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Comparison of a rational vs. high throughput approach for rapid salt screening and selection

机译:用于快速盐分筛选和选择的合理与高通量方法的比较

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In recent years, high throughput (HT) screening has become the most widely used approach for early phase salt screening and selection in a drug discovery/development setting. The purpose of this study was to compare a rational approach for salt screening and selection to those results previously generated using a HT approach. The rational approach involved a much smaller number of initial trials (one salt synthesis attempt per counterion) that were selected based on a few strategic solubility determinations of the free form combined with a theoretical analysis of the ideal solvent solubility conditions for salt formation. Salt screening results for sertraline, tamoxifen, and trazodone using the rational approach were compared to those previously generated by HT screening. The rational approach produced similar results to HT screening, including identification of the commercially chosen salt forms, but with a fraction of the crystallization attempts. Moreover, the rational approach provided enough solid from the very initial crystallization of a salt for more thorough and reliable solid-state characterization and thus rapid decision-making. The crystallization techniques used in the rational approach mimic larger-scale process crystallization, allowing smoother technical transfer of the selected salt to the process chemist.
机译:近年来,高通量(HT)筛选已成为在药物发现/开发环境中进行早期盐筛选和选择的最广泛使用的方法。这项研究的目的是将盐筛选和选择的合理方法与以前使用HT方法产生的结果进行比较。合理的方法涉及的初始试验数量少得多(每个抗衡离子进行一次盐合成尝试),这些试验是基于对游离形式的一些战略溶解度测定以及成盐的理想溶剂溶解度条件的理论分析而选择的。使用合理的方法对舍曲林,他莫昔芬和曲唑酮的盐筛选结果与以前通过HT筛选产生的结果进行了比较。合理的方法产生了与HT筛选相似的结果,包括鉴定商业选择的盐形式,但有少量的结晶尝试。此外,合理的方法从盐的最初结晶就可以提供足够的固体,以便更彻底,更可靠地进行固态表征,从而快速做出决策。合理方法中使用的结晶技术模仿了大规模的过程结晶,从而使选定的盐更平稳地技术转移至过程化学家。

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