Drug Research Program, Division of Pharmaceutical Chemistry and Technology, Faculty of Pharmacy , University of Helsinki , Viikinkaari 5 E , 00014 Helsinki , Finland.
Biomedicum Imaging Unit, Faculty of Medicine , University of Helsinki , Haartmaninkatu 8 , 00014 Helsinki , Finland.
Mol Pharm. 2018 Nov 5;15(11):5361-5373. doi: 10.1021/acs.molpharmaceut.8b00840. Epub 2018 Oct 9.
The tendency for crystallization during storage and administration is the most considerable hurdle for poorly water-soluble drugs formulated in the amorphous form. There is a need to better detect often subtle and complex surface crystallization phenomena and understand their influence on the critical quality attribute of dissolution. In this study, the interplay between surface crystallization of the amorphous form during storage and dissolution testing, and its influence on dissolution behavior, is analyzed for the first time with multimodal nonlinear optical imaging (coherent anti-Stokes Raman scattering (CARS) and sum frequency generation (SFG)). Complementary analyses are provided with scanning electron microscopy, X-ray diffraction and infrared and Raman spectroscopies. Amorphous indomethacin tablets were prepared and subjected to two different storage conditions (30 °C/23% RH and 30 °C/75% RH) for various durations and then dissolution testing using a channel flow-through device. Trace levels of surface crystallinity previously imaged with nonlinear optics after 1 or 2 days of storage did not significantly decrease dissolution and supersaturation compared to the freshly prepared amorphous tablets while more extensive crystallization after longer storage times did. Multimodal nonlinear optical imaging of the tablet surfaces after 15 min of dissolution revealed complex crystallization behavior that was affected by both storage condition and time, with up to four crystalline polymorphs simultaneously observed. In addition to the well-known α- and γ-forms, the less reported metastable ε- and η-forms were also observed, with the ε-form being widely observed in samples that had retained significant surface amorphousness during storage. This form was also prepared in the pure form and further characterized. Overall, this study demonstrates the potential value of nonlinear optical imaging, together with more established solid-state analysis methods, to understand complex surface crystallization behavior and its influence on drug dissolution during the development of amorphous drugs and dosage forms.
在储存和给药期间结晶的趋势是将以无定形形式配制的水溶性差的药物的最大障碍。需要更好地检测通常微妙和复杂的表面结晶现象,并了解它们对关键质量属性(溶出度)的影响。在这项研究中,首次使用多模态非线性光学成像(相干反斯托克斯拉曼散射(CARS)和和频产生(SFG))分析了在储存和溶出试验过程中无定形形式的表面结晶及其对溶出行为的相互作用。用扫描电子显微镜、X 射线衍射和红外及拉曼光谱进行了补充分析。制备了无定形吲哚美辛片剂,并在两种不同的储存条件(30°C/23%RH 和 30°C/75%RH)下储存不同的时间,然后使用通道流动通过装置进行溶出试验。在储存 1 或 2 天后用非线性光学成像检测到的痕量表面结晶度与新鲜制备的无定形片剂相比,对溶出度和过饱和度的影响不大,而在更长的储存时间后则发生了更广泛的结晶。在 15 分钟的溶出后对片剂表面进行多模态非线性光学成像显示了复杂的结晶行为,该行为受到储存条件和时间的影响,同时观察到多达四种晶型。除了众所周知的α-和γ-型外,还观察到报道较少的亚稳定ε-和η-型,ε-型在储存过程中保持显著表面无定形度的样品中广泛存在。还制备了这种形式的纯物质并进行了进一步的表征。总的来说,这项研究表明,非线性光学成像与更成熟的固态分析方法相结合,具有理解复杂表面结晶行为及其对无定形药物和剂型开发过程中药物溶出度的影响的潜力。
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