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Harnessing free energy calculations for kinome-wide selectivity in drug discovery campaigns with a Wee1 case study

Author

Listed:
  • Jennifer Lynn Knight

    (Inc.)

  • Anthony J. Clark

    (Inc.)

  • Jiashi Wang

    (Inc.)

  • Andrew Placzek

    (Inc.)

  • Pieter H. Bos

    (Inc.)

  • Sathesh Bhat

    (Inc.)

  • Jeffrey A. Bell

    (Inc.)

  • Sarah Silvergleid

    (Inc.)

  • Wu Yin

    (Inc.)

  • Felicia Gray

    (Inc.)

  • Shaoxian Sun

    (Inc.)

  • Karen Akinsanya

    (Inc.)

  • Robert Abel

    (Inc.)

  • Aleksey I. Gerasyuto

    (Inc.)

Abstract

Optimizing both on-target and off-target potencies is essential for developing effective and selective small-molecule therapeutics. Free energy calculations offer rapid potency predictions, usually within hours and with experimental accuracy and thus enables efficient identification of promising compounds for synthesis, accelerating early-stage drug discovery campaigns. While free energy predictions are routinely applied to individual proteins, here, we present a free energy framework for efficiently achieving kinome-wide selectivity that led to the discovery of selective Wee1 kinase inhibitors. Ligand-based relative binding free energy calculations rapidly identified multiple novel potent chemical scaffolds. Subsequent protein residue mutation free energy calculations that modified the Wee1 gatekeeper residue, significantly reduced their off-target liabilities across the kinome. Thus, with judicious use of this gatekeeper residue selectivity handle, applying this computational strategy streamlined the optimization of both on-target and off-target potencies, offering a roadmap to expedite drug discovery timelines by decreasing unanticipated off-target toxicities.

Suggested Citation

  • Jennifer Lynn Knight & Anthony J. Clark & Jiashi Wang & Andrew Placzek & Pieter H. Bos & Sathesh Bhat & Jeffrey A. Bell & Sarah Silvergleid & Wu Yin & Felicia Gray & Shaoxian Sun & Karen Akinsanya & R, 2025. "Harnessing free energy calculations for kinome-wide selectivity in drug discovery campaigns with a Wee1 case study," Nature Communications, Nature, vol. 16(1), pages 1-16, December.
  • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-62722-w
    DOI: 10.1038/s41467-025-62722-w
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