Screening of commercial cyclic peptide conjugated to HIV-1 Tat peptide as inhibitor of N-terminal heptad repeat glycoprotein-2 ectodomain Ebola virus through in silico analysis
[Display omitted] •About 614 ligands were computationally modified from 313 commercial cyclic peptides and an HIV-1 Tat peptide.•The ligands were tested against EBOV NHR GP2 ectodomain through molecular docking simulation, resulting 26 ligands which have lower free binding energy compared to the sta...
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Veröffentlicht in: | Journal of molecular graphics & modelling 2017-06, Vol.74, p.366-378 |
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Sprache: | eng |
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•About 614 ligands were computationally modified from 313 commercial cyclic peptides and an HIV-1 Tat peptide.•The ligands were tested against EBOV NHR GP2 ectodomain through molecular docking simulation, resulting 26 ligands which have lower free binding energy compared to the standards.•Computational pharmacological properties prediction was employed to determine the ADMET properties of the selected ligands.•Ligand 023 RMSD calculation from molecular dynamics simulation shows a promising stability to maintain its molecular interaction with the EBOV NHR GP2 ectodomain.
Ebola Hemorrhagic Fever (EHF) is a disease caused by viruses from genus Ebolavirus. Zaire ebolavirus (EBOV) is the deadliest species which has 76% case fatality rate. Up until now, there is no U.S. Food and Drug Administration (FDA) approved drugs to treat EHF. Antiviral drug based on EBOV N-terminal heptad repeat glycoprotein-2 (NHR GP2) Ectodomain inhibitor is one kind of treatment that has not well developed. NHR GP2 Ectodomain has an important role in the process of EBOV entry into the cell through endocytosis mechanism. In this study, we used in silico methods to investigate the activity of commercial cyclic peptide conjugated to Human Immunodeficiency Virus type 1 Trans-activator of the transcription (HIV-1 Tat) peptide as ligands which act as an inhibitor of EBOV NHR GP2 Ectodomain. The commercial cyclic peptides which we used in this study were obtained from the selected chemical companies. Conjugation of the commercial cyclic peptides to HIV-1 Tat peptide was done in order to accumulate it inside the endosome. The ligands which had the best inhibition properties were screened using molecular docking and molecular dynamics simulation. Prediction of pharmacological properties of the peptides was done to choose the best drug candidate. The result of screening processes shows that Ligand 023 has the highest potency as the drug lead. The ligand needs to undergo further analysis through in vitro, in vivo, and a clinical trial to ensure that this ligand has a therapeutic ability as an antiviral drug for Ebola virus infection. |
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ISSN: | 1093-3263 1873-4243 |
DOI: | 10.1016/j.jmgm.2017.04.001 |