Nature Communications (Apr 2025)

Targeting CCNE1 amplified ovarian and endometrial cancers by combined inhibition of PKMYT1 and ATR

  • Haineng Xu,
  • Erin George,
  • David Gallo,
  • Sergey Medvedev,
  • Xiaolei Wang,
  • Arindam Datta,
  • Rosie Kryczka,
  • Marc L. Hyer,
  • Jimmy Fourtounis,
  • Rino Stocco,
  • Elia Aguado-Fraile,
  • Adam Petrone,
  • Shou Yun Yin,
  • Ariya Shiwram,
  • Fang Liu,
  • Matthew Anderson,
  • Hyoung Kim,
  • Roger A. Greenberg,
  • C. Gary Marshall,
  • Fiona Simpkins

DOI
https://doi.org/10.1038/s41467-025-58183-w
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 19

Abstract

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Abstract Ovarian cancers (OVCAs) and endometrial cancers (EMCAs) with CCNE1-amplification are often resistant to standard treatment and represent an unmet clinical need. Synthetic-lethal screening identified loss of the CDK1 regulator, PKMYT1, as synthetically lethal with CCNE1-amplification. We hypothesize that CCNE1-amplification associated replication stress will be more effectively targeted by combining PKMYT1 inhibitor lunresertib (RP-6306), with ATR inhibitor camonsertib (RP-3500/RG6526). Low dose combination RP-6306 with RP-3500 synergistically increases cytotoxicity more so in CCNE1-amplified compared to non-amplified cells. Combination treatment produces durable antitumor activity, reduces metastasis and increases survival in CCNE1-amplified patient-derived OVCA and EMCA xenografts. Mechanistically, low doses of RP-6306 with RP-3500 increase CDK1 activation more so than monotherapy, triggering rapid and robust induction of premature mitosis, DNA damage, and apoptosis in a CCNE1-dependent manner. These findings suggest that targeting CDK1 activity by combining RP-6306 with RP-3500 is an effective therapeutic approach to treat CCNE1-amplifed OVCAs and EMCAs.