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Nanocarriers as Promising Novel Systems for Controlled Delivery of Diclofenac Sodium

机译:纳米载体作为有望用于控制双氯芬酸钠的新型系统

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The formulation and evaluation of diclofenac sodium from liposomes, niosomes and nanoemulsion are analyzed. The release profiles of diclofenac sodium were almost similar in all the formulations. It is found that 85% of diclofenac sodium diffused out from the colloidal systems within 8hrs and practically all the drug was released within 12hrs. In addition to this controlled release, the similarity of the release profiles obtained for liposomes, niosomes and nanoemulsion signifies that the internal structure has little role in the release process. The drug released fast and completely from the carriers upon high dilution, but it is slowed down a little when they are not diluted. The maximium amount of diclofenac sodium was released from nano emulsion as well as liposomes after 12 hrs at 1 in 200 dilution where as in niosomes, it was found at 1 in 100 dilution. But surprisingly, the release was decreased upon further dilution. The higher the surfactant content, the higher the globule size of the nanoemulsion. The mean size of the systems was decreased upon increasing dilution. Among all the systems, the mean size of niosomes was decreased upon increasing the dilution up to 1:200. It was finally depicted that the dilution effect on the zeta potential of the systems shifted from negative to positive by adding polysorbate 80. The zeta potential of all the systems was significantly good indicating stable systems.
机译:分析了脂质体,脂质体和纳米乳剂中双氯芬酸钠的配方和评价。在所有制剂中双氯芬酸钠的释放曲线几乎相似。已发现85%的双氯芬酸钠在8小时内从胶体系统中扩散出来,几乎所有药物都在12小时内释放出来。除了这种控制释放外,对于脂质体,脂质体和纳米乳剂获得的释放曲线的相似性表明,内部结构在释放过程中几乎没有作用。高稀释度时,药物可以从载体中快速完全释放出来,但是当未稀释时,药物的速度会放慢一点。在200稀释度下12小时后,纳米乳液和脂质体中释放出最大量的双氯芬酸钠,而在脂质体中,则以100稀释度下释放出双氯芬酸钠。但令人惊讶的是,进一步稀释后释放减少。表面活性剂含量越高,纳米乳液的小球尺寸越大。随着稀释度的增加,系统的平均尺寸减小。在所有系统中,将稀释液的稀释度提高至1:200时,均会降低脂质体的平均大小。最后描绘出,通过添加聚山梨酯80,对体系的ζ电势的稀释作用从负向正转变。所有系统的ζ电势都非常好,表明系统是稳定的。

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