Ligand and Structure-Based In Silico Determination of the Most Promising SARS-CoV-2 nsp16-nsp10 2′-o-Methyltransferase Complex Inhibitors among 3009 FDA Approved Drugs

Ligand and Structure-Based In Silico Determination of the Most Promising SARS-CoV-2 nsp16-nsp10 2′-o-Methyltransferase Complex Inhibitors among 3009 FDA Approved Drugs

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As a continuation of our earlier work against SARS-CoV-2, seven FDA-approved drugs were designated as the best SARS-CoV-2 nsp16-nsp10 2′-o-methyltransferase (2′OMTase) inhibitors through 3009 compounds. The in silico inhibitory potential of the examined compounds against SARS-CoV-2 nsp16-nsp10 2′-o-...

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Bibliographic Details
Main Authors: Alesawy, M.S (Author), Alsfouk, B.A (Author), Eissa, I.H (Author), El-Attar, A.-A.M.M (Author), Elkaeed, E.B (Author), Metwaly, A.M (Author), Saleh, A.M (Author)
Format: Article
Language:English
Published: MDPI 2022
Subjects:
FDA approved drugs
MD simulations
MMPBSA
molecular docking
molecular fingerprints
SARS-CoV-2 nsp16-nsp10 2′-o-methyltransferase
structural similarity
Online Access:View Fulltext in Publisher
LEADER 02920nam a2200289Ia 4500
001 10.3390-molecules27072287
008 220425s2022 CNT 000 0 und d
020 |a 14203049 (ISSN) 
245 1 0 |a Ligand and Structure-Based In Silico Determination of the Most Promising SARS-CoV-2 nsp16-nsp10 2′-o-Methyltransferase Complex Inhibitors among 3009 FDA Approved Drugs 
260 0 |b MDPI  |c 2022 
856 |z View Fulltext in Publisher  |u https://doi.org/10.3390/molecules27072287 
520 3 |a As a continuation of our earlier work against SARS-CoV-2, seven FDA-approved drugs were designated as the best SARS-CoV-2 nsp16-nsp10 2′-o-methyltransferase (2′OMTase) inhibitors through 3009 compounds. The in silico inhibitory potential of the examined compounds against SARS-CoV-2 nsp16-nsp10 2′-o-methyltransferase (PDB ID: (6W4H) was conducted through a multi-step screening approach. At the beginning, molecular fingerprints experiment with SAM (S-Adenosylmethionine), the co-crystallized ligand of the targeted enzyme, unveiled the resemblance of 147 drugs. Then, a structural similarity experiment recommended 26 compounds. Therefore, the 26 compounds were docked against 2′OMTase to reveal the potential inhibitory effect of seven promising compounds (Protirelin, (1187), Calcium folinate (1913), Raltegravir (1995), Regadenoson (2176), Ertapenem (2396), Methylergometrine (2532), and Thiamine pyrophosphate hydrochloride (2612)). Out of the docked ligands, Ertapenem (2396) showed an ideal binding mode like that of the co-crystallized ligand (SAM). It occupied all sub-pockets of the active site and bound the crucial amino acids. Accordingly, some MD simulation experiments (RMSD, RMSF, Rg, SASA, and H-bonding) have been conducted for the 2′OMTase—Ertapenem complex over 100 ns. The performed MD experiments verified the correct binding mode of Ertapenem against 2′OMTase exhibiting low energy and optimal dynamics. Finally, MM-PBSA studies indicated that Ertapenem bonded advantageously to the targeted protein with a free energy value of −43 KJ/mol. Furthermore, the binding free energy analysis revealed the essential amino acids of 2′OMTase that served positively to the binding. The achieved results bring hope to find a treatment for COVID-19 via in vitro and in vivo studies for the pointed compounds. © 2022 by the authors. Licensee MDPI, Basel, Switzerland. 
650 0 4 |a FDA approved drugs 
650 0 4 |a MD simulations 
650 0 4 |a MMPBSA 
650 0 4 |a molecular docking 
650 0 4 |a molecular fingerprints 
650 0 4 |a SARS-CoV-2 nsp16-nsp10 2′-o-methyltransferase 
650 0 4 |a structural similarity 
700 1 |a Alesawy, M.S.  |e author 
700 1 |a Alsfouk, B.A.  |e author 
700 1 |a Eissa, I.H.  |e author 
700 1 |a El-Attar, A.-A.M.M.  |e author 
700 1 |a Elkaeed, E.B.  |e author 
700 1 |a Metwaly, A.M.  |e author 
700 1 |a Saleh, A.M.  |e author 
773 |t Molecules 

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