Preparation and characteristics of monostearin nanostructured lipid carriers

化学 毒品携带者 纳米技术 材料科学 药物输送 有机化学
作者
Fuqiang Hu,Saiping Jiang,Yong‐Zhong Du,Hong Yuan,Yi-Qing Ye,Su Zeng
出处
期刊:International Journal of Pharmaceutics [Elsevier]
卷期号:314 (1): 83-89 被引量:242
标识
DOI:10.1016/j.ijpharm.2006.01.040
摘要

Nanostuctured lipid carriers (NLC) consisted of solid lipid and liquid lipid are a new type of lipid nanoparticles, which offer the advantage of improved drug loading capacity and release properties. In this study, solvent diffusion method was employed to produce NLC. Monostearin (MS) and caprylic/capric triglycerides (CT) were chosen as the solid lipid and liquid lipid. Clobetasol propionate used as a model drug was incorporated into the NLC. The influences of preparation temperature and CT content on physicochemical properties of the NLC were characterized. As a result, monostearin solid lipid nanoparticles (without CT content, SLN) obtained at higher temperature (70 °C) exhibited slightly higher drug loading capacity than that of 0 °C (P < 0.05). In contrast, the production temperature made little effect on NLC drug loading capacity (P > 0.05). The improved drug loading capacity was observed for NLC and it enhanced with increasing the CT content in NLC. The results were explained by differential scanning calorimetry (DSC) measurement for NLC. The incorporation of CT to NLC led to crystal order disturbance and thus left more space to accommodate drug molecules. NLC displayed a good ability to reduce the drug expulsion in storage compared to SLN. The in vitro release behaviors of NLC were dependent on the production temperature and CT content. NLC obtained at 70 °C exhibited biphasic drug release pattern with burst release at the initial 8 h and prolonged release afterwards, whereas NLC obtained at 0 °C showed basically sustained drug release throughout the release time. The drug release rates were increased with increasing the CT content. These results indicated that the NLC produced by solvent diffusion method could potentially be exploited as a carrier with improved drug loading capacity and controlled drug release.
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