熊果酸
哈卡特
银屑病
透皮
人口
角质形成细胞
化学
药理学
生物医学工程
皮肤病科
医学
色谱法
体外
生物化学
环境卫生
作者
Małgorzata Miastkowska,Agnieszka Kulawik‐Pióro,Elwira Lasoń,Karolina Śliwa,Magdalena Anna Malinowska,Elżbieta Sikora,Tomasz Kantyka,Ewa Bielecka,Anna Maksylewicz,Emilia Klimaszewska,Marta Ogorzałek,Małgorzata Tabaszewska,Łukasz Skoczylas,Krzysztof Nowak
出处
期刊:Pharmaceutics
[MDPI AG]
日期:2023-10-31
卷期号:15 (11): 2559-2559
被引量:5
标识
DOI:10.3390/pharmaceutics15112559
摘要
Psoriasis is a chronic disorder that causes a rash with itchy, scaly patches. It affects nearly 2-5% of the worldwide population and has a negative effect on patient quality of life. A variety of therapeutic approaches, e.g., glucocorticoid topical therapy, have shown limited efficacy with systemic adverse reactions. Therefore, novel therapeutic agents and physicochemical formulations are in constant need and should be obtained and tested in terms of effectiveness and minimization of side effects. For that reason, the aim of our study was to design and obtain various hybrid systems, nanoemulgel-macroemulsion and nanoemulgel-oleogel (bigel), as vehicles for ursolic acid (UA) and to verify their potential as topical formulations used in psoriasis treatment. Obtained topical formulations were characterized by conducting morphological, rheological, texture, and stability analysis. To determine the safety and effectiveness of the prepared ursolic acid carriers, in vitro studies on human keratinocyte cell-like HaCaT cells were performed with cytotoxicity analysis for individual components and each formulation. Moreover, a kinetic study of ursolic acid release from the obtained systems was conducted. All of the studied UA-loaded systems were well tolerated by keratinocyte cells and had suitable pH values and stability over time. The obtained formulations exhibit an apparent viscosity, ensuring the appropriate time of contact with the skin, ease of spreading, soft consistency, and adherence to the skin, which was confirmed by texture tests. The release of ursolic acid from each of the formulations is followed by a slow, controlled release according to the Korsmeyer-Peppas and Higuchi models. The elaborated systems could be considered suitable vehicles to deliver triterpene to psoriatic skin.
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