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首页> 外文期刊>Drug delivery. >New pharmaceutical microemulsion system for encapsulation and delivery of diospyrin, a plant-derived bioactive quinonoid compound.
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New pharmaceutical microemulsion system for encapsulation and delivery of diospyrin, a plant-derived bioactive quinonoid compound.

机译:新的药物微乳化系统,用于囊封和递送植物来源的生物活性醌类化合物薯精。

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摘要

A new vegetable oil based oil-in-water microemulsion is developed and characterized as a prospective delivery system for in vivo application A particular weight percent composition 5/30/65 (clove oil/Tween-20/water) was selected (V1) from the clear oil-in-water zone of the pseudoternary phase diagram comprising clove oil, polyoxyethylene sorbitan monolaurate (Tween-20), and water. Two modifications of V1, (V2 and V3) were prepared by addition of dipalmitoyl phosphatidyl choline (DPPC), and a mixture of DPPC and cholesterol, respectively. A model drug diospyrin (a plantderived quinonoid compound) was encapsulated in the dispersed clove oil droplets of the three systems and designated as DV1, DV2, and DV3, respectively. The size of the dispersed clove oil droplets ranged between 9-20 nm as determined by dynamic light scattering. The stability of the vehicles, before and after encapsulation, was assessed under varying conditions of time and temperature and was found to be stable for 1 year and over a temperature range of 4-40 degrees C. The ultraviolet-visible spectrum of diospyrin after encapsulation in the compartmentalized medium remained almost identical to that dissolved in chloroform. The single-dose acute toxicity of V1 and DV1 was assessed in vivo by carrying out survival study and enzyme assay in Swiss Albino mice.The vehicle was safe at a volume of 0.05 ml when injected intraperitoneally into the mice.
机译:开发了一种新的基于植物油的水包油型微乳液,并将其表征为体内应用的预期递送系统。从中选择了特定重量百分比的组合物5/30/65(丁香油/ Tween-20 /水)(V1)准三元相图中的透明水包油区,包含丁香油,聚氧乙烯脱水山梨糖醇单月桂酸酯(Tween-20)和水。通过分别添加二棕榈酰磷脂酰胆碱(DPPC)以及DPPC和胆固醇的混合物来制备V1的两个修饰(V2和V3)。将模型药物鬼臼毒素(一种植物衍生的醌类化合物)封装在三个系统的丁香油小滴中,分别命名为DV1,DV2和DV3。通过动态光散射测定,分散的丁香油滴的大小在9-20 nm之间。在不同的时间和温度条件下评估了载体在封装前后的稳定性,发现其在4-40摄氏度的温度范围内稳定了1年。封装后的二硫精的紫外-可见光谱在间隔介质中的溶解度几乎与溶解在氯仿中的溶解度相同。通过在瑞士白化病小鼠中进行存活研究和酶分析,对V1和DV1的单剂量急性毒性进行了体内评估。当腹膜内注射给小鼠时,该媒介物的安全剂量为0.05 ml。

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