首页> 外文期刊>ACS Omega >Effect of Vitamin E and a Long-Chain Alcohol n-Octanol on the Carbohydrate-Based Nonionic Amphiphile Sucrose Monolaurate—Formulation of Newly Developed Niosomes and Application in Cell Imaging
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Effect of Vitamin E and a Long-Chain Alcohol n-Octanol on the Carbohydrate-Based Nonionic Amphiphile Sucrose Monolaurate—Formulation of Newly Developed Niosomes and Application in Cell Imaging

机译:维生素E和长链醇正辛醇对以碳水化合物为基础的非离子两亲性蔗糖单月桂酸酯的作用—新制备的脂质体的制备及其在细胞成像中的应用

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We have introduced new niosome formulations using sucrose monolaurate, vitamin E and n -octanol as independent additives. Detailed characterization techniques including turbidity, dynamic light scattering, transmission electron microscopy, ξ potential, and proton nuclear magnetic resonance measurements have been introduced to monitor the morphological transition of the carbohydrate-based micellar assembly into niosomal aggregates. Moreover, microheterogeneity of these niosomal aggregates has been investigated through different fluorescence spectroscopic techniques using a hydrophobic probe molecule coumarin 153 (C153). Further, it has been observed that vitamin E and octanol have an opposing effect on the rotational motion of C153 in the respective niosome assemblies. The time-resolved anisotropy studies suggest that incorporation of vitamin E and octanol into the surfactant aggregates results in slower and faster rotational motion of C153, respectively, compared to the micellar assemblies. Moreover, the ability to entrap a probe molecule by these niosomes is utilized to encapsulate and deliver the anticancer drug doxorubicin inside the mammalian cells which is monitored through fluorescence microscopic images. Interestingly, the niosome composed of vitamin E demonstrated better cytocompatibility toward primary chondrocyte cell lines compared to the octanol-forming niosome.
机译:我们已经引入了使用蔗糖单月桂酸酯,维生素E和正辛醇作为独立添加剂的新的脂质体制剂。已经引入了详细的表征技术,包括浊度,动态光散射,透射电子显微镜,ξ电势和质子核磁共振测量,以监测基于碳水化合物的胶束组装体向核糖体聚集体的形态转变。此外,已经通过使用疏水性探针分子香豆素153(C153)的不同荧光光谱技术研究了这些染色体聚集体的微异质性。此外,已经观察到维生素E和辛醇对各个脂质体组件中C153的旋转运动具有相反的作用。时间分辨各向异性研究表明,与胶束组件相比,将维生素E和辛醇掺入表面活性剂聚集体分别导致C153的旋转运动更慢和更快。而且,利用这些脂质体捕获探针分子的能力被用于在哺乳动物细胞内包封和递送抗癌药阿霉素,这通过荧光显微镜图像进行监测。有趣的是,与形成辛醇的脂质体相比,由维生素E组成的脂质体对原代软骨细胞系表现出更好的细胞相容性。

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