Optimization Rules for SARS-CoV-2 M(pro) Antivirals: Ensemble Docking and Exploration of the Coronavirus Protease Active Site

Coronaviruses are viral infections that have a significant ability to impact human health. Coronaviruses have produced two pandemics and one epidemic in the last two decades. The current pandemic has created a worldwide catastrophe threatening the lives of over 15 million as of July 2020. Current re...

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Autores principales: Stoddard, Shana V., Stoddard, Serena D., Oelkers, Benjamin K., Fitts, Kennedi, Whalum, Kellen, Whalum, Kaylah, Hemphill, Alexander D., Manikonda, Jithin, Martinez, Linda Michelle, Riley, Elizabeth G., Roof, Caroline M., Sarwar, Nowreen, Thomas, Doni M., Ulmer, Emily, Wallace, Felissa E., Pandey, Pankaj, Roy, Sudeshna
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7552026/
https://www.ncbi.nlm.nih.gov/pubmed/32859008
http://dx.doi.org/10.3390/v12090942
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author Stoddard, Shana V.
Stoddard, Serena D.
Oelkers, Benjamin K.
Fitts, Kennedi
Whalum, Kellen
Whalum, Kaylah
Hemphill, Alexander D.
Manikonda, Jithin
Martinez, Linda Michelle
Riley, Elizabeth G.
Roof, Caroline M.
Sarwar, Nowreen
Thomas, Doni M.
Ulmer, Emily
Wallace, Felissa E.
Pandey, Pankaj
Roy, Sudeshna
author_facet Stoddard, Shana V.
Stoddard, Serena D.
Oelkers, Benjamin K.
Fitts, Kennedi
Whalum, Kellen
Whalum, Kaylah
Hemphill, Alexander D.
Manikonda, Jithin
Martinez, Linda Michelle
Riley, Elizabeth G.
Roof, Caroline M.
Sarwar, Nowreen
Thomas, Doni M.
Ulmer, Emily
Wallace, Felissa E.
Pandey, Pankaj
Roy, Sudeshna
author_sort Stoddard, Shana V.
collection PubMed
description Coronaviruses are viral infections that have a significant ability to impact human health. Coronaviruses have produced two pandemics and one epidemic in the last two decades. The current pandemic has created a worldwide catastrophe threatening the lives of over 15 million as of July 2020. Current research efforts have been focused on producing a vaccine or repurposing current drug compounds to develop a therapeutic. There is, however, a need to study the active site preferences of relevant targets, such as the SARS-CoV-2 main protease (SARS-CoV-2 M(pro)), to determine ways to optimize these drug compounds. The ensemble docking and characterization work described in this article demonstrates the multifaceted features of the SARS-CoV-2 M(pro) active site, molecular guidelines to improving binding affinity, and ultimately the optimization of drug candidates. A total of 220 compounds were docked into both the 5R7Z and 6LU7 SARS-CoV-2 M(pro) crystal structures. Several key preferences for strong binding to the four subsites (S1, S1′, S2, and S4) were identified, such as accessing hydrogen binding hotspots, hydrophobic patches, and utilization of primarily aliphatic instead of aromatic substituents. After optimization efforts using the design guidelines developed from the molecular docking studies, the average docking score of the parent compounds was improved by 6.59 −log(10)(Kd) in binding affinity which represents an increase of greater than six orders of magnitude. Using the optimization guidelines, the SARS-CoV-2 M(pro) inhibitor cinanserin was optimized resulting in an increase in binding affinity of 4.59 −log(10)(Kd) and increased protease inhibitor bioactivity. The results of molecular dynamic (MD) simulation of cinanserin-optimized compounds CM02, CM06, and CM07 revealed that CM02 and CM06 fit well into the active site of SARS-CoV-2 M(pro) [Protein Data Bank (PDB) accession number 6LU7] and formed strong and stable interactions with the key residues, Ser-144, His-163, and Glu-166. The enhanced binding affinity produced demonstrates the utility of the design guidelines described. The work described herein will assist scientists in developing potent COVID-19 antivirals.
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spelling pubmed-75520262020-10-14 Optimization Rules for SARS-CoV-2 M(pro) Antivirals: Ensemble Docking and Exploration of the Coronavirus Protease Active Site Stoddard, Shana V. Stoddard, Serena D. Oelkers, Benjamin K. Fitts, Kennedi Whalum, Kellen Whalum, Kaylah Hemphill, Alexander D. Manikonda, Jithin Martinez, Linda Michelle Riley, Elizabeth G. Roof, Caroline M. Sarwar, Nowreen Thomas, Doni M. Ulmer, Emily Wallace, Felissa E. Pandey, Pankaj Roy, Sudeshna Viruses Article Coronaviruses are viral infections that have a significant ability to impact human health. Coronaviruses have produced two pandemics and one epidemic in the last two decades. The current pandemic has created a worldwide catastrophe threatening the lives of over 15 million as of July 2020. Current research efforts have been focused on producing a vaccine or repurposing current drug compounds to develop a therapeutic. There is, however, a need to study the active site preferences of relevant targets, such as the SARS-CoV-2 main protease (SARS-CoV-2 M(pro)), to determine ways to optimize these drug compounds. The ensemble docking and characterization work described in this article demonstrates the multifaceted features of the SARS-CoV-2 M(pro) active site, molecular guidelines to improving binding affinity, and ultimately the optimization of drug candidates. A total of 220 compounds were docked into both the 5R7Z and 6LU7 SARS-CoV-2 M(pro) crystal structures. Several key preferences for strong binding to the four subsites (S1, S1′, S2, and S4) were identified, such as accessing hydrogen binding hotspots, hydrophobic patches, and utilization of primarily aliphatic instead of aromatic substituents. After optimization efforts using the design guidelines developed from the molecular docking studies, the average docking score of the parent compounds was improved by 6.59 −log(10)(Kd) in binding affinity which represents an increase of greater than six orders of magnitude. Using the optimization guidelines, the SARS-CoV-2 M(pro) inhibitor cinanserin was optimized resulting in an increase in binding affinity of 4.59 −log(10)(Kd) and increased protease inhibitor bioactivity. The results of molecular dynamic (MD) simulation of cinanserin-optimized compounds CM02, CM06, and CM07 revealed that CM02 and CM06 fit well into the active site of SARS-CoV-2 M(pro) [Protein Data Bank (PDB) accession number 6LU7] and formed strong and stable interactions with the key residues, Ser-144, His-163, and Glu-166. The enhanced binding affinity produced demonstrates the utility of the design guidelines described. The work described herein will assist scientists in developing potent COVID-19 antivirals. MDPI 2020-08-26 /pmc/articles/PMC7552026/ /pubmed/32859008 http://dx.doi.org/10.3390/v12090942 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Stoddard, Shana V.
Stoddard, Serena D.
Oelkers, Benjamin K.
Fitts, Kennedi
Whalum, Kellen
Whalum, Kaylah
Hemphill, Alexander D.
Manikonda, Jithin
Martinez, Linda Michelle
Riley, Elizabeth G.
Roof, Caroline M.
Sarwar, Nowreen
Thomas, Doni M.
Ulmer, Emily
Wallace, Felissa E.
Pandey, Pankaj
Roy, Sudeshna
Optimization Rules for SARS-CoV-2 M(pro) Antivirals: Ensemble Docking and Exploration of the Coronavirus Protease Active Site
title Optimization Rules for SARS-CoV-2 M(pro) Antivirals: Ensemble Docking and Exploration of the Coronavirus Protease Active Site
title_full Optimization Rules for SARS-CoV-2 M(pro) Antivirals: Ensemble Docking and Exploration of the Coronavirus Protease Active Site
title_fullStr Optimization Rules for SARS-CoV-2 M(pro) Antivirals: Ensemble Docking and Exploration of the Coronavirus Protease Active Site
title_full_unstemmed Optimization Rules for SARS-CoV-2 M(pro) Antivirals: Ensemble Docking and Exploration of the Coronavirus Protease Active Site
title_short Optimization Rules for SARS-CoV-2 M(pro) Antivirals: Ensemble Docking and Exploration of the Coronavirus Protease Active Site
title_sort optimization rules for sars-cov-2 m(pro) antivirals: ensemble docking and exploration of the coronavirus protease active site
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7552026/
https://www.ncbi.nlm.nih.gov/pubmed/32859008
http://dx.doi.org/10.3390/v12090942
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