Structure-Activity Relationship Studies Towards Analogues of Pleconaril as Novel Enterovirus-D68 Capsid-Targeting Antivirals

  1. David L Cousins
  2. Ed J Griffen
  3. Jessica Stacey
  4. Alpha A Lee
  5. Yuliia Filimonova
  6. Anton Hlavin
  7. Yuliia Holota
  8. Roman Khmil
  9. Mykyta Kordubailo
  10. Oleksii Kostinov
  11. Dmytro Lesyk
  12. Ivan Logvinenko
  13. Mariia Lototska
  14. Viacheslav Lysenko
  15. Anna Pashchenko
  16. Mariia Pavlichenko
  17. Anzhela Rodnichenko
  18. Anton Tkachenko
  19. Brett L Hurst
  20. Justin G Julander
  21. Hong Wang
  22. Rebecca Pearl
  23. Jared Benjamin
  24. Randy Diaz-Tapia
  25. Mary E Gordon
  26. Randy A Albrecht
  27. Kris White
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Abstract

Non-polio enteroviruses (NPEV) such as enterovirus D68 (EV-D68) that are highly infectious and associated with polio-like neurological complications have caused outbreaks, globally, in recent years. While some clinical and preclinical compounds have shown efficacy against NPEV in-vitro, liabilities that caused historical compounds such as pleconaril to fall short of FDA approval still remain. We present herein SAR and SPR studies of analogues of clinical compounds such as pleconaril and vapendavir against EV-D68 as a representative NPEV. Numerous structurally differentiated analogues with EV-D68 antiviral activity and useful ADME properties were discovered, which could serve as starting points for future EV drug discovery campaigns. Screening against a panel of enteroviruses revealed moderately broad-spectrum anti-EV activity of compound 26.

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