Synthesis of Metforminium Succinate by Melting. Crystal Structure, Thermal, Spectroscopic and Dissolution Properties

Eduardo Plata-Vargas, C. Cruz-Hernandez, A. Dorazco‐González, I. Fuentes-Noriega, D. Morales‐Morales, J. M. Germán-Acacio
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引用次数: 7

Abstract

The reaction by melt mixing at 220 °C of the antihyperglycemic drug metformin hydrochloride 1 with dehydrated sodium succinate yields efficiently the organic salt [MET] 2 [SUC] 2 (H-MET + = metforminium and SUC 2- = succinate). Solid state CPMAS NMR 13 C spectroscopy experiments, powder X-ray diffraction and FT-IR results support the formation of the pharmaceutical salt 2 in good yields. Besides, the charged-assisted hydrogen bonding interactions of type N-H …- O(carboxylate) were thoroughly analyzed by single crystal X-Ray diffraction techniques. Thus, the pharmaceutical salt 2 possesses considerable thermal differences when compared to the pure starting reagents. In addition, intrinsic dissolution rate experiments in buffered aqueous solutions at pH= 6.8 showed a sustained-release behavior of the drug in 2 with a constant value of K int = 0.885 mg/min * cm 2 .
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熔融法制备琥珀酸二甲双胍。晶体结构,热,光谱和溶解性质
降糖药盐酸二甲双胍1与脱水琥珀酸钠在220℃下熔融混合,有效地生成了有机盐[MET] 2 [SUC] 2 (H-MET + =二甲双胍,SUC - =琥珀酸盐)。固体CPMAS核磁共振13c光谱实验、粉末x射线衍射和傅里叶变换红外(FT-IR)结果表明,制备的药物盐2收率较高。此外,利用单晶x射线衍射技术对N-H - O型(羧酸盐)的带电辅助氢键相互作用进行了深入分析。因此,与纯起始试剂相比,药用盐2具有相当大的热差异。此外,在pH= 6.8的缓冲水溶液中,固有溶出率实验表明,在K = 0.885 mg/min * cm 2的恒定值下,药物在2中具有缓释行为。
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