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Susceptibility analysis of mutations that confer resistance to inhibitors of the main protease (Mpro) and RNA-dependent RNA polymerase (RdRp) of the SARS-CoV-2 virus

Authors

  • Daysi Espín-Sánchez Instituto de Investigaciones Bioquímicas de La Plata “Profesor Doctor Rodolfo R. Brenner”
  • Carolina Vizuete-Rubio Facultad de Ciencia e Ingeniería en Alimentos y Biotecnología, Universidad Técnica de Ambato
  • karen Jaramillo-Guapisaca Facultad de Ciencia e Ingeniería en Alimentos y Biotecnología, Universidad Técnica de Ambato
  • María Ramos-Aristimbay Facultad de Ciencia e Ingeniería en Alimentos y Biotecnología, Universidad Técnica de Ambato
  • Andrés Sánchez-Vaca Facultad de Ciencia e Ingeniería en Alimentos y Biotecnología, Universidad Técnica de Ambato
  • Fernanda Chico-Terán Facultad de Ciencia e Ingeniería en Alimentos y Biotecnología (FCIAB), Universidad Técnica de ; Universidad Central del Ecuador (Facultad de Ciencias Biológicas)
  • Liliana Cerda-Mejía Facultad de Ciencia e Ingeniería en Alimentos y Biotecnología, Universidad Técnica de Ambato
  • Mario García

DOI:

https://doi.org/10.31243/aci.v29i2.1845

Keywords:

SARS-CoV-2, Mpro, RdRp, homology, mutations, docking.

Abstract

Enormous efforts have been made worldwide to generate therapeutic options to prevent the transmissibility of the SARS-CoV-2 and reduce its replication in humans. Currently, the emergence of new variants of the virus is of great concern because the evolution of the viral genome and the inherent mutations introduced in the viral proteins could decrease the effectiveness of the first line therapeutic agents used to prevent and treat COVID-19. The present study evaluated the susceptibility of two important pharmacological drug targets of SARS-CoV-2, the major protease (Mpro) and the RNA-dependent RNA polymerase (RdRp), to suffer point mutations that could produce resistance to inhibitors of these enzymes. The results showed that the residues that contour the inhibitor binding site in RdRp are extremely conserved between the different RNA virus species. This suggests the RdRp enzyme has a low probability to suffer mutation that could confer resistance to therapeutic drugs, such as remdesivir, an FDA approved compound to treat COVID-19. In contrast, we observed that the Mpro enzyme could undergo up to ten-point mutations in the active site, which is the binding site of several experimental drugs under development, such as Carmofur and N3. Molecular docking analysis showed that the presence of single point mutations in the Mpro active site produces an increase in the binding affinity of carmofur, probably due to the small size and high flexibility of this molecule. However, the Pro168Ser and Ala191Val mutations significantly decrease the affinity of N3 binding to Mpro, suggesting the possible emergence of resistance to this drug. These results could help to anticipate the effect of different mutations on the way Mpro inhibitors bind to the enzyme, and design new inhibitors that address the effect of resistance.

References

Gao, Y., Yan, L., Huang, Y., Liu, F., Zhao, Y., Cao, L., . . . Zhang, L. (2020). Structure of the RNA-dependent RNA polymerase from COVID-19 virus. Science, 368(6492), 779-782. doi:10.1126/science.abb7498

García, M. L., de Pascual Teresa, B., & Braña, M. F. (2004). Estudio teórico del modo de unión entre CDK2 y butirolactona I. Paper presented at the Anales de la Real Academia Nacional de Farmacia.

Gervasoni, S., Vistoli, G., Talarico, C., Manelfi, C., Beccari, A. R., Studer, G., . . . Pedretti, A. (2020). A comprehensive mapping of the druggable cavities within the SARS-CoV-2 therapeutically relevant proteins by combining pocket and docking searches as implemented in pockets 2.0. International journal of molecular sciences, 21(14), 5152.

González-Paz, L., Paz, J. L., Vera-Villalobos, J., & Alvarado, Y. J. (2020). Compuestos Fitoquímicos Dirigidos al Bloqueo de la Polimerasa Viral del SARS-CoV-2 causante del COVID-19: un Análisis Comparativo de Funciones de Puntuación para Acoplamientos con Interés Biomédico. Revista Politécnica, 46, 7-20.

Published

2022-12-28

Versions

Issue

Section

Artículos de investigación

How to Cite

Susceptibility analysis of mutations that confer resistance to inhibitors of the main protease (Mpro) and RNA-dependent RNA polymerase (RdRp) of the SARS-CoV-2 virus. (2022). Alimentos Ciencia E Ingeniería, 29(2), 102-119. https://doi.org/10.31243/aci.v29i2.1845

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