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Physicochemical and cytotoxicity analysis of glycerol monoolein-based nanoparticles

机译:基于甘油单烯醇基纳米粒子的物理化学和细胞毒性分析

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Lyotropic liquid crystalline dispersions, such as cubosomes, have been proposed as potential drug delivery vehicles. A recently described 'salt induced' method of cubosome production may be suitable for the encapsulation of macromolecular bioactive therapeutics, such as proteins, within the cubic phase. Here, we develop and characterise glycerol-monoolein (GMO)-based cubosomes using this novel method of cubosome production. Using the anionic biological lipid 1,2-dipalmitoyl phosphatidylserine (DPPS) to prevent GMO from forming its natural cubic-phase, we validate that addition of phosphate buffered saline (PBS) can be used to reverse the effects of DPPS. However, this transition is dependent on the type of Pluronic (R) block copolymer stabiliser used to prevent re-flocculation of the cubosome dispersions. Using small angle X-ray scattering (SAXS) and cryogenic transmission electron microscopy, we show that the 'salt induced' phase transition, from small unilamellar vesicles to cubosomes, is inhibited when using Pluronic (R) F127. In contrast, using the larger, more hydrophilic stabiliser Pluronic (R) F108, cubosomes can be formed, although further analysis using SAXS suggests these GMO-based cubosomes are less thermally stable than those comprising GMO alone. In addition, we find no significant difference in the in vitro cytotoxicity of cubosome dispersions formed using either of these stabilisers, or between those containing DPPS and those without. The ability to control cubic phase transitions may present an opportunity for the incorporation of therapeutically relevant proteins in these nanoparticles.
机译:已经提出了典型液晶分散体,例如立方体,作为潜在的药物递送载体。最近描述的“盐诱导”的立方体生产方法可以适用于在立方相中封装大分子生物活性治疗剂,例如蛋白质。在这里,我们使用这种新的立方体生产方法开发和表征甘油 - 单烯醇素(GMO)的基础缔约置。使用阴离子生物脂质脂质1,2-Dipalmitoyl磷脂酰丝氨酸(DPP)以防止Gmo形成其天然立方相,我们验证磷酸盐缓冲盐水(PBS)的添加可用于逆转DPP的影响。然而,这种转变取决于Pluronic嵌段共聚物稳定剂的类型,用于防止卧间分散体的再絮凝。使用小角度X射线散射(萨克斯)和低温透射电子显微镜,我们表明使用Pluronic(R)F127时,从小非偶集囊泡到缔囊泡的“盐诱导的”相转变。相反,使用较大的更亲水性稳定剂PluronicF108,可以形成突起,尽管使用SAXS进一步分析表明这些基于GMO的突起比单独包含GMO的基因稳定性较小。此外,我们发现使用这些稳定剂中任一种或含有DPP的那些的缔约方组分散体的体外细胞毒性没有显着差异,以及没有。控制立方相转变的能力可以在这些纳米颗粒中掺入治疗相关蛋白质的机会。

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