Unidad de Investigación de Diseño de Fármacos y Conectividad Molecular, Departamento de Química Física, Facultad de Farmacia, Universitat de València, 46100 Burjassot, Spain.
Departamento de Química, Universitat de Girona, 17071 Girona, Spain.
Int J Mol Sci. 2022 Dec 1;23(23):15057. doi: 10.3390/ijms232315057.
A method to identify molecular scaffolds potentially active against the Mycobacterium tuberculosis complex (MTBC) is developed. A set of structurally heterogeneous agents against MTBC was used to obtain a mathematical model based on topological descriptors. This model was statistically validated through a Leave-n-Out test. It successfully discriminated between active or inactive compounds over 86% in database sets. It was also useful to select new potential antituberculosis compounds in external databases. The selection of new substituted pyrimidines, pyrimidones and triazolo[1,5-]pyrimidines was particularly interesting because these structures could provide new scaffolds in this field. The seven selected candidates were synthesized and six of them showed activity in vitro.
开发了一种鉴定可能对抗结核分枝杆菌复合群(MTBC)的分子支架的方法。使用了一组针对 MTBC 的结构异构试剂,以获得基于拓扑描述符的数学模型。该模型通过Leave-n-Out 测试进行了统计学验证。它成功地将数据库集中 86%以上的活性或非活性化合物区分开来。它也可用于在外部数据库中选择新的潜在抗结核化合物。选择新的取代嘧啶、嘧啶酮和三唑并[1,5-a]嘧啶特别有趣,因为这些结构可以为该领域提供新的支架。选择了 7 个候选化合物进行合成,其中 6 个具有体外活性。
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