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Preparation and characterization of magnetic cationic liposome in gene delivery.

机译:基因传递中磁性阳离子脂质体的制备与表征。

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Low transfection efficiency in vivo and failure to deliver therapeutic nucleic acids to the target organs limit the use of cationic liposomes (CLs) in gene therapy. Magnetic drug targeting (MDT) was applied in this study to improve the transfection efficiency and overcome the limitations. Magnetic cationic liposomes (MCLs) were prepared by incorporating MAG-T (magnetite) into CLs. The inclusion of relatively high concentration of MAG-T significantly increased the size of liposomes/lipoplexes, reduced the zeta potential, and decreased the cell viability. The transfection efficiency of MCLs in gene delivery was evaluated by using plasmid DNA (pDNA) containing a luciferase reporter gene in THLE-3 cells. Results suggested that the transfection efficiency of MCLs/pDNA complexes with a relatively lower content of MAG-T (0.75mg/ml) was the same as that of CLs/pDNA complexes without a magnetic field but was higher (about 2.6-fold) with magnetic induction. Finally, using MCLs/pDNA complexes and a static magnetic field placed over the liver of rats, luciferase reporter gene expression in the liver increased as compared to MCLs/pDNA complexes and CLs/pDNA complexes in the absence of an external magnetic field.
机译:体内的低转染效率以及无法将治疗性核酸递送至靶器官均限制了阳离子脂质体(CLs)在基因治疗中的使用。磁性药物靶向(MDT)被用于这项研究中,以提高转染效率并克服局限性。磁性阳离子脂质体(MCL)是通过将MAG-T(磁铁矿)掺入CL制备的。包含相对较高浓度的MAG-T会显着增加脂质体/脂质复合物的大小,降低zeta电位并降低细胞活力。通过在THLE-3细胞中使用含有荧光素酶报告基因的质粒DNA(pDNA)评估了MCL在基因传递中的转染效率。结果表明,具有相对较低的MAG-T(0.75mg / ml)的MCLs / pDNA复合物的转染效率与没有磁场的CLs / pDNA复合物的转染效率相同,但较高(约2.6倍)。磁感应。最后,与MCLs / pDNA复合物和CLs / pDNA复合物相比,在没有外部磁场的情况下,使用MCLs / pDNA复合物和置于大鼠肝脏上的静磁场,肝脏中的荧光素酶报告基因表达增加。

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