Homology modeling and virtual screening approaches to identify potent inhibitors of VEB-1 β-lactamase

被引:109
|
作者
Messaoudi, Abdelmonaem [1 ]
Belguith, Hatem [1 ]
Ben Hamida, Jeannette [1 ]
机构
[1] Univ Tunis El Manar, Inst Super Sci Biol Appl Tunis, Unite Prote Fonct & Biopreservat Alimentaire, Tunis 1006, Tunisia
关键词
VEB-1; beta-lactamase; Homology modeling; Virtual screening; Docking; Inhibitor; MEDIATED QUINOLONE RESISTANCE; PSEUDOMONAS-AERUGINOSA; ESCHERICHIA-COLI; SWISS-MODEL; MOLECULAR DOCKING; SEQUENCE-ANALYSIS; CLAVULANIC ACID; SPECTRUM; INTEGRON; GENE;
D O I
10.1186/1742-4682-10-22
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
Background: bla(VEB-1) is an integron-located extended-spectrum beta-lactamase gene initially detected in Escherichia coli and Pseudomonas aeruginosa strains from southeast Asia. Several recent studies have reported that VEB-1-positive strains are highly resistant to ceftazidime, cefotaxime and aztreonam antibiotics. One strategy to overcome resistance involves administering antibiotics together with beta-lactamase inhibitors during the treatment of infectious diseases. During this study, four VEB-1 beta-lactamase inhibitors were identified using computer-aided drug design. Methods: The SWISS-MODEL tool was utilized to generate three dimensional structures of VEB-1 beta-lactamase, and the 3D model VEB-1 was verified using PROCHECK, ERRAT and VERIFY 3D programs. Virtual screening was performed by docking inhibitors obtained from the ZINC Database to the active site of the VEB-1 protein using AutoDock Vina software. Results and conclusion: Homology modeling studies were performed to obtain a three-dimensional structure of VEB-1 beta-lactamase. The generated model was validated, and virtual screening of a large chemical ligand library with docking simulations was performed using AutoDock software with the ZINC database. On the basis of the dock-score, four molecules were subjected to ADME/TOX analysis, with ZINC4085364 emerging as the most potent inhibitor of the VEB-1 beta-lactamase.
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页数:10
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