npj Precision Oncology (Aug 2022)

Comparative biomarker analysis of PALOMA-2/3 trials for palbociclib

  • Zhou Zhu,
  • Nicholas C. Turner,
  • Sherene Loi,
  • Fabrice André,
  • Miguel Martin,
  • Véronique Diéras,
  • Karen A. Gelmon,
  • Nadia Harbeck,
  • Cathy Zhang,
  • Joan Q. Cao,
  • Zhengming Yan,
  • Dongrui R. Lu,
  • Ping Wei,
  • Todd L. VanArsdale,
  • Paul A. Rejto,
  • Xin Huang,
  • Hope S. Rugo,
  • Sibylle Loibl,
  • Massimo Cristofanilli,
  • Richard S. Finn,
  • Yuan Liu

DOI
https://doi.org/10.1038/s41698-022-00297-1
Journal volume & issue
Vol. 6, no. 1
pp. 1 – 10

Abstract

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Abstract While cyclin-dependent kinase 4/6 (CDK4/6) inhibitors, including palbociclib, combined with endocrine therapy (ET), are becoming the standard-of-care for hormone receptor–positive/human epidermal growth factor receptor 2‒negative metastatic breast cancer, further mechanistic insights are needed to maximize benefit from the treatment regimen. Herein, we conducted a systematic comparative analysis of gene expression/progression-free survival relationship from two phase 3 trials (PALOMA-2 [first-line] and PALOMA-3 [≥second-line]). In the ET-only arm, there was no inter-therapy line correlation. However, adding palbociclib resulted in concordant biomarkers independent of initial ET responsiveness, with shared sensitivity genes enriched in estrogen response and resistance genes over-represented by mTORC1 signaling and G2/M checkpoint. Biomarker patterns from the combination arm resembled patterns observed in ET in advanced treatment-naive patients, especially patients likely to be endocrine-responsive. Our findings suggest palbociclib may recondition endocrine-resistant tumors to ET, and may guide optimal therapeutic sequencing by partnering CDK4/6 inhibitors with different ETs. Pfizer (NCT01740427; NCT01942135).