原料药/聚合物配方中的非晶-非晶相分离

C. Luebbert, F. Huxoll, G. Sadowski
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引用次数: 54

摘要

聚合物中难溶性药物制剂的长期稳定性决定了它们的生物利用度和治疗适用性。然而,这些配方不仅在储存过程中容易结晶,而且还容易发生不必要的非晶-非晶相分离(APS)。尽管在过去的几年里,人们已经测量并模拟了聚合物中原料药的结晶行为,但对APS现象的了解仍然很少。在本研究中,通过热级显微镜和DSC研究了布洛芬和非洛地平在PLGA链上具有不同乳酸和乙醇酸单体比例的聚合物PLGA配体中的结晶行为、APS和玻璃化转变温度配方。在布洛芬/PLGA制剂中观察到APS和再结晶,而在非洛地平/PLGA制剂中仅发生再结晶。基于摄动链统计关联流体理论(PC-SAFT)对结晶行为的成功建模,预测了APS的发生,与实验结果一致。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Amorphous-Amorphous Phase Separation in API/Polymer Formulations
The long-term stability of pharmaceutical formulations of poorly-soluble drugs in polymers determines their bioavailability and therapeutic applicability. However, these formulations do not only often tend to crystallize during storage, but also tend to undergo unwanted amorphous-amorphous phase separations (APS). Whereas the crystallization behavior of APIs in polymers has been measured and modeled during the last years, the APS phenomenon is still poorly understood. In this study, the crystallization behavior, APS, and glass-transition temperatures formulations of ibuprofen and felodipine in polymeric PLGA excipients exhibiting different ratios of lactic acid and glycolic acid monomers in the PLGA chain were investigated by means of hot-stage microscopy and DSC. APS and recrystallization was observed in ibuprofen/PLGA formulations, while only recrystallization occurred in felodipine/PLGA formulations. Based on a successful modeling of the crystallization behavior using the Perturbed-Chain Statistical Associating Fluid Theory (PC-SAFT), the occurrence of APS was predicted in agreement with experimental findings.
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