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High-Throughput Surveys of Crystal Form Diversity of Highly Polymorphic Pharmaceutical Compounds

机译:高度多态性药物化合物的晶型多样性的高通量调查

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摘要

Surveys of crystal form diversity of two test compounds. 1 (an experimental angiotensin II antagonist) and 2 (sertraline HCl, the active drug in Zoloft), have been performed with high-throughput (HT) crystallization. Compound 1 was found to have at least 18 crystal forms based on a HT recrystallization experiment using diverse solvents, compared with nine forms originally reported from a traditional screening effort. The efficiency of screening in HT mode is estimated to be about 2 orders of magnitude greater than traditional bench-scale approaches. The multiple patented forms of 2 have been summarized and evaluated based on published information, which is found to include several transient species and at least one mixture of known phases. A comparison between results of HT experiments and data on the disclosed forms shows that the HT effort generates the viable crystal forms; highly unstable hydrates and one metastable polymorph IV were not observed. In attempting to recover form IV, a novel acetic acid solvate was discovered and characterized by single crystal X-ray diffraction. Additionally, a previously undisclosed ethyl acetate hemisolvate of 2 was identified as an intermediate en route to form T1. The study demonstrates that highly polymorphic pharmaceutical compounds can be surveyed by HT form experimentation, and that an HT strategy coupled with critical analysis of reported form diversity can be used to rank the utility of crystal forms.
机译:两种测试化合物的晶型多样性调查。 1(实验性血管紧张素II拮抗剂)和2(盐酸舍曲林盐酸盐,Zoloft中的活性药物)已通过高通量(HT)结晶进行。根据使用多种溶剂进行的HT重结晶实验,发现化合物1具有至少18种晶形,而传统筛选工作最初报道的是9种晶形。估计HT模式下的筛选效率比传统的台式规模方法高约2个数量级。基于已公开的信息,对2的多种专利形式进行了总结和评估,发现这些信息包括几种过渡物种和至少一种已知相的混合物。 HT实验的结果与所公开形式的数据之间的比较表明,HT的努力产生了可行的晶型。没有观察到高度不稳定的水合物和一种亚稳的多晶型物IV。在尝试回收IV型时,发现了一种新的乙酸溶剂化物,并通过单晶X射线衍射对其进行了表征。另外,先前未公开的乙酸乙酯半溶剂化物2被鉴定为形成T1的中间体。该研究表明,可以通过HT形式实验来调查高度多态性的药物化合物,并且HT策略与已报道的形式多样性的关键分析相结合可以用来对晶型的效用进行排名。

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