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Presentation of a structurally diverse and commercially available drug data set for correlation and benchmarking studies

机译:呈现结构多样且可商购的药物数据集,以进行相关性和基准研究

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A multivariate analysis of drugs on the Swedish market was the basis for the selection of a small, physicochemically diverse set of 24 drug compounds. Factors such as structural diversity, commercial availability, price, and a suitable analytical technique for quantification were considered in the selection. Lipophilicity, pK(a), solubility, and permeability across human Caco-2 cell monolayers were measured for the compiled data set. The results show that, by use of a physicochemically diverse data set, experimental responses over a wide range were obtained. The paper also shows how experimental difficulties due to the diversity of the data set can be overcome. We anticipate that this data set can serve as a benchmark set for validation of new experimental techniques or in silico models. It can also be used as a diverse starting data set for the development of new computational models.
机译:在瑞典市场上对药物进行多变量分析是选择少量,理化不同的24种药物化合物的基础。选择时要考虑诸如结构多样性,商业可用性,价格以及合适的定量分析技术等因素。测量汇编数据集的亲脂性,pK(a),溶解度和跨人Caco-2细胞单层的通透性。结果表明,通过使用理化多样化的数据集,可以获得广泛的实验响应。本文还显示了如何克服由于数据集的多样性而带来的实验困难。我们希望该数据集可以用作验证新实验技术或计算机模型的基准集。它也可以用作开发新计算模型的各种初始数据集。

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