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首页> 外文期刊>International Journal of Nanomedicine >Peptide T7-modified polypeptide with disulfide bonds for targeted delivery of plasmid DNA for gene therapy of prostate cancer
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Peptide T7-modified polypeptide with disulfide bonds for targeted delivery of plasmid DNA for gene therapy of prostate cancer

机译:具有二硫键的肽T7修饰的多肽可靶向递送质粒DNA用于前列腺癌的基因治疗

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摘要

Background: Vectors are essential for successful gene delivery. In the present study, a tumor-targeting cationic gene vector, known as the disulfide cross-linked arginine-aspartic acid peptide modified by HAIYPRH (T7) peptide (CRD-PEG-T7), was designed for targeted delivery of plasmid DNA (pDNA) for gene therapy of prostate cancer (PCa). Methods: The structure of CRD-PEG-T7 was determined and the cellular uptake efficacy, gene transfection efficacy, cytotoxicity, and the targeting effect of the CRD-PEG-T7–plasmid DNA complex were examined. Results: The results demonstrated that the CRD-PEG-T7–plasmid DNA complex was nanosized and had a positively charged surface, good cellular uptake efficacy, minimal cytotoxicity, and a dual-targeting effect as compared with the CRD-PEG–plasmid DNA complex. The peptide T7-modifed new delivery system was able to target the highly expressed transferrin receptor (TfR) on tumor cells with an efficiency four-fold higher than that of the non-modified system. Conclusion: The results above indicatd that the CRD-PEG-T7–plasmid DNA complex may prove to be a promising gene delivery system targeting bone-metastatic tumor.
机译:背景:载体对于成功的基因传递至关重要。在本研究中,设计了一种靶向肿瘤的阳离子基因载体,即被HAIYPRH(T7)肽(CRD-PEG-T7)修饰的二硫键交联的精氨酸-天冬氨酸肽,用于靶向递送质粒DNA(pDNA )用于前列腺癌(PCa)的基因治疗。方法:确定CRD-PEG-T7的结构,并检测CRD-PEG-T7-质粒DNA复合物的细胞摄取功效,基因转染功效,细胞毒性和靶向作用。结果:结果表明,与CRD-PEG-质粒DNA复合物相比,CRD-PEG-T7-质粒DNA复合物具有纳米大小,表面带正电荷,具有良好的细胞摄取功效,细胞毒性最小,并且具有双重靶向作用。肽T7修饰的新传递系统能够靶向高表达的转铁蛋白受体(TfR)在肿瘤细胞上,其效率是非修饰系统的四倍。结论:以上结果表明,CRD-PEG-T7-质粒DNA复合物可能被证明是针对骨转移肿瘤的有前途的基因传递系统。

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