3D-QSAR and Docking Studies of 1,3,4-Thiazolidinone Derivatives Using R-Group Search and Surflex-dock  被引量：19

作　　者：TONG Jian-Bo WANG Yang LEI Shan QIN Shang-Shang 仝建波;王洋;雷珊;秦尚尚(College of Chemistry and Chemical Engineering,Shaanxi University of Science and Technology;Shaanxi Key Laboratory of Chemical Additives for Industry)

机构地区：[1]College of Chemistry and Chemical Engineering,Shaanxi University of Science and Technology [2]Shaanxi Key Laboratory of Chemical Additives for Industry

出　　处：《Chinese Journal of Structural Chemistry》2019年第3期464-475,共12页结构化学（英文）

基　　金：supported by the National Natural Science Foundation of China(21475081,21275094);the Graduate Innovation Fund of Shaanxi University of Science and Technology

摘　　要：In this paper, a three-dimensional quantitative structure-activity relationships(3 D-QSAR) study for 20 HIV-1 reverse transcriptase(RT) inhibitors was established using Topomer Co MFA. The models were built based on different fragment cutting models, with the most effective model of the multiple correlation coefficients of fitting(r^2) to be 0.920, cross-validation(q^2) of 0.575, and external validation(Q_(ext)~2) being 0.701. The results indicated that the model obtained has both favorable estimation stability and good prediction capability. Topomer Search was used to search R-group from ZINC database. As a result, a series of R-groups with relatively high activity contribution was obtained. By No. 6 molecule filtering, 3 R_1 and 15 R_2 groups were selected, and employed to alternately substitute for the R_1 and R_2 of sample 6. Finally, 45 new compounds were designed, and the Topomer CoMFA model was used to predicate the biological activity, so the Topomer Search is effective in screening and can guide the design of new HIV/AIDS drugs. The molecular docking method was also used to study the interactions of these drugs by docking the ligands into HIV-1 RT active site, which revealed the likely bioactive conformations. This study showed that there are extensive interactions between the 1,3,4-thiazolidinone revertase inhibitors and His84, Asp145, Lys33 and Leu83 residues in the active site of HIV-1 RT. These results provide useful insights for the design of potent new inhibitors of RT.

关 键 词：QSAR RT INHIBITORS Topomer COMFA Topomer SEARCH design of new INHIBITORS molecular docking 

分 类 号：TQ[化学工程]