首页> 美国卫生研究院文献>International Journal of Nanomedicine >Enhancement of physicochemical properties of nanocolloidal carrier loaded with cyclosporine for topical treatment of psoriasis: in vitro diffusion and in vivo hydrating action
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Enhancement of physicochemical properties of nanocolloidal carrier loaded with cyclosporine for topical treatment of psoriasis: in vitro diffusion and in vivo hydrating action

机译:负载环孢素的纳米胶体载体的物理化学性质的增强用于牛皮癣的局部治疗:体外扩散和体内水合作用

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摘要

Psoriasis is a chronic autoimmune disease that cannot be cured. It can however be controlled by various forms of treatment, including topical, systemic agents, and phototherapy. Topical treatment is the first-line treatment and favored by most physicians, as this form of therapy has more patient compliance. Introducing a nanoemulsion for transporting cyclosporine as an anti-inflammatory drug to an itchy site of skin disease would enhance the effectiveness of topical treatment for psoriasis. The addition of nutmeg and virgin coconut-oil mixture, with their unique properties, could improve cyclosporine loading and solubility. A high-shear homogenizer was used in formulating a cyclosporine-loaded nanoemulsion. A D-optimal mixture experimental design was used in the optimization of nanoemulsion compositions, in order to understand the relationships behind the effect of independent variables (oil, surfactant, xanthan gum, and water content) on physicochemical response (particle size and polydispersity index) and rheological response (viscosity and k-value). Investigation of these variables suggests two optimized formulations with specific oil (15% and 20%), surfactant (15%), xanthan gum (0.75%), and water content (67.55% and 62.55%), which possessed intended responses and good stability against separation over 3 months’ storage at different temperatures. Optimized nanoemulsions of pH 4.5 were further studied with all types of stability analysis: physical stability, coalescence-rate analysis, Ostwald ripening, and freeze–thaw cycles. In vitro release proved the efficacy of nanosize emulsions in carrying cyclosporine across rat skin and a synthetic membrane that best fit the Korsmeyer–Peppas kinetic model. In vivo skin analysis towards healthy volunteers showed a significant improvement in the stratum corneum in skin hydration.
机译:牛皮癣是一种无法治愈的慢性自身免疫性疾病。但是,它可以通过各种形式的治疗来控制,包括局部,全身性药物和光疗。局部治疗是一线治疗,受到大多数医生的青睐,因为这种治疗形式具有更多的患者依从性。引入用于将环孢菌素作为抗炎药运输到皮肤瘙痒部位的纳米乳剂将增强牛皮癣局部治疗的有效性。添加肉豆蔻和原始椰子油混合物具有独特的性能,可以改善环孢菌素的负载量和溶解度。使用高剪切均质机配制环孢素负载的纳米乳液。 D-最佳混合物实验设计用于优化纳米乳液的组成,以了解自变量(油,表面活性剂,黄原胶和水含量)对理化响应(粒度和多分散指数)的影响之间的关系。和流变响应(粘度和k值)。对这些变量的研究表明,两种优化配方具有特定的油(15%和20%),表面活性剂(15%),黄原胶(0.75%)和水含量(67.55%和62.55%),具有预期的响应和良好的稳定性。避免在不同温度下存放3个月以上。通过各种类型的稳定性分析进一步研究了优化的pH 4.5纳米乳液:物理稳定性,聚结速率分析,奥斯特瓦尔德熟化和冻融循环。体外释放证明了纳米乳剂在环孢菌素穿过大鼠皮肤和最适合Korsmeyer-Peppas动力学模型的合成膜上的功效。对健康志愿者的体内皮肤分析显示,角质层的皮肤水合作用显着改善。

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