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卡马西平共晶体与市售产品的性能比较。

Performance comparison of a co-crystal of carbamazepine with marketed product.

作者信息

Hickey Magali B, Peterson Matthew L, Scoppettuolo Lisa A, Morrisette Sherry L, Vetter Anna, Guzmán Hector, Remenar Julius F, Zhang Zhong, Tawa Mark D, Haley Sean, Zaworotko Michael J, Almarsson Orn

机构信息

TransForm Pharmaceuticals, Inc., Lexington, MA 02421, USA.

出版信息

Eur J Pharm Biopharm. 2007 Aug;67(1):112-9. doi: 10.1016/j.ejpb.2006.12.016. Epub 2006 Dec 28.

Abstract

The carbamazepine: saccharin co-crystal (1) was studied in terms of a series of attributes, including suitability for multi-gram scale-up, propensity for crystal polymorphism, physical stability, in vitro dissolution and oral bioavailability, with the goal of comparing 1 with the marketed form of carbamazepine (Tegretol). Preparation of 1 was achieved on a 30g scale with a conventional cooling crystallization process from alcohol solution without seeding. The compound is not overtly polymorphic. This finding is in contrast to the form diversity of pure carbamazepine, which has four known polymorphs and a host of solvates, including a dihydrate, which is the stable form in the presence of water. Physical and chemical stability of the co-crystal is also shown to be quantitatively similar to the pure drug in the marketed product (Tegretol). Finally, comparison of oral bioavailability of 1 with Tegretol tablets in dogs shows the co-crystal to be a viable alternative to the anhydrous polymorph in formulated solid oral products. The balance of properties and performance of 1 as a model co-crystal is discussed.

摘要

对卡马西平 - 糖精共晶体(1)进行了一系列属性研究,包括适合多克规模放大、晶体多晶型倾向、物理稳定性、体外溶出度和口服生物利用度,目的是将其与市售形式的卡马西平( Tegretol )进行比较。通过常规冷却结晶过程,在不接种晶种的情况下从醇溶液中以30克规模制备了1。该化合物没有明显的多晶型现象。这一发现与纯卡马西平的形式多样性形成对比,纯卡马西平有四种已知的多晶型物和许多溶剂化物,包括二水合物,它是在有水存在时的稳定形式。共晶体的物理和化学稳定性在定量上也显示与市售产品(Tegretol)中的纯药物相似。最后,在犬类中对1与Tegretol片剂的口服生物利用度进行比较,结果表明共晶体在固体口服制剂中是无水多晶型物的可行替代物。讨论了1作为模型共晶体的性质和性能平衡。

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