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SAXS investigation of a cubic to a sponge (L3) phase transition in self-assembled lipid nanocarriers

机译:自组装脂质纳米载体中立方到海绵(L3)相变的SAXS研究

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The encapsulation and release of peptides, proteins, nucleic acids, and drugs in nanostructured lipid carriers depend on the type of the self-assembled liquid-crystalline organization and the structural dimensions of the aqueous and membraneous compartments, which can be tuned by the multicomponent composition of the systems. In this work, small-angle X-ray scattering (SAXS) investigation is performed on the 'melting' transition of the bicontimious double diamond cubic phase, formed by pure glycerol monooleate (MO), upon progressive inclusion of varying fractions of pharmaceutical-grade glycerol monooleate (GO) in the hydrated system. The self-assembled MO/GO mixtures are found to form diamond (Priirri) inverted cubic, inverted hexagonal (H_(II)), and sponge (L3) phases at ambient temperature in excess of aqueous medium without heat treatment. Mixing of the inverted-cubic-phase-forming MO and the sponge-phase-forming GO components, in equivalent proportions (50/50 w/w), yields an inverted hexagonal (H_(II)) phase nanostructured carrier. Scattering models are applied for fitting of the experimental SAXS patterns and identification of the structural changes in the aqueous and lipid bilayer subcompartments. The possibility of transforming, at ambient temperature (20 °C), the bicontinuous cubic nanostructures into inverted hexagonal (H_(II)) or sponge (L3) mesophases may facilitate novel biomedical applications of the investigated liquid crystalline self-assemblies.
机译:肽,蛋白质,核酸和药物在纳米结构脂质载体中的包封和释放取决于自组装液晶组织的类型以及水性和膜状隔室的结构尺寸,可通过多组分组成进行调整的系统。在这项工作中,小剂量X射线散射(SAXS)研究是在逐步掺入不同含量的药物级分后,由纯甘油单油酸酯(MO)形成的双连双金刚石立方相的“熔融”转变。水合系统中的甘油单油酸酯(GO)。发现自组装的MO / GO混合物在环境温度下在未经热处理的情况下,会在超过水性介质的情况下形成金刚石(Priirri)倒立立方,倒六角形(H_(II))和海绵(L3)相。以等比例(50/50 w / w)混合倒立方相的MO和形成海绵相的GO组分,即可得到倒六方(H_(II))相纳米结构载体。散射模型用于拟合实验SAXS模式,并确定水和脂质双层子隔间的结构变化。在环境温度(20°C)下,将双连续立方纳米结构转变为倒六方(H_(II))或海绵(L3)中间相的可能性可能有助于所研究的液晶自组装体的新型生物医学应用。

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