合成子
磺胺
化学
酰胺
超分子化学
共晶
氢键
组合化学
分子
甲酰胺
晶体工程
立体化学
有机化学
作者
Geetha Bolla,Ashwini Nangia
出处
期刊:IUCrJ
[International Union of Crystallography]
日期:2019-06-21
卷期号:6 (4): 751-760
被引量:12
标识
DOI:10.1107/s2052252519005037
摘要
Sulfonamide drugs are well known antibacterial and antimicrobial molecules for pharmaceutical development. Building a library of suitable supramolecular synthons for the sulfonamide functional group and understanding their crystal structures with partner coformer molecules continues to be a challenge in crystal engineering. Although a few sulfonamide cocrystals with amides and N -oxides have been reported, the body of work on sulfonamide synthons is limited compared with those that have carboxylic acids and carboxamides. To address this structural gap, the present work is primarily focused on sulfonamide–lactam and sulfonamide– syn -amide synthons with drugs such as celecoxib, hydrochlorothiazide and furosemide. Furthermore, the electrostatic potential of previously reported cocrystals has been recalculated to show that the negative electrostatic potential on the lactam and syn -amide O atom is higher compared with the charge on carboxamide and pyridine N -oxide O atoms. The potential of sulfonamide molecules to form cocrystals with syn -amides and lactams are evaluated in terms of the electrostatic potential energy for the designed supramolecular synthons.
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