| Literature DB >> 29546582 |
Noorakmar Jusoh1, Hasanuddin Zainal2, Azzmer Azzar Abdul Hamid2, Noraslinda M Bunnori2, Khairul Bariyyah Abd Halim2, Shafida Abd Hamid3.
Abstract
Recent outbreaks of highly pathogenic influenza strains have highlighted the need to develop new anti-influenza drugs. Here, we report an in silico study of carvone derivatives to analyze their binding modes with neuraminidase (NA) active sites. Two proposed carvone analogues, CV(A) and CV(B), with 36 designed ligands were predicted to inhibit NA (PDB ID: 3TI6) using molecular docking. The design is based on structural resemblance with the commercial inhibitor, oseltamivir (OTV), ligand polarity, and amino acid residues in the NA active sites. Docking simulations revealed that ligand A18 has the lowest energy binding (∆Gbind) value of -8.30 kcal mol-1, comparable to OTV with ∆Gbind of -8.72 kcal mol-1. A18 formed seven hydrogen bonds (H-bonds) at residues Arg292, Arg371, Asp151, Trp178, Glu227, and Tyr406, while eight H-bonds were formed by OTV with amino acids Arg118, Arg292, Arg371, Glu119, Asp151, and Arg152. Molecular dynamics (MD) simulation was conducted to compare the stability between ligand A18 and OTV with NA. Our simulation study showed that the A18-NA complex is as stable as the OTV-NA complex during the MD simulation of 50 ns through the analysis of RMSD, RMSF, total energy, hydrogen bonding, and MM/PBSA free energy calculations.Entities:
Keywords: Carvone; Influenza neuraminidase; MM/PBSA; Molecular docking
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Year: 2018 PMID: 29546582 DOI: 10.1007/s00894-018-3619-6
Source DB: PubMed Journal: J Mol Model ISSN: 0948-5023 Impact factor: 1.810