Melt extrusion vs. spray drying: The effect of processing methods on crystalline content of naproxen-povidone formulations

喷雾干燥 结晶度 无定形固体 萘普生 再结晶(地质) 结晶 材料科学 挤压 玻璃化转变 化学工程 化学 成核 差示扫描量热法 聚合物 有机化学 复合材料 工程类 病理 古生物学 物理 热力学 生物 替代医学 医学
作者
Abbe Haser,Tu Cao,Joe Lubach,Tony Listro,Larry Acquarulo,Feng Zhang
出处
期刊:European Journal of Pharmaceutical Sciences [Elsevier BV]
卷期号:102: 115-125 被引量:31
标识
DOI:10.1016/j.ejps.2017.02.038
摘要

Our hypothesis is that melt extrusion is a more suitable processing method than spray drying to prepare amorphous solid dispersions of drugs with a high crystallization tendency. Naproxen-povidone K25 was used as the model system in this study. Naproxen-povidone K25 solid dispersions at 30% and 60% drug loadings were characterized by modulated DSC, powder X-ray diffraction, FT-IR, and solid-state 13C NMR to identify phase separation and drug recrystallization during processing and storage. At 30% drug loading, hydrogen bond (H-bond) sites of povidone K25 were not saturated and the glass transition (Tg) temperature of the formulation was higher. As a result, both melt-extruded and spray-dried materials were amorphous initially and remained so after storage at 40°C. At 60% drug loading, H-bond sites were saturated, and Tg was low. We were not able to prepare amorphous materials. The initial crystallinity of the formulations was 0.4%±0.2% and 5.6%±0.6%, and increased to 2.7%±0.3% and 21.6%±1.0% for melt-extruded and spray-dried materials, respectively. Spray-dried material was more susceptible to re-crystallization during processing, due to the high diffusivity of naproxen molecules in the formulation matrix and lack of kinetic stabilization from polymer solution. A larger number of crystalline nucleation sites and high surface area made the spray-dried material more susceptible to recrystallization during storage. This study demonstrated the unique advantages of melt extrusion over spray drying for the preparation of amorphous solid dispersions of naproxen at high drug level.
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