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首页> 外文期刊>Crystal growth & design >Multidrug Cocrystal of Anticonvulsants: Influence of Strong Intermolecular Interactions on Physiochemical Properties
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Multidrug Cocrystal of Anticonvulsants: Influence of Strong Intermolecular Interactions on Physiochemical Properties

机译:抗惊厥药的多药COCRYSTAL:强分子间相互作用对生理化学性质的影响

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src="http://pubs.acs.org/appl/literatum/publisher/achs/journals/content/cgdefu/2017/cgdefu.2017.17.issue-10/acs.cgd.7b00741/20170928/images/medium/cg-2017-00741a_0008.gif">A drug–drug cocrystal of two anticonvulsants, lamotrigine and phenobarbital, is presented. In the crystal structure, molecules form heterodimers via N–H···O and N–H···N hydrogen bonding. The intrinsic dissolution rate (IDR) and solubility of the cocrystal were measured in phosphate buffer (pH 7.2) and simulated gastric fluid (without pepsin), and compared to pure APIs. Dissolution experiments found suppressed IDR of the cocrystal with rates in the order pure PB > pure LTG > cocrystal. The solubility measurements were consistent with the dissolution behavior. The presence of strong heterodimers in the cocrystal compared to weaker homodimers in the parent drugs is implicated for the reduced solubility and dissolution rate.
机译:src =“http://pubs.acs.org/appl/literatum/publisher/achs/journals/content/cgdefu/2017/cgdefu.2017.17.issue-10/acs.cgd.7b00741/20170928/images/medium 介绍了两种抗惊厥药,乳草嗪和苯甲虫的药物 - 药物酰基吡咯。 在晶体结构中,分子通过N-H····o和N-H···n氢键形成异二聚体。 在磷酸盐缓冲液(pH7.2)和模拟胃液(没有胃蛋白)中测量COCRYSTAL的内在溶解速率(IDR)和溶解度,并与纯API相比。 溶出实验发现抑制纯Pb>纯LTG> Cocrystal rates的Cocrystal的IdR。 溶解度测量与溶解行为一致。 与母体药物中的较弱的同杂体相比,与母体药物中的较弱的偶发剂相比存在强的异二聚体的存在,用于降低溶解度和溶解速率。

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  • 来源
    《Crystal growth & design 》 |2017年第10期| 共5页
  • 作者单位

    Department of Chemistry Department of Pharmaceutical Sciences and Macromolecular Science and Engineering University of Michigan Ann Arbor Michigan 48109 United States;

    Department of Chemistry Department of Pharmaceutical Sciences and Macromolecular Science and Engineering University of Michigan Ann Arbor Michigan 48109 United States;

    Department of Chemistry Department of Pharmaceutical Sciences and Macromolecular Science and Engineering University of Michigan Ann Arbor Michigan 48109 United States;

    Department of Chemistry Department of Pharmaceutical Sciences and Macromolecular Science and Engineering University of Michigan Ann Arbor Michigan 48109 United States;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 晶体学 ;
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