸受体靶向的树枝状大分子纳米粒子进行化学生物学组合药物递送以治疗肺癌

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摘要

Co-administration of functionally distinct anti-cancer agents has emerged as an efficient strategy in lung cancer treatment. However, a specially designed drug delivery system is required to co-encapsulate functionally different agents, such as a combination of siRNA and chemotherapy, for targeted delivery. We developed a folic acid (FA) -conjugated polyamidoamine dendrimer (Den) -based nanoparticle (NP) system for co-delivery of siRNA against HuR mRNA (HuR siRNA) and cis-diamine platinum (CDDP) to folate receptor-α (FRA) -overexpressing H1299 lung cancer cells. The co-delivery of HuR siRNA and CDDP using the FRA-targeted NP had a significantly greater therapeutic effect than did individual therapeutics. Further, the FRA-targeted NP exhibited improved cytotoxicity compared to non-targeted NP against lung cancer cells. Finally, the NP showed negligible toxicity towards normal MRC9 lung fibroblast cells. Thus, the present study demonstrates FRA-targeted Den nanoparticle system as a suitable carrier for targeted co-delivery of siRNA and chemotherapy agents in lung cancer cells.
机译:在肺癌治疗中,功能上独特的抗癌药的共同给药已成为一种有效策略。但是,需要专门设计的药物递送系统来共封装功能不同的药物(例如siRNA和化学疗法的组合)以进行靶向递送。我们开发了基于叶酸(FA)的聚酰胺酸胺树枝状聚合物(Den)的纳米颗粒(NP)系统,可共同递送针对HuR mRNA的siRNA(HuR siRNA)和顺式二胺铂(CDDP)到叶酸受体-α(FRA) )-过表达H1299肺癌细胞。使用FRA靶向的NP共同递送HuR siRNA和CDDP的治疗效果比单独的治疗剂要大得多。此外,与针对肺癌细胞的非靶向NP相比,针对FRA的NP表现出改善的细胞毒性。最后,NP对正常MRC9肺成纤维细胞的毒性可忽略不计。因此,本研究证明以FRA为靶标的Den纳米颗粒系统可作为siRNA和化学治疗剂在肺癌细胞中靶向共递送的合适载体。

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