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Int J Pharm. 2024 May 25;657:124189. doi: 10.1016/j.ijpharm.2024.124189. Epub 2024 May 1.
Amorphous solid dispersions (ASDs) represent an important approach for enhancing oral bioavailability for poorly water soluble compounds; however, assuring that these ASDs do not recrystallize to a significant extent during storage can be time-consuming. Therefore, various efforts have been undertaken to predict ASD crystallization levels with kinetic models. However, only limited success has been achieved due to limits on crystal content quantification methods and the complexity of crystallization kinetics. To increase the prediction accuracy, the accelerated stability assessment program (ASAP), employing isoconversion (time to hit a specification limit) and a modified Arrhenius approach, are employed here for predictive shelf-life modeling. In the current study, a model ASD was prepared by spray drying griseofulvin and HPMC-AS-LF. This ASD was stressed under a designed combinations of temperature, relative humidity and time with the conditions set to ensure stressing was carried out below the glass transition temperature (T) of the ASD. Crystal content quantification method by X-ray powder diffraction (XRPD) with sufficient sensitivity was developed and employed for stressed ASD. Crystallization modeling of the griseofulvin ASD using ASAPprime® demonstrated good agreement with long-term (40 °C/75 %RH) crystallinity levels and support the use of this type of accelerated stability studies for further improving ASD shelf-life prediction accuracy.
无定形固体分散体(ASD)是提高低水溶性化合物口服生物利用度的重要方法;然而,确保这些 ASD 在储存过程中不会在很大程度上重新结晶可能需要很长时间。因此,人们已经做出了各种努力,通过动力学模型来预测 ASD 的结晶水平。然而,由于晶体含量定量方法的限制和结晶动力学的复杂性,仅取得了有限的成功。为了提高预测准确性,这里采用等转化率(达到规定限度的时间)和改进的 Arrhenius 方法的加速稳定性评估计划(ASAP),用于预测货架期建模。在当前的研究中,通过喷雾干燥灰黄霉素和 HPMC-AS-LF 制备了模型 ASD。该 ASD 在温度、相对湿度和时间的设计组合下受到压力,条件设置确保在 ASD 的玻璃化转变温度(T)以下进行压力处理。开发了一种具有足够灵敏度的 X 射线粉末衍射(XRPD)晶体含量定量方法,并用于受应力的 ASD。使用 ASAPprime®对灰黄霉素 ASD 进行结晶建模,结果与长期(40°C/75%RH)结晶度水平吻合良好,支持使用这种类型的加速稳定性研究进一步提高 ASD 货架期预测准确性。