Equipe Orpailleur, INRIA Nancy - Grand Est, LORIA, 54506 Vandoeuvre-lès-Nancy, France.
Department of Chemistry and Pharmacy and Interdisciplinary Center for Molecular Materials (ICMM), Friedrich-Alexander-Universität Erlangen-Nürnberg, Egerlandstrasse 3, 91058 Erlangen, Germany.
Mol Inform. 2011 Mar 14;30(2-3):151-9. doi: 10.1002/minf.201000149. Epub 2010 Dec 22.
Ligand-based virtual screening (VS) techniques have become well established in the drug discovery process. However, despite their relative success, there still exists the problem of how to define the initial query compounds and which of their conformations should be used. Here, we propose a novel shape plus surface property approach using multiple local spherical harmonic (SH) functions. We also investigate the use of shape-based and shape plus property-based consensus SH queries calculated in several different ways. The utility of these approaches is compared using the 40 pharmaceutically relevant targets of the DUD database. Our results show that using a combination of SH-based properties often gives better VS performance than using simple shape-based queries. Shape-based consensus queries also perform well, but we find that explicit 3D shape-property conformations should be retained for highly flexible ligands.
基于配体的虚拟筛选(VS)技术已经在药物发现过程中得到了很好的应用。然而,尽管它们相对成功,仍然存在如何定义初始查询化合物以及应该使用它们的哪些构象的问题。在这里,我们提出了一种使用多个局部球谐(SH)函数的新的形状加表面特性方法。我们还研究了使用基于形状和基于形状和特性的共识 SH 查询的方法,这些方法以几种不同的方式计算。使用 DUD 数据库的 40 个药物相关靶点比较了这些方法的效用。我们的结果表明,使用基于 SH 的特性的组合通常比使用简单的基于形状的查询具有更好的 VS 性能。基于形状的共识查询也表现良好,但我们发现对于高度灵活的配体,应该保留明确的 3D 形状-特性构象。
