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Indexed by:期刊论文
Date of Publication:2013-05-01
Journal:CURRENT MEDICINAL CHEMISTRY
Included Journals:SCIE、PubMed、Scopus
Volume:20
Issue:15
Page Number:2032-2042
ISSN No.:0929-8673
Key Words:falcipain-2; 3D-QSAR; molecular docking; molecular dynamics
Abstract:Evidence indicates that cysteine protease falcipain-2 plays essential role in malaria parasites; therefore the potent and selective inhibitors of falcipain-2 may be therapeutically useful drugs for treatment of various forms of malaria parasite plasmodium. In order to understand the structure-activity correlation of falcipain-2 inhibitors, a set of ligand- and receptor-based 3D-QSAR models were, for the first time, developed in the present work employing Comparative Molecular Field Analysis (CoMFA) and Comparative Molecular Similarity Index Analysis (CoMSIA) for 240 promising molecules. Based on the ligand- based alignment, an optimal 3D-QSAR model was obtained with good predictive power of Q(2) - 0.501, R-ncv(2) - 0.890, SEE - 0.282, F - 153.522 and R-pred(2) - 0.768. And the contour maps intuitively suggest where to modify the molecular structures in order to improve the binding affinity. In addition, docking analysis and molecular dynamics simulation (MD) study were also carried out on the dataset with purpose of exploring the detailed binding modes of ligand in the falcipain-2 binding pocket. The combination of docking analysis and MD simulation shows that Gly83, Trp43 and Ala175 which formed several H-bonds are crucial for falcipain-2 inhibitors. The analysis of the best QSAR model reveals the structural features related to the activity, and provides an insight into molecular mechanisms of inhibition and possible modification of the molecules for better activity.