Scientific Reports (Aug 2024)

Discovery of the DNA-PKcs inhibitor DA-143 which exhibits enhanced solubility relative to NU7441

  • Zachary J. Waldrip,
  • Baku Acharya,
  • Daniel Armstrong,
  • Maha Hanafi,
  • Randall R. Rainwater,
  • Sharon Amole,
  • Madeline Fulmer,
  • Ana Clara Azevedo-Pouly,
  • Alaina Burns,
  • Lyle Burdine,
  • Brendan Frett,
  • Marie Schluterman Burdine

DOI
https://doi.org/10.1038/s41598-024-70858-w
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 12

Abstract

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Abstract DNA-dependent protein kinase catalytic subunit (DNA-PKcs) plays a vital role in DNA damage repair and lymphocyte function, presenting a significant target in cancer and immune diseases. Current DNA-PKcs inhibitors are undergoing Phase I/II trials as adjuncts to radiotherapy and chemotherapy in cancer. Nevertheless, clinical utility is limited by suboptimal bioavailability. This study introduces DNA-PKcs inhibitors designed to enhance bioavailability. We demonstrate that a novel DNA-PKcs inhibitor, DA-143, surpasses NU7441 in aqueous solubility as well as other available inhibitors. In addition, DA-143 displayed an improvement in DNA-PKcs inhibition relative to NU7441 achieving an IC50 of 2.5 nM. Consistent with current inhibitors, inhibition of DNA-PKcs by DA-143 resulted in increased tumor cell sensitivity to DNA-damage from chemotherapy and inhibition of human T cell function. The improved solubility of DA-143 is critical for enhanced efficacy at reduced doses and facilitates more effective evaluation of DNA-PKcs inhibition in both preclinical and clinical development.