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Journal of Biomolecular Structure and Dynamics Volume 39, 2021 - Issue 10
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Research Articles

Repurposing of chloroquine and some clinically approved antiviral drugs as effective therapeutics to prevent cellular entry and replication of coronavirus

Akinwunmi O. Adeoyea Department of Biochemistry, Federal University Oye-Ekiti, Oye-Ekiti, Nigeria
,
Babatunde Joseph Osob Department of Biochemistry, McPherson University, Seriki Sotayo, NigeriaCorrespondence[email protected]
ORCID Iconhttps://orcid.org/0000-0001-8667-7108
ORCID Icon,
Ige Francis Olaoyeb Department of Biochemistry, McPherson University, Seriki Sotayo, Nigeria
,
Habibu Tijjanic Department of Biochemistry, Natural Product Research Laboratory, Bauchi State University, Gadau, Nigeria
&
Ahmed I. Adebayod Department of Biochemistry, University of Ilorin, Ilorin, Nigeria
Pages 3469-3479 | Received 24 Apr 2020, Accepted 01 May 2020, Published online: 15 May 2020
 
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Abstract

The reemergence of coronavirus prompts the need for the development of effective therapeutics to prevent the cellular entry and replication of coronavirus. This study demonstrated the putative inhibitory potential of lopinavir, remdesivir, oseltamir, azithromycin, ribavirin, and chloroquine towards V-ATPase, protein kinase A, SARS-CoV spike glycoprotein/ACE-2 complex and viral proteases. The pharmacodynamic and pharmacokinetic properties were predicted through the pkCSM server while the corresponding binding affinity of the selected drugs towards the proteins was computed using AutodockVina Screening tool. The ADMET properties revealed all the drugs possess drug-like properties. Lopinavir has the highest binding affinities to the pocket site of SARS-CoV spike glycoprotein/ACE-2 complex, cyclic AMP-dependent protein kinase A and 3-Chymotrypsin like protease while redemsivir has the highest binding affinities for vacuolar proton-translocating ATPase (V-ATPase) and papain-like proteins. The amino acids Asp269, Leu370, His374, and His345 were predicted as the key residues for lopinavir binding to human SARS-CoV spike glycoprotein/ACE-2 complex while His378, Tyr515, Leu73, Leu100, Phe32 and Phe40 for remdesivir and Tyr510, Phe504, Met62, Tyr50, and His378 were predicted for azithromycin as the key residues for binding to SARS-CoV spike glycoprotein/ACE-2 complex. Moreover, it was also observed that chloroquine has appreciable binding affinities for 3-Chymotrpsin- like protease and cyclic AMP-dependent protein kinase A when compared to Oseltamivir and ribavirin. The study provided evidence suggesting putative repurposing of the selected drugs for the development of valuable drugs for the prevention of cellular entry and replication of coronavirus.

Communicated by Ramaswamy H. Sarma

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Disclosure statement

No potential conflict of interest was reported by the authors.

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