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Rational approach toward COVID-19 main protease inhibitors via molecular docking, molecular dynamics simulation and free energy calculation

Seketoulie Keretsu, Swapnil P. Bhujbal, Seung Joo Cho

2020Scientific Reports156 citationsDOIOpen Access PDF

Abstract

Abstract In the rapidly evolving coronavirus disease (COVID-19) pandemic, repurposing existing drugs and evaluating commercially available inhibitors against druggable targets of the virus could be an effective strategy to accelerate the drug discovery process. The 3C-Like proteinase (3CL pro ) of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has been identified as an important drug target due to its role in viral replication. The lack of a potent 3CL pro inhibitor and the availability of the X-ray crystal structure of 3CL pro (PDB-ID 6LU7) motivated us to perform computational studies to identify commercially available potential inhibitors. A combination of modeling studies was performed to identify potential 3CL pro inhibitors from the protease inhibitor database MEROPS ( https://www.ebi.ac.uk/merops/index.shtml ). Binding energy evaluation identified key residues for inhibitor design. We found 15 potential 3CL pro inhibitors with higher binding affinity than that of an α-ketoamide inhibitor determined via X-ray structure. Among them, saquinavir and three other investigational drugs aclarubicin, TMC-310911, and faldaprevir could be suggested as potential 3CL pro inhibitors. We recommend further experimental investigation of these compounds.

Topics & Concepts

Docking (animal)ProteaseDrug repositioningProtein Data Bank (RCSB PDB)Protease inhibitor (pharmacology)CoronavirusDrug discoverySaquinavirDruggabilityChemistryComputational biologyPharmacologyVirologyBiologyCoronavirus disease 2019 (COVID-19)DrugBiochemistryEnzymeMedicineInfectious disease (medical specialty)VirusDiseaseViral loadAntiretroviral therapyNursingGenePathologyComputational Drug Discovery MethodsSARS-CoV-2 and COVID-19 ResearchEnzyme function and inhibition
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