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Preparation and characterization of non-viral gene delivery systems with pEGFP-C1 Plasmid DNA

机译:pEGFP-C1质粒DNA的非病毒基因递送系统的制备和表征

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In recent years, non-viral delivery systems for plasmid DNA have become particularly important. They can overcome the disadvantages of viral systems such as insertional mutagenesis and unpredicted immunogenicity. Some additional advantages of non-viral gene delivery systems are; good stability, low cost, targetability, delivery of a high amount of genetic materials. The aim of the study was to develop novel non-viral nanosystems suitable for gene delivery. Two formulations were developed for this purpose: water-in-oil microemulsion (ME) and solid lipid nanoparticles (SLN). The microemulsion was composed of Peceol, Tween 80, Plurol oleique, ethanol and water. The SLN was consisting of Precirol, Esterquat-1 (EQ1), Tween 80, Lecithin, ethanol and water. Characterization studies were carried out by measuring particle size, zeta potential, viscosity and pH. TEM imaging was performed on SLN formulations. Protection against DNase I degradation was examined. Cytotoxicity and transfection efficacy of selected formulations were tested on L929 mouse fibroblast cells. Particle sizes of complexes were below 100 nm and with high positive zeta potential. TEM images revealed that SLNs are spherical. The SLN:DNA complexes have low toxicity and good transfection ability. All results showed that the developed SLN formulations can be considered as suitable non-viral gene delivery systems.
机译:近年来,用于质粒DNA的非病毒递送系统变得特别重要。它们可以克服病毒系统的缺点,例如插入诱变和无法预测的免疫原性。非病毒基因递送系统的一些其他优点是;稳定性好,成本低,可靶向性强,传递大量遗传物质。该研究的目的是开发适用于基因传递的新型非病毒纳米系统。为此目的,开发了两种配方:油包水微乳液(ME)和固体脂质纳米颗粒(SLN)。该微乳液由Peceol,Tween 80,Plurol oleique,乙醇和水组成。 SLN由Precirol,Esterquat-1(EQ1),Tween 80,卵磷脂,乙醇和水组成。通过测量粒度,ζ电势,粘度和pH进行表征研究。对SLN配方进行TEM成像。检查了针对DNase I降解的保护。在L929小鼠成纤维细胞上测试了所选制剂的细胞毒性和转染效力。配合物的粒径小于100 nm,且具有较高的正Zeta电位。 TEM图像显示SLN是球形的。 SLN:DNA复合物具有低毒性和良好的转染能力。所有结果表明,已开发的SLN制剂可被认为是合适的非病毒基因递送系统。

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