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Small-molecule inhibition of SARS-CoV-2 NSP14 RNA cap methyltransferase

Author

Listed:
  • Cindy Meyer

    (The Rockefeller University)

  • Aitor Garzia

    (The Rockefeller University)

  • Michael W. Miller

    (The Rockefeller University)

  • David J. Huggins

    (The Rockefeller University
    Weill Cornell Medical College)

  • Robert W. Myers

    (The Rockefeller University)

  • Hans-Heinrich Hoffmann

    (The Rockefeller University)

  • Alison W. Ashbrook

    (The Rockefeller University)

  • Syeda Y. Jannath

    (The Rockefeller University)

  • Nigel Liverton

    (The Rockefeller University)

  • Stacia Kargman

    (The Rockefeller University)

  • Matthew Zimmerman

    (Hackensack Meridian Health)

  • Andrew M. Nelson

    (Hackensack Meridian Health)

  • Vijeta Sharma

    (Hackensack Meridian Health)

  • Enriko Dolgov

    (Hackensack Meridian Health)

  • Julianna Cangialosi

    (Hackensack Meridian Health)

  • Suyapa Penalva-Lopez

    (Hackensack Meridian Health)

  • Nadine Alvarez

    (Hackensack Meridian Health)

  • Ching-Wen Chang

    (The Rockefeller University
    Hackensack Meridian Health
    Columbia University)

  • Neelam Oswal

    (Hackensack Meridian Health)

  • Irene Gonzalez

    (Hackensack Meridian Health)

  • Risha Rasheed

    (Hackensack Meridian Health)

  • Kira Goldgirsh

    (Hackensack Meridian Health)

  • Jada A. Davis

    (The Rockefeller University)

  • Lavoisier Ramos-Espiritu

    (The Rockefeller University)

  • Miriam-Rose Menezes

    (The Rockefeller University)

  • Chloe Larson

    (The Rockefeller University)

  • Julius Nitsche

    (PROTEROS Biostructures GmbH)

  • Oleg Ganichkin

    (PROTEROS Biostructures GmbH)

  • Hanan Alwaseem

    (The Rockefeller University)

  • Henrik Molina

    (The Rockefeller University)

  • Stefan Steinbacher

    (PROTEROS Biostructures GmbH)

  • J. Fraser Glickman

    (The Rockefeller University)

  • David S. Perlin

    (Hackensack Meridian Health)

  • Charles M. Rice

    (The Rockefeller University)

  • Peter T. Meinke

    (The Rockefeller University)

  • Thomas Tuschl

    (The Rockefeller University)

Abstract

Coronavirus disease 2019 (COVID-19) is caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2)1. The rapid development of highly effective vaccines2,3 against SARS-CoV-2 has altered the trajectory of the pandemic, and antiviral therapeutics4 have further reduced the number of COVID-19 hospitalizations and deaths. Coronaviruses are enveloped, positive-sense, single-stranded RNA viruses that encode various structural and non-structural proteins, including those critical for viral RNA replication and evasion from innate immunity5. Here we report the discovery and development of a first-in-class non-covalent small-molecule inhibitor of the viral guanine-N7 methyltransferase (MTase) NSP14. High-throughput screening identified RU-0415529, which inhibited SARS-CoV-2 NSP14 by forming a unique ternary S-adenosylhomocysteine (SAH)-bound complex. Hit-to-lead optimization of RU-0415529 resulted in TDI-015051 with a dissociation constant (Kd) of 61 pM and a half-maximal effective concentration (EC50) of 11 nM, inhibiting virus infection in a cell-based system. TDI-015051 also inhibited viral replication in primary small airway epithelial cells and in a transgenic mouse model of SARS CoV-2 infection with an efficacy comparable with the FDA-approved reversible covalent protease inhibitor nirmatrelvir6. The inhibition of viral cap methylases as an antiviral strategy is also adaptable to other pandemic viruses.

Suggested Citation

  • Cindy Meyer & Aitor Garzia & Michael W. Miller & David J. Huggins & Robert W. Myers & Hans-Heinrich Hoffmann & Alison W. Ashbrook & Syeda Y. Jannath & Nigel Liverton & Stacia Kargman & Matthew Zimmerm, 2025. "Small-molecule inhibition of SARS-CoV-2 NSP14 RNA cap methyltransferase," Nature, Nature, vol. 637(8048), pages 1178-1185, January.
  • Handle: RePEc:nat:nature:v:637:y:2025:i:8048:d:10.1038_s41586-024-08320-0
    DOI: 10.1038/s41586-024-08320-0
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