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首页> 外文期刊>Colloids and Surfaces, B. Biointerfaces >Tunable pDNA/DODAB:MO lipoplexes: The effect of incubation temperature on pDNA/DODAB:MO lipoplexes structure and transfection efficiency
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Tunable pDNA/DODAB:MO lipoplexes: The effect of incubation temperature on pDNA/DODAB:MO lipoplexes structure and transfection efficiency

机译:可调节的pDNA / DODAB:MO脂质复合物:孵育温度对pDNA / DODAB:MO脂质复合物的结构和转染效率的影响

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Dioctadecyldimethylammonium bromide (DODAB): 1-monooleoyl-rac-glycerol (MO) cationic liposomes were reported as a promising alternative to common transfection agents, showing superior effectiveness on the transfection of the 293T mammalian cell line with pSV-β-gal plasmid DNA. The study of DODAB: MO aggregates in the absence of DNA has indicated that their morphology depends on the balance between DODAB's tendency to form bilayer structures and MO's propensity to form inverted non-lamellar structures. Other parameters, such as the temperature have proved to be crucial in the definition of the morphology of the developed nanocarrier. Therefore, in this work, a step forward to the current gene carrier system will be given by studying the effect of the tunable parameters (incubation temperature and MO content) on the structure of pDNA:DODAB:MO lipoplexes. More importantly, the implications that these tunable parameters could have in terms of lipoplex transfection efficiency will be investigated. Dynamic light scattering(DLS), zeta (ζ) potential, cryo-transmission electron microscopy (cryo-TEM) and ethidium bromide (EtBr) exclusion were used to assess the formation, structure and destabilization of pDNA:DODAB:MO lipoplexes at DODAB molar fractions of (1:1) and above equimolarity (2:1,4:1) prepared at incubation temperatures from 25 to 50 ℃. Experimental results indicate that pDNA:DODAB:MO's structure is sensitive to the lipoplex incubation temperature, resulting in particles of distinct size, superficial charge and structure. These variations are also visible on the complexation dynamics of pDNA, and subsequent release upon incubation with the model proteoglycan heparin (HEP), at 25 and 50 ℃. Increase in temperature leads to re-organization of DODAB and MO molecules within the liposomal formulation, causing a positive charge re-localization in the lipoplex surface, which not only alters its structure but also its transfection efficiency. Altogether, these results confirm that in the DODAB:MO carriers, an increase in the incubation temperature has a similar effect on aggregate morphology as the observed with an increase in MO content. This conclusion is extended to the pDNA:DODAB:MO lipoplexes morphology and subsequent transfection efficiency defining new strategies in lipoplexes preparation that could be used to modulate the properties of other lipid formulations for nonviral gene delivery applications.
机译:据报道,二十八烷基二甲基溴化铵(DODAB):1-单油酰基-外消旋甘油(MO)阳离子脂质体是常见转染剂的一种有前途的替代品,在用pSV-β-gal质粒DNA转染293T哺乳动物细胞系中显示出优异的效果。对DODAB的研究:MO在没有DNA的情况下聚集,其形态取决于DODAB形成双层结构的趋势与MO形成倒置非层状结构的倾向之间的平衡。事实证明,其他参数(例如温度)对于所开发的纳米载体的形态定义至关重要。因此,在这项工作中,将通过研究可调参数(孵育温度和MO含量)对pDNA:DODAB:MO脂质复合物结构的影响,向当前的基因载体系统迈出一步。更重要的是,将研究这些可调参数对脂质复合物转染效率的影响。使用动态光散射(DLS),ζ(ζ)电位,低温透射电子显微镜(cryo-TEM)和溴化乙锭(EtBr)排除来评估DODAB摩尔处pDNA:DODAB:MO脂质复合物的形成,结构和去稳定作用在25至50℃的孵育温度下制备的(1:1)和等摩尔以上(2:1,4:1)的馏分。实验结果表明,pDNA:DODAB:MO的结构对脂质复合体的孵育温度敏感,从而导致了大小不同,表面电荷和结构不同的颗粒。这些变化在pDNA的复合动力学上也很明显,随后在25和50℃与蛋白多糖肝素(HEP)孵育后释放。温度升高导致脂质体制剂中的DODAB和MO分子重新组织,从而在脂质复合物表面引起正电荷重新定位,这不仅改变了其结构,而且改变了其转染效率。总而言之,这些结果证实了在DODAB:MO载体中,孵育温度的升高对聚集体形态具有与观察到的相似的MO含量增加的影响。该结论扩展到pDNA:DODAB:MO脂质复合物形态学和随后的转染效率,定义了脂质复合物制备中的新策略,可用于调节其他脂质制剂在非病毒基因递送应用中的特性。

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