Biophysical Analysis of Potential Inhibitors of SARS-CoV-2 Cell Recognition and Their Effect on Viral Dynamics in Different Cell Types: A Computational Prediction from In Vitro Experimental Data

González-Paz, Lenin; Lossada, Carla; Hurtado-León, María Laura; Vera-Villalobos, Joan; L. Paz, José; Marrero Ponce, Yovani; Martínez Ríos, Félix Orlando; Alvarado, Ysaías. J.

doi:10.1021/acsomega.3c06968

Biophysical Analysis of Potential Inhibitors of SARS-CoV-2 Cell Recognition and Their Effect on Viral Dynamics in Different Cell Types: A Computational Prediction from In Vitro Experimental Data

Journal

ACS Omega

ISSN

2470-1343

Publisher

American Chemical Society

Date Issued

2024

Author(s)

González-Paz, Lenin

Lossada, Carla

Hurtado-León, María Laura

Vera-Villalobos, Joan

L. Paz, José

Marrero Ponce, Yovani

Facultad de Ingeniería - CampCM

Martínez Ríos, Félix Orlando

Facultad de Ingeniería - CampCM

Alvarado, Ysaías. J.

Type

text::journal::journal article

DOI

10.1021/acsomega.3c06968

URL

https://scripta.up.edu.mx/handle/20.500.12552/10151

Abstract

Recent reports have suggested that the susceptibility of cells to SARS-CoV-2 infection can be influenced by various proteins that potentially act as receptors for the virus. To investigate this further, we conducted simulations of viral dynamics using different cellular systems (Vero E6, HeLa, HEK293, and CaLu3) in the presence and absence of drugs (anthelmintic, ARBs, anticoagulant, serine protease inhibitor, antimalarials, and NSAID) that have been shown to impact cellular recognition by the spike protein based on experimental data. Our simulations revealed that the susceptibility of the simulated cell systems to SARS-CoV-2 infection was similar across all tested systems. Notably, CaLu3 cells exhibited the highest susceptibility to SARS-CoV-2 infection, potentially due to the presence of receptors other than ACE2, which may account for a significant portion of the observed susceptibility. Throughout the study, all tested compounds showed thermodynamically favorable and stable binding to the spike protein. Among the tested compounds, the anticoagulant nafamostat demonstrated the most favorable characteristics in terms of thermodynamics, kinetics, theoretical antiviral activity, and potential safety (toxicity) in relation to SARS-CoV-2 spike protein-mediated infections in the tested cell lines. This study provides mathematical and bioinformatic models that can aid in the identification of optimal cell lines for compound evaluation and detection, particularly in studies focused on repurposed drugs and their mechanisms of action. It is important to note that these observations should be experimentally validated, and this research is expected to inspire future quantitative experiments. ©American Chemical Society

How to cite

González-Paz, L., Lossada, C., Hurtado-León, M. L., Vera-Villalobos, J., Paz, J. L., Marrero-Ponce, Y., Martinez-Rios, F., & Alvarado, Ysaías. J. (2024). Biophysical Analysis of Potential Inhibitors of SARS-CoV-2 Cell Recognition and Their Effect on Viral Dynamics in Different Cell Types: A Computational Prediction from In Vitro Experimental Data. In ACS Omega (Vol. 9, Issue 8, pp. 8923–8939). American Chemical Society (ACS). https://doi.org/10.1021/acsomega.3c06968