Molecular docking and molecular dynamics studies of sars-cov-2 inhibitors: Crocin, digitoxigenin, beta-eudesmol and favipiravir: Comparative study

J.R.Mora,S. A. Cuesta,Assia Belhassan,G. S. Moran,Tahar Lakhlifi,Mohammed Bouachrine,P. F. Carlos,G. C. Lorena,L.H. Mendoza-Huizar

Molecular docking and molecular dynamics studies of sars-cov-2 inhibitors: Crocin, digitoxigenin, beta-eudesmol and favipiravir: Comparative study

2022

J.R.Mora
S. A. Cuesta
Assia Belhassan
G. S. Moran
Tahar Lakhlifi
Mohammed Bouachrine
P. F. Carlos
G. C. Lorena
L.H. Mendoza-Huizar

In this study, Crocin, Digitoxigenin, Beta-Eudesmol, and Favipiravir were docked in the active site of SARS-CoV-2 main protease (PDB code: 6LU7). The docking study was followed by Molecular Dynamics simulation. The result indicates that Crocin and Digitoxigenin are the structures with the best affinity in the studied enzyme's binding site. Still, Molecular Dynamics simulation showed that Digitoxigenin is the molecule that fits better in the active site of the main protease. Therefore, this molecule could have a more potent antiviral treatment of COVID-19 than the other three studied compounds. © 2021 by the authors.

Keywords:

Protease
Stereochemistry
Active site
Docking (molecular)
Binding site
Digitoxigenin
Chemistry
Favipiravir
Crocin
Protein Data Bank (RCSB PDB)

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