Stimuli-Responsive in situ Spray Gel of Miconazole Nitrate for Vaginal Candidiasis

硝酸咪康唑 泊洛沙姆 差示扫描量热法 咪康唑 泊洛沙姆407 原位 聚合物 壳聚糖 材料科学 色谱法 黏膜黏附 化学工程 化学 抗真菌 复合材料 有机化学 共聚物 微生物学 生物粘附 工程类 物理 热力学 生物
作者
Yong Kai Hsin,Thaneswary Thangarajoo,Hira Choudhury,Manisha Pandey,Wei‐Meng Lim,Bapi Gorain
出处
期刊:Journal of Pharmaceutical Sciences [Elsevier BV]
卷期号:112 (2): 562-572 被引量:22
标识
DOI:10.1016/j.xphs.2022.09.002
摘要

Vaginal candidiasis is a common form of infection in women caused by Candida species. Due to several drawbacks of conventional treatments, the current research is attempted to formulate and optimize a miconazole nitrate-loaded in situ spray gel for vaginal candidiasis. The stimuli-responsive (pH and thermo-responsive) polymers selected for the in situ gel were chitosan and poloxamer 407, respectively, whereas hydroxypropyl methylcellulose (HPMC) was introduced in the formulation to further improve the mucoadhesive property. The dispersion of each polymer was carried out using the cold method, whereas the optimization of the formulation was achieved using Box-Behnken statistical design considering viscosity and gelation temperature as dependent variables. Present design achieved the optimized outcome with HPMC, poloxamer and chitosan at 0.52% (w/v), 18.68% (w/v) and 0.41% (w/v), respectively. Evaluation of drug-excipients compatibility was performed using differential scanning calorimetry, Fourier transform infrared spectroscopy, and thermogravimetric analysis where the results showed the absence of any chemical interaction between the polymers and drug component. The optimized formulation showed gelation temperature at 31°C allowing in situ phase transition in a vaginal environment; pH of 4.21 is suitable for use in the vaginal cavity, and appropriate viscosity (290 cP) at storage temperature (below 30°C) would allow spraying at ease, whereas strong mucoadhesive force (22.4±0.513 g) would prevent leaking of the formulation after application. The drug release profile showed sustained release up to 24 h with a cumulative drug release of 81.72%, which is significantly better than the marketed miconazole nitrate cream. In addition, an improved antifungal activity could be correlated to the sustained release of the drug from the formulation. Finally, the safety of the formulation was established while tested on HaCaT cell lines. Based on our findings, it could be concluded that the in situ hydrogel formulation using stimuli-responsive polymers could be a viable alternative to the conventional dosage form that can help to reduce the frequency of administration with ease of application to the site of infection, thus will provide better patient compliance.
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