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Covalent narlaprevir- and boceprevir-derived hybrid inhibitors of SARS-CoV-2 main protease

Author

Listed:
  • Daniel W. Kneller

    (Oak Ridge National Laboratory)

  • Hui Li

    (Oak Ridge National Laboratory)

  • Gwyndalyn Phillips

    (Oak Ridge National Laboratory)

  • Kevin L. Weiss

    (Oak Ridge National Laboratory)

  • Qiu Zhang

    (Oak Ridge National Laboratory)

  • Mark A. Arnould

    (Oak Ridge National Laboratory)

  • Colleen B. Jonsson

    (University of Tennessee Health Science Center
    University of Tennessee Health Science Center
    The University of Tennessee Health Science Center)

  • Surekha Surendranathan

    (The University of Tennessee Health Science Center)

  • Jyothi Parvathareddy

    (The University of Tennessee Health Science Center)

  • Matthew P. Blakeley

    (Institut Laue–Langevin)

  • Leighton Coates

    (Oak Ridge National Laboratory)

  • John M. Louis

    (National Institutes of Health, DHHS)

  • Peter V. Bonnesen

    (Oak Ridge National Laboratory)

  • Andrey Kovalevsky

    (Oak Ridge National Laboratory)

Abstract

Emerging SARS-CoV-2 variants continue to threaten the effectiveness of COVID-19 vaccines, and small-molecule antivirals can provide an important therapeutic treatment option. The viral main protease (Mpro) is critical for virus replication and thus is considered an attractive drug target. We performed the design and characterization of three covalent hybrid inhibitors BBH-1, BBH-2 and NBH-2 created by splicing components of hepatitis C protease inhibitors boceprevir and narlaprevir, and known SARS-CoV-1 protease inhibitors. A joint X-ray/neutron structure of the Mpro/BBH-1 complex demonstrates that a Cys145 thiolate reaction with the inhibitor’s keto-warhead creates a negatively charged oxyanion. Protonation states of the ionizable residues in the Mpro active site adapt to the inhibitor, which appears to be an intrinsic property of Mpro. Structural comparisons of the hybrid inhibitors with PF-07321332 reveal unconventional F···O interactions of PF-07321332 with Mpro which may explain its more favorable enthalpy of binding. BBH-1, BBH-2 and NBH-2 exhibit comparable antiviral properties in vitro relative to PF-07321332, making them good candidates for further design of improved antivirals.

Suggested Citation

  • Daniel W. Kneller & Hui Li & Gwyndalyn Phillips & Kevin L. Weiss & Qiu Zhang & Mark A. Arnould & Colleen B. Jonsson & Surekha Surendranathan & Jyothi Parvathareddy & Matthew P. Blakeley & Leighton Coa, 2022. "Covalent narlaprevir- and boceprevir-derived hybrid inhibitors of SARS-CoV-2 main protease," Nature Communications, Nature, vol. 13(1), pages 1-11, December.
  • Handle: RePEc:nat:natcom:v:13:y:2022:i:1:d:10.1038_s41467-022-29915-z
    DOI: 10.1038/s41467-022-29915-z
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    1. Xiangrui Jiang & Haixia Su & Weijuan Shang & Feng Zhou & Yan Zhang & Wenfeng Zhao & Qiumeng Zhang & Hang Xie & Lei Jiang & Tianqing Nie & Feipu Yang & Muya Xiong & Xiaoxing Huang & Minjun Li & Ping Ch, 2023. "Structure-based development and preclinical evaluation of the SARS-CoV-2 3C-like protease inhibitor simnotrelvir," Nature Communications, Nature, vol. 14(1), pages 1-15, December.

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