Redox regulation of the SARS-CoV-2 main protease provides new opportunities for drug design

  1. Lisa-Marie Funk
  2. Gereon Poschmann
  3. Ashwin Chari
  4. Fabian Rabe von Pappenheim
  5. Kim-Maren Stegmann
  6. Antje Dickmanns
  7. Nora Eulig
  8. Marie Wensien
  9. Elham Paknia
  10. Gabi Heyne
  11. Elke Penka
  12. Arwen R. Pearson
  13. Carsten Berndt
  14. Tobias Fritz
  15. Sophia Bazzi
  16. Jon Uranga
  17. Ricardo A. Mata
  18. Matthias Dobbelstein
  19. Rolf Hilgenfeld
  20. Ute Curth
  21. Kai Tittmann
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Abstract

Besides vaccines, the development of antiviral drugs targeting SARS-CoV-2 is critical for stopping the current COVID-19 pandemic and preventing future outbreaks. The SARS-CoV-2 main protease (Mpro), a cysteine protease with essential functions in viral replication, has been validated as an effective drug target. Here, we show that Mpro is subject to redox regulation and reversibly switches between the enzymatically active dimer and the functionally dormant monomer through redox modifications of cysteine residues. These include sulfenylation, disulfide formation between the catalytic cysteine and a proximal cysteine, and generation of an allosteric lysine-cysteine SONOS bridge that is required for structural stability under oxidative stress conditions, such as those exerted by the innate immune system. We identify homo- and heterobifunctional reagents that mimic the redox switching and possess antiviral activity. The discovered redox switches are conserved in main proteases from other coronaviruses, e.g. MERS and SARS-CoV, indicating their potential as common druggable sites.

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