npj Breast Cancer (Oct 2024)

Predictors of response to CDK4/6i retrial after prior CDK4/6i failure in ER+ metastatic breast cancer

  • Nicholas Mai,
  • Carlos H. dos Anjos,
  • Pedram Razavi,
  • Anton Safonov,
  • Sujata Patil,
  • Yuan Chen,
  • Joshua Z. Drago,
  • Shanu Modi,
  • Jacqueline F. Bromberg,
  • Chau T. Dang,
  • Dazhi Liu,
  • Larry Norton,
  • Mark Robson,
  • Sarat Chandarlapaty,
  • Komal Jhaveri

DOI
https://doi.org/10.1038/s41523-024-00699-3
Journal volume & issue
Vol. 10, no. 1
pp. 1 – 9

Abstract

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Abstract After disease progression on endocrine therapy (ET) plus a CDK4/6 inhibitor, there is no standardized sequence for subsequent treatment lines for estrogen receptor positive (ER+) metastatic breast cancer (MBC). CDK4/6i retrial as a treatment strategy is commonplace in modern clinical practice; however, the available prospective data investigating this strategy have had inconclusive results. To frame this data in a real-world context, we performed a retrospective analysis assessing the efficacy of CDK4/6is in 195 patients who had previous exposure to CDK4/6i in a prior treatment line at our institution. Among patients who had stopped a CDK4/6i due to toxicity, CDK4/6i retrial either immediately after with a different CDK4/6i or in a further treatment line with the same initial CDK4/6i was both safe and effective, with a median time to treatment failure (TTF) of 10.1 months (95%CI, 4.8–16.9). For patients whose disease progressed on a prior CDK4/6i, we demonstrated comparable median TTFs for patients rechallenged with the same CDK4/6i (4.3 months, 95%CI 3.2–5.5) and with a different CDK4/6i (4.7 months, 95%CI 3.7–6.0) when compared to the recent PACE, PALMIRA, and MAINTAIN trials. Exploratory genomic analysis suggested that the presence of mutations known to confer CDK4/6i resistance, such as TP53 mutations, CDK4 amplifications, and RB1 or FAT1 loss of function mutations may be molecular biomarkers predictive of CDK4/6i retrial failure.