@article{Fonseca_Cavalcante_Carvalho_Amaral_Colares_Marinho_Neto_2020, title={STUDY OF THE INHIBITION POTENTIAL OF REMDESIVIR DERIVATIVES ON MPRO OF SARS-COV-2}, volume={8}, url={https://www.granthaalayahpublication.org/journals/granthaalayah/article/view/IJRG20_B11_3887}, DOI={10.29121/granthaalayah.v8.i11.2020.2342}, abstractNote={<p>The emergence of the new coronavirus (SARS-COV-2) is known to trigger some common diseases in humans such as pneumonia and diarrhea, the search for appropriate therapy combat COVID-19 has been intense and exhaustive.</p> <p><strong>Motivation/Background:</strong> Thus, based on the rational study of drugs, a survey of potential ligands that can inhibit the vital protein in virus replication, the main protease (Mpro), has been carried out worldwide.</p> <p><strong>Method: </strong>In this battle, the antiviral Remdesivir, which was created to fight the Ebola virus, proved, through the molecular anchorage, to be quite effective against its target because it presented affinity energy far superior to its co-crystallized ligand.</p> <p><strong>Results: </strong>In this work, a study was carried out with Remdesivir and its derivatives, obtained in a zinc database15, to present a possible alternative, based on its structure-affinity, as potential Inhibitors of SARS-COV-2 MPro, with affinity energy ranging from -6.3 to -8.2 kcal/mol.</p> <p><strong>Conclusions:</strong> It was found that both remdesivir and its diastereoisomeric derivatives have an affinity with the main protease (Mpro), responsible for viral replication, with inhibition capacity and possible alternative in its treatment.</p>}, number={11}, journal={International Journal of Research -GRANTHAALAYAH}, author={Fonseca, Aluísio Marques da and Cavalcante, Antonio Luthierre Gama and Carvalho, Rubson Mateus Matos and Amaral, Jeferson Falcão do and Colares, Regilany Paulo and Marinho, Emmanuel Silva and Neto, Moises Maia}, year={2020}, month={Dec.}, pages={164–174} }