Dipartimento di Scienze della Salute, Università degli Studi Magna Grecia di Catanzaro, Campus Salvatore Venuta, 88100, Catanzaro, Italy.
Eur J Med Chem. 2012 Apr;50:216-29. doi: 10.1016/j.ejmech.2012.01.056. Epub 2012 Feb 5.
We report the first application of ligand-based virtual screening (VS) methods for discovering new compounds able to inhibit both human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT)-associated functions, DNA polymerase and ribonuclease H (RNase H) activities. The overall VS campaign consisted of two consecutive screening processes. In the first, the VS platform Rapid Overlay of Chemical Structures (ROCS) was used to perform in silico shape-based similarity screening on the NCI compounds database in which a hydrazone derivative, previously shown to inhibit the HIV-1 RT, was chosen. As a result, 34 hit molecules were selected and assayed on both RT-associated functions. In the second, the 4 most potent RT inhibitors identified were selected as queries for parallel VS performed by combining shape-based, 2D-fingerprint and 3D-pharmacophore VS methods. Overall, a set of molecules characterized by new different scaffolds were identified as novel inhibitors of both HIV-1 RT-associated activities in the low micromolar range.
我们报告了首例应用配体为基础的虚拟筛选(VS)方法来发现能够抑制人类免疫缺陷病毒 1 型(HIV-1)逆转录酶(RT)相关功能、DNA 聚合酶和核糖核酸酶 H(RNase H)活性的新型化合物。整个 VS 活动由两个连续的筛选过程组成。在第一个过程中,VS 平台 Rapid Overlay of Chemical Structures(ROCS)被用于对 NCI 化合物数据库进行基于形状的相似性虚拟筛选,其中选择了一种先前显示能够抑制 HIV-1 RT 的腙衍生物。结果,选择了 34 个命中分子,并在 RT 相关功能上进行了测定。在第二个过程中,选择了 4 种最有效的 RT 抑制剂作为查询,用于通过结合基于形状、2D-指纹和 3D-药效团 VS 方法进行平行 VS。总体而言,一组具有新型不同支架的分子被鉴定为新型低微摩尔范围内抑制 HIV-1 RT 相关活性的抑制剂。
