Computational hunting of natural active compounds as an alternative for Remdesivir to target RNA-dependent polymerase

Mohd Saeed; Amir Saeed; Md Jahoor Alam; Mousa Alreshidi

doi:10.14715/cmb/2021.67.1.7

Issue

Vol. 67 No. 1: Issue 1

Issue Published : March 8, 2021

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Computational hunting of natural active compounds as an alternative for Remdesivir to target RNA-dependent polymerase

https://doi.org/10.14715/cmb/2021.67.1.7

Mohd Saeed

Department of Biology, college of Sciences, University of Ha'il, Hail, Saudi Arabia

Amir Saeed

Deapertment of Clinical Lbaoratory Sciences, College of Sciences, University of Ha'il, Hail, Saudi Arabia

Md Jahoor Alam

Department of Biology, college of Sciences, University of Ha'il, Hail, Saudi Arabia

Mousa Alreshidi

Department of Biology, college of Sciences, University of Ha'il, Hail, Saudi Arabia

Corresponding Author(s) : Mohd Saeed

mo.saeed@uoh.edu.sa

Cellular and Molecular Biology, Vol. 67 No. 1: Issue 1
Article Published : January 31, 2021

Abstract

The hunt for potential lead/drug molecules from different resources, especially from natural resources, for possible treatment of COVID-19 is ongoing. Several compounds have already been identified, but only a few are good enough to show potential against the virus. Among the identified druggable target proteins of SARS-CoV-2, this study focuses on non-structural RNA-dependent RNA polymerase protein (RdRp), a well-known enzyme for both viral genome replication and viral mRNA synthesis, and is therefore considered to be the primary target. In this study, the virtual screening followed by an in-depth docking study of the Compounds Library found that natural compound Cyclocurcumin and Silybin B have strong interaction with RdRp and much better than the remdesivir with free binding energy and inhibition constant value as êžŒ-6.29 kcal/mol and 58.39 µMêžŒ, and êžŒ-7.93kcal/mol and 45.3 µMêžŒ, respectively. The finding indicated that the selected hits (Cyclocurcumin and Silybin B) could act as non-nucleotide anti-polymerase agents, and can be further optimized as a potential inhibitor of RdRp by benchwork experiments.

Keywords

Virtual screening Remdesivir COVID-19 Cyclocurcumin.

Saeed, M., Saeed, A., Alam, M. J., & Alreshidi, M. (2021). Computational hunting of natural active compounds as an alternative for Remdesivir to target RNA-dependent polymerase. Cellular and Molecular Biology, 67(1), 45–49. https://doi.org/10.14715/cmb/2021.67.1.7