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Cyclodextrin-induced change in crystal habit of acetylsalicylic acid in aqueous solution

机译:环糊精诱导的乙酰水杨酸水溶液晶体习性变化

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摘要

The present work refers to a method to selectively modify the crystal habit of acetylsalicylic acid (ASA) through the use of the cyclic oligosaccharide derivatives 2-hydroxybutyl-β-cyclodextrin (HB-β-CD) and 2,6-di-O-methyl-β-cyclodextrin (DM-β-CD) as a growth inhibitor. ASA crystallized in plate crystals in solutions containing only drug. On the other hand, the addition of HB-β-CD or DM-β-CD markedly changed the crystal habit of the drug to needle crystals that elongated along the crystallographic b-axis. The habit modification of these CDs was attributable to the suppression of the crystal growth of ASA toward the c-axis direction, which is perpendicular to the {001} surface and consisted of phenyl and methyl groups of ASA. These results suggested that HB- and DM-β-CDs inhibited the access of ASA to the {001} face due to the inclusion complex formation with the drug and/or due to the adsorption of the amphiphilic hosts on this face. These CDs can work as a tailor-made additive and may be useful for control of crystal habits of drugs.
机译:本工作涉及通过使用环状寡糖衍生物2-羟基丁基-β-环糊精(HB-β-CD)和2,6-二-O-来选择性修饰乙酰水杨酸(ASA)晶体习性的方法甲基-β-环糊精(DM-β-CD)作为生长抑制剂。 ASA在仅包含药物的溶液中在平板晶体中结晶。另一方面,添加HB-β-CD或DM-β-CD可以显着改变药物的晶体习性,使其变成沿晶体b轴伸长的针状晶体。这些CD的习性修饰归因于抑制了ASA向c轴方向的晶体生长,该晶体垂直于{001}表面并且由ASA的苯基和甲基组成。这些结果表明,HB-和DM-β-CDs抑制了ASA进入{001}面,这是由于与药物形成了包合物,和/或由于两亲宿主在该面上的吸附。这些CD可以用作量身定制的添加剂,并且对于控制药物的晶体习惯可能有用。

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