Department of Bioscience and Biotechnology, Sejong University, 98 Kunja-Dong, Kwangjin-Ku, Seoul 143-747, Republic of Korea.
Bioorg Med Chem. 2009 Nov 15;17(22):7769-74. doi: 10.1016/j.bmc.2009.09.034. Epub 2009 Sep 20.
The inhibitors of factor-inhibiting HIF-1 (FIH1) have been shown to be useful as therapeutics for the treatment of anemia. We have been able to identify eight novel FIH1 inhibitors with IC(50) values ranging from 30 to 80microM by means of the virtual screening with docking simulations under consideration of the effects of ligand solvation in the scoring function. The newly identified inhibitors are structurally diverse and have various chelating groups for the active-site ferrous ion including sulfonamide, carboxylate, N-benzo[1,2,5]oxadiazol-4-yl amide, and 2-[1,2,4]triazolo[3,4-b]][1,3,4]thiadiazol-3-yl-quinoline moieties. Each of these four structural classes has not been reported as FIH1 inhibitor, and therefore can be considered for further development by structure-activity relationship or denovo design methods. The interactions with the amino acid residues responsible for the stabilizations of the inhibitors in the active site are addressed in detail.
已证实,抑制因子抑制 HIF-1(FIH1)的抑制剂可有效用作治疗贫血的药物。我们已经能够通过对接模拟的虚拟筛选,在评分函数中考虑配体溶剂化的影响,鉴定出 8 种新型 FIH1 抑制剂,其 IC(50)值范围为 30 至 80μM。新鉴定的抑制剂结构多样,并且具有用于活性部位亚铁离子的各种螯合基团,包括磺酰胺、羧酸盐、N-苯并[1,2,5]恶二唑-4-基酰胺和 2-[1,2,4]三唑[3,4-b]][1,3,4]噻二唑-3-基-喹啉部分。这四个结构类别中的每一个都没有被报道为 FIH1 抑制剂,因此可以考虑通过构效关系或从头设计方法进一步开发。详细讨论了与负责抑制剂在活性部位稳定的氨基酸残基的相互作用。
