首页> 外文期刊>Journal of drug targeting >Efficient gene delivery with serum into human cancer cells using targeted anionic liposomes.
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Efficient gene delivery with serum into human cancer cells using targeted anionic liposomes.

机译:使用靶向阴离子脂质体将血清有效地传递到人癌细胞中。

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摘要

Success of human gene therapy depends upon the development of delivery vehicles or vectors, which can selectively deliver therapeutic genes to target cells with efficiency and safety. Previous studies have shown an efficient, systemic trans-gene expression in many cell lines (in vitro) by using an anionic liposomal vector, based on the composition of retroviral envelopes (artificial viral envelopes, AVEs). The AVE-liposomes and their complexes with plasmid (DNA) were characterized according to zeta potential measurements and transmission electron microscopy (TEM). We successfully demonstrated that AVE liposomes, dispersed in 10% serum-containing growth medium, efficiently delivered plasmid DNA to HuH-7 (human hepatoma cell line) cells. We assessed the utility of liver-targeted vesicles as a drug/gene delivery system for the treatment of liver diseases. We found that small unilamellar AVE vesicles containing 15 mol% digalactosyl diglyceride (DGDG) are efficiently targeted to the liver via the hepatic asialoglycoprotein receptor.
机译:人类基因治疗的成功取决于递送载体或载体的发展,所述载体或载体可以有效且安全地将治疗性基因选择性地递送至靶细胞。先前的研究表明,基于逆转录病毒包膜(人工病毒包膜,AVE)的组成,使用阴离子脂质体载体,可以在许多细胞系中(体外)高效,系统地表达转基因。根据ζ电势测量和透射电子显微镜(TEM)对AVE脂质体及其与质粒(DNA)的复合物进行表征。我们成功地证明,分散在含10%血清的生长培养基中的AVE脂质体可有效地将质粒DNA输送至HuH-7(人肝癌细胞系)细胞。我们评估了靶向肝的囊泡作为药物/基因传递系统治疗肝病的实用性。我们发现,包含15摩尔%的双半乳糖基甘油二酸酯(DGDG)的单层小AVE囊泡可通过肝脱唾液酸糖蛋白受体有效地靶向肝脏。

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