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Enhanced delivery efficiency of recombinant adenovirus into tumor and mesenchymal stem cells by a novel PTD

机译:新型PTD提高重组腺病毒向肿瘤和间充质干细胞的递送效率

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Protein transduction domains (PTDs) are small peptides that facilitate the transduction of large molecules such as polyproteins, DNA and viruses into a eukaryotic cell. Here, we demonstrated that a novel PTD (HP4) derived from herring protamine appeared to enter C6Bu1 rat glioma cell lines more rapidly than other known PTDs such as Tat, Antp and Hph-1. Moreover, HP4 significantly enhanced in vitro transduction of recombinant adenoviruses (rAds) into various cancer cell lines, mesenchymal stem cells (MSCs) and dendritic cells, which are relatively resistant to rAd infection. Enhancement of rAd delivery into C6Bu1 and MSCs by HP4 is 20 and 7 times higher than that by Tat, respectively. The increase in the expression of rAd encoding IL-12N220L by HP4 is proportional to its antitumor effect in the ex vivo transduced mouse colon cancer model. Thus, these results suggest that HP4 could be utilized to improve the transduction efficiency of rAd, resulting in enhanced efficacy of rAd-mediated gene therapy, especially for ex vivo-transduced cell therapy.
机译:蛋白质转导域(PTD)是小肽,可促进将大分子(例如多蛋白,DNA和病毒)转导到真核细胞中。在这里,我们证明了从鲱鱼精蛋白衍生的新型PTD(HP4)似乎比其他已知PTD(例如Tat,Antp和Hph-1)更快地进入C6Bu1大鼠神经胶质瘤细胞系。此外,HP4显着增强了重组腺病毒(rAds)体外转导至各种对rAd感染具有抵抗力的癌细胞系,间充质干细胞(MSCs)和树突状细胞的能力。 HP4对rAd递送至C6Bu1和MSC的作用分别比Tat高20倍和7倍。 HP4编码IL-12N220L的rAd的表达增加与其在体外转导的小鼠结肠癌模型中的抗肿瘤作用成正比。因此,这些结果表明HP4可用于改善rAd的转导效率,从而导致rAd介导的基因治疗的功效增强,尤其是离体转导的细胞治疗。

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