首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >CODES, a novel procedure for ligand-based virtual screening: PDE7 inhibitors as an application example.
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CODES, a novel procedure for ligand-based virtual screening: PDE7 inhibitors as an application example.

机译:CODES,一种基于配体的虚拟筛选的新方法:PDE7抑制剂作为应用实例。

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Phosphodiesterase (PDE) 7 is a high affinity cAMP-specific PDE whose functional role in T-cells has been the subject of some controversy. Recent findings on tissue distribution, however, support the hypothesis that PDE7 could be a good target for the treatment of airway diseases, T-cell related diseases or central nervous system (CNS) disorders. Therefore, the identification of selective inhibitors targeted against PDE7 enzyme has become an attractive area of research. We report here the first use of the descriptors generated by the CODES program for ligand-based virtual screening. This program codifies molecules from a topological point of view and the generated descriptors are related to the chemical nature of the atoms, the atomic bonds and the connectivity with the rest of the molecule. They are also able to distinguish among stereoisomers. By using this approach, 173 compounds were codified, and their similarity with the reference compound was analysed. Based on the analysis, new potential PDE7 inhibitors have been identified, synthesized and biologically evaluated confirming that CODES descriptors are valid for ligand-based virtual screening and provided new lead compounds for further optimization as potent and selective PDE7 inhibitors.
机译:磷酸二酯酶(PDE)7是一种高亲和力的cAMP特异性PDE,其在T细胞中的功能作用一直是一些争议的主题。但是,有关组织分布的最新发现支持以下假设:PDE7可能是治疗气道疾病,T细胞相关疾病或中枢神经系统(CNS)疾病的良好靶标。因此,鉴定针对PDE7酶的选择性抑制剂已成为研究的一个有吸引力的领域。我们在这里报告了首次使用CODES程序生成的描述符进行基于配体的虚拟筛选。该程序从拓扑的角度对分子进行编码,生成的描述符与原子的化学性质,原子键以及与分子其余部分的连通性有关。它们还能够区分立体异构体。通过这种方法,对173种化合物进行了编码,并分析了它们与参考化合物的相似性。在分析的基础上,新的潜在PDE7抑制剂已被鉴定,合成和生物学评估,从而确认CODES描述符对于基于配体的虚拟筛选是有效的,并提供了新的先导化合物作为有效和选择性的PDE7抑制剂,可进一步优化。

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