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Chemical substructures that enrich for biological activity

机译:丰富生物活性的化学亚结构

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MOTIVATION: Certain chemical substructures are present in many drugs. This has led to the claim of 'privileged' substructures which are predisposed to bioactivity. Because bias in screening library construction could explain this phenomenon, the existence of privilege has been controversial. RESULTS: Using diverse phenotypic assays, we defined bioactivity for multiple compound libraries. Many substructures were associated with bioactivity even after accounting for substructure prevalence in the library, thus validating the privileged substructure concept. Determinations of privilege were confirmed in independent assays and libraries. Our analysis also revealed 'underprivileged' substructures and 'conditional privilege'-rules relating combinations of substructure to bioactivity. Most previously reported substructures have been flat aromatic ring systems. Although we validated such substructures, we also identified three-dimensional privileged substructures. Most privileged substructures display a wide variety of substituents suggesting an entropic mechanism of privilege. Compounds containing privileged substructures had a doubled rate of bioactivity, suggesting practical consequences for pharmaceutical discovery.
机译:动机:许多药物中都存在某些化学亚结构。这导致了倾向于具有生物活性的“特权”子结构的主张。由于筛选库建设方面的偏见可以解释这种现象,因此特权的存在一直引起争议。结果:使用不同的表型分析,我们定义了多种化合物库的生物活性。即使考虑了库中的子结构流行度,许多子结构也与生物活性相关联,从而验证了特权子结构的概念。特权的确定在独立的分析和库中得到确认。我们的分析还揭示了“弱势”子结构和“条件特权”规则,这些规则将子结构与生物活性组合在一起。先前报道的大多数子结构都是扁平的芳香环系统。尽管我们验证了此类子结构,但我们也确定了三维特权子结构。大多数特权子结构显示了各种各样的取代基,表明熵的特权机制。含有特权亚结构的化合物具有两倍的生物活性,这提示了药物发现的实际后果。

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