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Do Zebrafish Obey Lipinski Rules?

机译:斑马鱼服从Lipinski规则吗?

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The use of zebrafish in whole organism phenotypic assays has become a valuable strategy throughout the drug discovery process. Zebrafish assays can be used not only to screen libraries of compounds at the earliest stages but also to evaluate advanced leads for their effects on specific biological pathways or for toxicity. However, when confronted with inactivity of a compound in a zebrafish assay, there are little data that can be used to judge if the compound is truly biologically inert or inactive due to a lack of permeability into the model organism. While medicinal chemistry principles suggest parameters that are predictive of human oral bioavailability, cellular permeability, and even bacterial permeability, there have been no such parameters developed for zebrafish absorption. To address this question, we compiled a set of 700 compounds reported in the literature to be active in zebrafish assays, evaluated their properties, and compared them to properties derived from a set of historical drugs and a set of recently approved oral drugs. While some properties overlap, the averages and 10th and 90th percentiles of molecular weight, octanol water partition coefficient (logP), H-bond counts, and polar surface area for zebrafish-active compounds are statistically different from those of known drugs. This analysis should be useful to scientists interpreting structure activity relationships based on data from zebrafish assays and help to inform the translation from fish to mammals.
机译:在整个生物体表型测定中使用斑马鱼已成为在药物发现过程中的宝贵策略。斑马鱼测定不仅可以在最早的阶段筛选化合物文库,而且还可以评估其对特定生物途径或毒性的效果的先进引线。然而,当在斑马鱼测定中遇到化合物的不活动时,几乎没有数据可以用于判断该化合物是否真正生物学上的惰性或因子是由于模型生物体缺乏渗透性而无活性。虽然药用化学原理表明了预测人口腔生物利用度,细胞渗透性甚至细菌渗透性的参数,但没有为斑马鱼吸收而开发的这些参数。为了解决这个问题,我们编制了一套700个在文献中报告的化合物,以在斑马鱼测定中活跃,评估它们的性质,并将其与来自一组历史药物的性质进行比较,以及一套最近批准的口服药物。虽然一些性质重叠,但斑马鱼活性化合物的分子量,辛醇水分配系数(LOMP),H键计数和极性表面积的分子量和第90百分位数与已知药物的分子量有统计学不同。这种分析应该对科学家基于来自斑马鱼测定的数据来解释结构活动关系,并有助于向哺乳动物向哺乳动物通知翻译。

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