Effect of Different Lipid Ratios on Physicochemical Stability and Drug Release of Nanostructured Lipid Carriers Loaded Coenzyme Q10

Abdulloh Suyuti, Esti Hendradi, Tutiek Purwanti
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引用次数: 1

Abstract

Background: For treatment or skin care via topical route, Coenzyme Q10 needs to permeate the epidermis which it is practically insoluble in water and a high molecular weight that make it difficult to penetrate the skin. Nanostructured Lipid Carriers (NLC) is chosen because of its ability to dissolve and solve the problem of low skin permeation. The type and ratio of solid and liquid lipids used in NLC affect the physicochemical characteristics, thus affecting the release profile and system stability. Objective: This study aimed to determine the effect of various ratios of Compritol 888 ATO as solid lipid and Miglyol 812 as liquid lipid on the physicochemical stability and Coenzyme Q10 release profile of NLC system. Methods: NLC was prepared using High Shear Homogenization method with three different lipid ratios. The ratio of Compritol 888 ATO : Miglyol 812 was 70:30, 80:20, and 90:10, respectively. NLC was evaluated for drug release and stability parameters including organoleptic, particle size, polydispersity index (PI), pH, viscosity, assay, and entrapment efficiency. Results: The stability test result for 90 days showed increments in the particle size and viscosity, whereas for assay and entrapment efficiency were decreased. The release test results showed no significant difference in the release parameters of the three tested formulas. Conclusion: During stability evaluation, NLC-CoQ10 systems did not significantly change pH and PI values, but statistically significantly changed particle size, viscosity, assay, and entrapment efficiency. The different in lipid ratios used in the formulas did not show significantly different results for release parameters.
不同脂质比例对辅酶Q10纳米结构脂质载体的物理化学稳定性和药物释放的影响
背景:对于通过局部途径进行的治疗或皮肤护理,辅酶Q10需要渗透到表皮中,它实际上不溶于水,而且分子量高,难以渗透到皮肤中。选择纳米结构脂质载体(NLC)是因为它能够溶解并解决皮肤渗透性低的问题。NLC中使用的固体和液体脂质的类型和比例影响物理化学特性,从而影响释放特性和系统稳定性。目的:本研究旨在确定不同比例的固体脂质形式的Compitol 888 ATO和液体脂质形式的Miglyol 812对NLC系统理化稳定性和辅酶Q10释放谱的影响。方法:采用高剪切均化法制备三种不同脂质比例的NLC。Compritol 888 ATO与Miglyol 812的比例分别为70:30、80:20和90:10。评估NLC的药物释放和稳定性参数,包括感官、粒度、多分散指数(PI)、pH、粘度、测定和包封效率。结果:90天的稳定性测试结果显示颗粒大小和粘度增加,而测定和包封效率降低。释放试验结果显示,三种试验配方的释放参数没有显著差异。结论:在稳定性评估过程中,NLC-CoQ10体系没有显著改变pH和PI值,但在统计学上显著改变了颗粒大小、粘度、含量和包封率。配方中使用的不同脂质比例没有显示出释放参数的显著不同结果。
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