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首页> 外文期刊>Crystal growth & design >Formation of Piroxicam Polymorphism in Solution Crystallization: Effect and Interplay of Operation Parameters
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Formation of Piroxicam Polymorphism in Solution Crystallization: Effect and Interplay of Operation Parameters

机译:溶液结晶中吡罗昔康多晶型的形成:操作参数的影响和相互作用

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摘要

Recently, new insights into crystallization prior to actual nucleation have shown interesting results for drugs showing differences in hydrogen bonding or orientation in various polymorphic forms. On the basis of this concept, piroxicam was chosen as a model compound because the two common forms, I and II, show hydrogen bonding between different parts of the molecules and differences in the orientation of molecules in the crystal lattice. The goal of this work is to explore how various methods of controlling polymorphism during production could be employed. The mechanisms behind the nucleation were also explored, and new insights into polymorphic control are documented and discussed. The crystal landscape was mapped for cooling crystallization of piroxicam from acetone/water mixtures (0.5 K/min) and for antisolvent crystallization from acetone with water as the antisolvent. Varying cooling rates and the use of seeding were used to determine if the system was controlled by a single nucleation event or if the initial form was not the determining factor for the produced form. Finally, the use of soluble additives have previously been found to impact the polymorphic form and was thus employed to impact the nucleation rate as well as the formation of the solid forms in batch cooling crystallization.
机译:最近,对实际成核之前结晶的新见解显示出有趣的结果,这些药物显示出氢键或取向以各种多晶型形式的差异。基于该概念,选择吡罗昔康作为模型化合物,因为两种常见的形式I和II在分子的不同部分之间表现出氢键键合,并且在晶格中分子的取向也不同。这项工作的目的是探索如何在生产过程中采用各种控制多态性的方法。还探讨了成核的机制,并记录和讨论了对多态控制的新见解。绘制了晶体图谱,用于从丙酮/水混合物(0.5 K / min)中冷却吡罗昔康的结晶,并以水作为反溶剂从丙酮中进行反溶剂结晶。使用不同的冷却速率和播种方式来确定系统是否由单个成核事件控制,或者初始形式是否不是生产形式的决定因素。最后,先前已经发现使用可溶性添加剂会影响多晶型物,因此已被用来影响成核速率以及分批冷却结晶中固体形式的形成。

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