1. 3-oxoacyl-ACP reductase from Schistosoma japonicum: integrated in silico-in vitro strategy for discovering antischistosomal lead compounds.
- Author
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Liu J, Dyer D, Wang J, Wang S, Du X, Xu B, Zhang H, Wang X, and Hu W
- Subjects
- 3-Oxoacyl-(Acyl-Carrier-Protein) Reductase antagonists & inhibitors, 3-Oxoacyl-(Acyl-Carrier-Protein) Reductase genetics, Animals, Cell Death drug effects, Cloning, Molecular, Drug Evaluation, Preclinical, Enzyme Inhibitors pharmacology, Genes, Helminth genetics, Helminth Proteins antagonists & inhibitors, Helminth Proteins genetics, Helminth Proteins isolation & purification, Hep G2 Cells, Humans, Kinetics, Schistosoma japonicum cytology, Schistosoma japonicum drug effects, Schistosoma japonicum ultrastructure, Structure-Activity Relationship, Survival Analysis, Time Factors, 3-Oxoacyl-(Acyl-Carrier-Protein) Reductase isolation & purification, Anthelmintics pharmacology, Computer Simulation, Drug Discovery, Schistosoma japonicum enzymology
- Abstract
Background: Schistosomiasis is a disease caused by parasitic worms and more than 200 million people are infected worldwide. The emergence of resistance to the most commonly used drug, praziquantel (PZQ), makes the development of novel drugs an urgent task. 3-oxoacyl-ACP reductase (OAR), a key enzyme involved in the fatty acid synthesis pathway, has been identified as a potential drug target against many pathogenic organisms. However, no research on Schistosoma japonicum OAR (SjOAR) has been reported. The characterization of the SjOAR protein will provide new strategies for screening antischistosomal drugs that target SjOAR., Methodology/principal Findings: After cloning the SjOAR gene, recombinant SjOAR protein was purified and assayed for enzymatic activity. The tertiary structure of SjOAR was obtained by homology modeling and 27 inhibitor candidates were identified from 14,400 compounds through molecular docking based on the structure. All of these compounds were confirmed to be able to bind to the SjOAR protein by BIAcore analysis. Two compounds exhibited strong antischistosomal activity and inhibitory effects on the enzymatic activity of SjOAR. In contrast, these two compounds showed relatively low toxicity towards host cells., Conclusions/significance: The work presented here shows the feasibility of isolation of new antischistosomal compounds using a combination of virtual screening and experimental validation. Based on this strategy, we successfully identified 2 compounds that target SjOAR with strong antischistosomal activity but relatively low cytotoxicity to host cells.
- Published
- 2013
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