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首页> 外文期刊>Journal of microbiology and biotechnology >Selective gene transfer to hepatocellular carcinoma using homing peptide-grafted cationic liposomes
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Selective gene transfer to hepatocellular carcinoma using homing peptide-grafted cationic liposomes

机译:使用归巢肽移植的阳离子脂质体将基因选择性转移至肝细胞癌

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摘要

Gene delivery that provides targeted delivery of therapeutic genes to the cells of a lesion enhances therapeutic efficacy and reduces toxic side effects. This process is especially important in cancer therapy when it is advantageous to avoid unwanted damage to healthy normal cells. Incorporating cancer-specific ligands that recognize receptors overexpressed on cancer cells can increase selective binding and uptake and, as a result, increase targeted transgene expression. In this study, we investigated whether a peptide capable of homing to hepatocellular carcinoma (HCC) could facilitate targeted gene delivery by cationic liposomes. This homing peptide (HBP) exhibited selective binding to a human hepatocarcinoma cell line, HepG2, at a concentration ranging from 5 to 5,000 nM. When conjugated to a cationic liposome, HBP substantially increased cellular internalization of plasmid DNA to increase the transgene expression in HepG2 cells. In addition, there was no significant enhancement in gene transfer detected for other human cell lines tested, including THLE-3, AD293, and MCF-7 cells. Therefore, we demonstrate that HBP provides targeted gene delivery to HCC by cationic liposomes.
机译:提供将治疗基因靶向递送至病变细胞的基因递送增强了治疗功效并减少了毒副作用。当有利于避免对健康正常细胞的有害损害时,该过程在癌症治疗中尤其重要。掺入识别癌细胞上过表达的受体的癌症特异性配体可以增加选择性结合和摄取,结果,可以增加靶向转基因的表达。在这项研究中,我们调查了一种能够归巢到肝细胞癌(HCC)的肽是否可以促进阳离子脂质体靶向基因的传递。该归巢肽(HBP)表现出与人肝癌细胞系HepG2的选择性结合,浓度范围为5至5,000 nM。当结合到阳离子脂质体上时,HBP实质上增加了质粒DNA的细胞内在化,从而增加了HepG2细胞中的转基因表达。此外,对于其他测试的人类细胞系(包括THLE-3,AD293和MCF-7细胞),检测到的基因转移没有明显增强。因此,我们证明HBP通过阳离子脂质体向HCC提供靶向基因递送。

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