R&D Center, Equis & Zaroo Co., Ltd, Gyeonggi-do 443-766, Republic of Korea.
Bioorg Med Chem Lett. 2011 Jun 1;21(11):3329-34. doi: 10.1016/j.bmcl.2011.04.010. Epub 2011 Apr 9.
We report the use of pharmacophore-based virtual screening as an efficient tool for the discovery of novel HCV polymerase inhibitors. A three-dimensional pharmacophore model for the HCV-796 binding site, NNI site IV inhibitor, to the enzyme was built by means of the structure-based focusing module in Cerius2 program. Using these models as a query for virtual screening, we produced a successful example of using pharmacophore-based virtual screening to identify novel compounds with HCV replicon assay through inhibition of HCV polymerization. Among the hit compounds, compounds 1 and 2 showed 56% and 48% inhibition of NS5B polymerization activity at 20 μM, respectively. In addition, compound 1 also exhibited replicon activity with EC(50) value of 2.16 μM. Following up the initial hit, we obtained derivatives of compound 1 and evaluated polymerization inhibition activity and HCV replicon assay. These results provide information necessary for the development of more potent NS5B inhibitors.
我们报告了基于药效团的虚拟筛选在发现新型 HCV 聚合酶抑制剂方面的应用。通过 Cerius2 程序中的基于结构的聚焦模块,构建了 HCV-796 结合部位(NNI 位点 IV 抑制剂)与酶的三维药效团模型。使用这些模型作为虚拟筛选的查询,我们通过抑制 HCV 聚合成功地利用基于药效团的虚拟筛选识别出具有 HCV 复制子测定抑制活性的新型化合物。在命中化合物中,化合物 1 和 2 分别在 20 μM 时显示出对 NS5B 聚合活性的 56%和 48%抑制。此外,化合物 1 还表现出 EC(50)值为 2.16 μM 的复制子活性。在对最初的命中化合物进行跟踪后,我们获得了化合物 1 的衍生物,并评估了聚合抑制活性和 HCV 复制子测定。这些结果为开发更有效的 NS5B 抑制剂提供了必要的信息。
