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用于靶向黑素细胞和治疗黄褐斑的纳米囊泡系统:体外表征、离体皮肤滞留及初步临床评估

Nano-vesicular systems for melanocytes targeting and melasma treatment: In-vitro characterization, ex-vivo skin retention, and preliminary clinical appraisal.

作者信息

Hatem Shymaa, Kamel Amany O, Elkheshen Seham A, Nasr Maha, Moftah Noha H, Ragai Maha H, El Hoffy Nada M, Elezaby Reham S

机构信息

Department of Pharmaceutics and Pharmaceutical Technology, Faculty of Pharmacy, Future University in Egypt, Egypt.

Department of Pharmaceutics and Industrial Pharmacy, Faculty of Pharmacy, Ain Shams University, Cairo, Egypt.

出版信息

Int J Pharm. 2024 Nov 15;665:124731. doi: 10.1016/j.ijpharm.2024.124731. Epub 2024 Sep 19.

Abstract

Melasma represents an acquired melanogenesis disorder resulting in skin's hyperpigmentation effect. Although several approaches are adopted for melasma treatment, nanotechnology presents the most convenient one. Therefore, the present work aimed to formulate and characterize three nano-vesicular systems namely, liposomes, penetration enhancer containing vesicles (PEVs) and invasomes to enhance the topical delivery of the skin whitening agent; alpha arbutin (α-arbutin) for the treatment of melasma. Liposomes were prepared according to a 2 full factorial design and the selected formula was further employed for the preparation of PEVs and invasomes. Results showed that the three vesicular systems exhibited nano-sizes ranging from 151.95 to 672.5 nm, negative charges ranging from -12.50 to -28.20 mV, high entrapment efficiencies ranging from 80.59 to 99.53 %, good stability and prolonged-release of α-arbutin for 24 h after dispersion in hydrogel form. The deposition study from the vesicular hydrogel confirmed their effectiveness for the drug's accumulation in the skin reaching an average of 1.6-fold higher in the stratum corneum, 1.6-1.8-fold higher in the epidermis, and 1.6-1.8-fold higher in the dermis compared to the free drug dispersion in hydrogel. A preliminary clinical split-face study on patients suffering from melasma revealed that α-arbutin-loaded liposomes and PEVs in hydrogel forms showed better clinical outcomes compared to the free α-arbutin hydrogel as well as to the previously published α-arbutin encapsulated in chitosan nanoparticles and dispersed in hydrogel form. This delineates the aforementioned nano-vesicular systems as effective and clinically superior delivery means for melasma management.

摘要

黄褐斑是一种后天性黑素生成紊乱疾病,会导致皮肤色素沉着。尽管黄褐斑的治疗方法多种多样,但纳米技术是最便捷的一种。因此,本研究旨在制备并表征三种纳米囊泡系统,即脂质体、含渗透促进剂囊泡(PEV)和侵入体,以增强皮肤美白剂α - 熊果苷(α - arbutin)的局部递送,用于治疗黄褐斑。脂质体根据二因素全因子设计制备,所选配方进一步用于制备PEV和侵入体。结果表明,这三种囊泡系统的粒径在151.95至672.5nm之间,表面电荷在 - 12.50至 - 28.20mV之间,包封率高达80.59至99.53%,稳定性良好,以水凝胶形式分散后α - 熊果苷可缓释24小时。囊泡水凝胶的沉积研究证实了它们能有效促进药物在皮肤中的蓄积,与水凝胶中的游离药物分散体相比,角质层中的蓄积量平均高1.6倍,表皮中高1.6 - 1.8倍,真皮中高1.6 - 1.8倍。一项针对黄褐斑患者的初步临床半脸研究表明,水凝胶形式的载α - 熊果苷脂质体和PEV与游离α - 熊果苷水凝胶以及先前发表的壳聚糖纳米粒包裹并分散在水凝胶中的α - 熊果苷相比,临床效果更好。这表明上述纳米囊泡系统是治疗黄褐斑有效且临床效果更佳的递送手段。

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