1. Academic Validation
  2. Multiscale Simulations of the Covalent Inhibition of the SARS-CoV-2 Main Protease: Four Compounds and Three Reaction Mechanisms

Multiscale Simulations of the Covalent Inhibition of the SARS-CoV-2 Main Protease: Four Compounds and Three Reaction Mechanisms

  • J Am Chem Soc. 2023 Jun 21;145(24):13204-13214. doi: 10.1021/jacs.3c02229.
Bella L Grigorenko 1 2 Igor V Polyakov 1 2 Maria G Khrenova 1 3 Goran Giudetti 4 Shirin Faraji 5 Anna I Krylov 4 Alexander V Nemukhin 1 2
Affiliations

Affiliations

  • 1 Department of Chemistry, Lomonosov Moscow State University, Moscow 119991, Russia.
  • 2 Emanuel Institute of Biochemical Physics, Russian Academy of Sciences, Moscow 119334, Russia.
  • 3 Bach Institute of Biochemistry, Federal Research Centre "Fundamentals of Biotechnology", Russian Academy of Sciences, Moscow 119071, Russia.
  • 4 Department of Chemistry, University of Southern California, Los Angeles, California 90089-0482, United States.
  • 5 Zernike Institute for Advanced Materials, University of Groningen, Groningen 9747 AG, The Netherlands.
Abstract

We report the results of computational modeling of the reactions of the SARS-CoV-2 main protease (MPro) with four potential covalent inhibitors. Two of them, carmofur and nirmatrelvir, have shown experimentally the ability to inhibit MPro. Two Other compounds, X77A and X77C, were designed computationally in this work. They were derived from the structure of X77, a non-covalent inhibitor forming a tight surface complex with MPro. We modified the X77 structure by introducing warheads capable of reacting with the catalytic cysteine residue in the MPro active site. The reaction mechanisms of the four molecules with MPro were investigated by quantum mechanics/molecular mechanics (QM/MM) simulations. The results show that all four compounds form covalent adducts with the catalytic cysteine Cys 145 of MPro. From the chemical perspective, the reactions of these four molecules with MPro follow three distinct mechanisms. The reactions are initiated by a nucleophilic attack of the thiolate group of the deprotonated cysteine residue from the catalytic dyad Cys145-His41 of MPro. In the case of carmofur and X77A, the covalent binding of the thiolate to the ligand is accompanied by the formation of the fluoro-uracil leaving group. The reaction with X77C follows the nucleophilic aromatic substitution SNAr mechanism. The reaction of MPro with nirmatrelvir (which has a reactive nitrile group) leads to the formation of a covalent thioimidate adduct with the thiolate of the Cys145 residue in the Enzyme active site. Our results contribute to the ongoing search for efficient inhibitors of the SARS-CoV-2 Enzymes.

Figures
Products