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Nonionic Microemulsions as Solubilizers of Hydrophobic Drugs: Solubilization of Paclitaxel

机译:非离子微乳液作为疏水药物的增溶剂:紫杉醇的增溶

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摘要

The strategy using nonionic microemulsion as a solubilizer for hydrophobic drugs was studied and is demonstrated in this work. The aqueous phase behaviors of mixed nonionic surfactants with various oils at 37 °C are firstly constructed to give the optimal formulations of nonionic microemulsions with applications in the enhanced solubilization of the model hydrophobic drug, paclitaxel, at 37 °C. Briefly, the suitable oil phase with paclitaxel significantly dissolved is microemulsified with appropriate surfactants. Surfactants utilized include Tween 80, Cremophor EL, and polyethylene glycol (4.3) cocoyl ether, while various kinds of edible oils and fatty esters are used as the oil phase. On average, the apparent solubility of paclitaxel is increased to ca. 70–100 ppm in the prepared microemulsions at 37 °C using tributyrin or ethyl caproate as the oil phases. The sizes of the microemulsions attained are mostly from ca. 60 nm to ca. 200 nm. The cytotoxicity of the microemulsion formulations is assessed with the cellular viability of 3T3 cells. In general, the cell viability is above 55% after 24 h of cultivation in media containing these microemulsion formulations diluted to a concentration of total surfactants equal to 50 ppm and 200 ppm.
机译:研究了使用非离子型微乳液作为疏水药物的增溶剂的策略,并在这项工作中得到了证明。首先构建了在37°C下与各种油混合的非离子表面活性剂的水相行为,以提供非离子微乳液的最佳配方,并用于在37°C下增强模型疏水性药物紫杉醇的增溶作用。简而言之,将具有明显溶解的紫杉醇的合适的油相用合适的表面活性剂微乳化。使用的表面活性剂包括吐温80,Cremophor EL和聚乙二醇(4.3)椰子油醚,而各种食用油和脂肪酯用作油相。平均而言,紫杉醇的表观溶解度增加至约10。在37°C下使用三丁酸甘油酯或己酸乙酯作为油相制备的微乳液中的浓度为70–100 ppm。所获得的微乳液的大小主要来自约。 60 nm至大约200纳米用3T3细胞的细胞生存力评估微乳剂的细胞毒性。通常,在含有稀释至总表面活性剂浓度等于50 ppm和200 ppm的这些微乳液制剂的培养基中培养24小时后,细胞活力高于55%。

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