Molecules (Sep 2024)

Strategic Fluorination to Achieve a Potent, Selective, Metabolically Stable, and Orally Bioavailable Inhibitor of CSNK2

  • Han Wee Ong,
  • Xuan Yang,
  • Jeffery L. Smith,
  • Sharon Taft-Benz,
  • Stefanie Howell,
  • Rebekah J. Dickmander,
  • Tammy M. Havener,
  • Marcia K. Sanders,
  • Jason W. Brown,
  • Rafael M. Couñago,
  • Edcon Chang,
  • Andreas Krämer,
  • Nathaniel J. Moorman,
  • Mark Heise,
  • Alison D. Axtman,
  • David H. Drewry,
  • Timothy M. Willson

DOI
https://doi.org/10.3390/molecules29174158
Journal volume & issue
Vol. 29, no. 17
p. 4158

Abstract

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The host kinase casein kinase 2 (CSNK2) has been proposed to be an antiviral target against β-coronaviral infection. To pharmacologically validate CSNK2 as a drug target in vivo, potent and selective CSNK2 inhibitors with good pharmacokinetic properties are required. Inhibitors based on the pyrazolo[1,5-a]pyrimidine scaffold possess outstanding potency and selectivity for CSNK2, but bioavailability and metabolic stability are often challenging. By strategically installing a fluorine atom on an electron-rich phenyl ring of a previously characterized inhibitor 1, we discovered compound 2 as a promising lead compound with improved in vivo metabolic stability. Compound 2 maintained excellent cellular potency against CSNK2, submicromolar antiviral potency, and favorable solubility, and was remarkably selective for CSNK2 when screened against 192 kinases across the human kinome. We additionally present a co-crystal structure to support its on-target binding mode. In vivo, compound 2 was orally bioavailable, and demonstrated modest and transient inhibition of CSNK2, although antiviral activity was not observed, possibly attributed to its lack of prolonged CSNK2 inhibition.

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