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Solutol HS15 based binary mixed micelles with penetration enhancers for augmented corneal delivery of sertaconazole nitrate: optimization, in vitro , ex vivo and in vivo characterization

机译:基于Solutol HS15的二元混合胶束和渗透促进剂,用于增强硝酸舍他康唑的角膜递送:优化,体外,离体和体内表征

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Keratomycosis is a serious corneal disease that can cause a permanent visual disability if not treated effectively. Sertaconazole nitrate (STZ), a novel broad spectrum antifungal drug, was suggested as a promising treatment. However, its utility in the ocular route is restricted by its poor solubility, along with other problems facing the ocular delivery like short residence time, and the existing corneal barrier. Therefore, the objective of this study was to formulate STZ loaded binary mixed micelles (STZ-MMs) enriched with different penetration enhancers using thin-film hydration method, based on a 31.22 mixed factorial design. Different formulation variables were examined, namely, type of auxiliary surfactant, type of penetration enhancer, and total surfactants: drug ratio, and their effects on the solubility of STZ in MMs (SM), particle size (PS), polydispersity index (PDI), and zeta potential (ZP) were evaluated. STZ-MMs enhanced STZ aqueous solubility up to 338.82-fold compared to free STZ. Two optimized formulations (MM-8 and MM-11) based on the desirability factor (0.891 and 0.866) were selected by Design expert? software for further investigations. The optimized formulations were imaged by TEM which revealed nanosized spherical micelles. Moreover, they were examined for corneal mucoadhesion, stability upon dilution, storage effect, and ex vivo corneal permeation studies. Finally, both in vivo corneal uptake and in vivo corneal tolerance were investigated. MM-8 showed superiority in the ex vivo and in vivo permeation studies when compared to the STZ-suspension. The obtained results suggest that the aforementioned STZ loaded mixed micellar system could be an effective candidate for Keratomycosis-targeted therapy.
机译:角膜霉菌病是一种严重的角膜疾病,如果治疗不当,会导致永久性视力障碍。新型硝酸广谱抗真菌药硝酸舍他康唑(STZ)被认为是一种有前途的治疗方法。然而,其在眼部途径中的实用性受到其溶解性差,以及眼部递送面临的其他问题(如停留时间短)和现有角膜屏障的限制。因此,本研究的目的是基于31.22混合因子设计,通过薄膜水化法配制富含不同渗透促进剂的STZ负载二元混合胶束(STZ-MM)。检查了不同的配方变量,即辅助表面活性剂的类型,渗透促进剂的类型以及表面活性剂:药物的总比例,以及它们对STZ在MM中的溶解度(SM),粒度(PS),多分散指数(PDI)的影响,并评估了Zeta电位(ZP)。与游离STZ相比,STZ-MMs将STZ的水溶性提高了338.82倍。设计专家根据需求因子(0.891和0.866)选择了两种优化配方(MM-8和MM-11)。用于进一步调查的软件。通过TEM对优化的制剂进行成像,其显示出纳米级球形胶束。此外,还检查了它们的角膜粘膜粘附性,稀释后的稳定性,储存效果以及离体角膜渗透性研究。最后,研究了体内角膜摄取和体内角膜耐受性。与STZ悬浮液相比,MM-8在离体和体内渗透研究中显示出优越性。获得的结果表明,上述负载STZ的混合胶束系统可能是针对角膜霉菌病靶向治疗的有效候选者。

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