npj Breast Cancer (Nov 2022)

Ruxolitinib and exemestane for estrogen receptor positive, aromatase inhibitor resistant advanced breast cancer

  • Igor Makhlin,
  • Nicholas P. McAndrew,
  • E. Paul Wileyto,
  • Amy S. Clark,
  • Robin Holmes,
  • Lisa N. Bottalico,
  • Clementina Mesaros,
  • Ian A. Blair,
  • Grace R. Jeschke,
  • Kevin R. Fox,
  • Susan M. Domchek,
  • Jennifer M. Matro,
  • Angela R. Bradbury,
  • Michael D. Feldman,
  • Elizabeth O. Hexner,
  • Jacqueline F. Bromberg,
  • Angela DeMichele

DOI
https://doi.org/10.1038/s41523-022-00487-x
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 9

Abstract

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Abstract Circulating IL-6, an activator of JAK/STAT signaling, is associated with poor prognosis and aromatase inhibitor (AI) resistance in hormone-receptor positive (HR+) breast cancer. Here we report the results of a phase 2 single-arm Simon 2-stage trial combining Ruxolitinib, an oral selective inhibitor of JAK1/2, with exemestane, a steroidal AI, in patients with HR+ metastatic breast cancer (MBC) after progression on non-steroidal AI (NSAI). Safety and efficacy were primary objectives, and analysis of inflammatory markers as predictors of response was a key secondary objective. Twenty-five subjects enrolled. The combination of ruxolitinib and exemestane was safe, though anemia requiring transfusion in 5/15 (33%) at the 25 mg dose in stage 1 led to a reduction to 15 mg twice daily in stage 2 (with no additional transfusions). Clinical benefit rate (CBR) in the overall study population was 24% (95% CI 9.4–45.1); 6/25 patients demonstrated stable disease for ≥6 months. Median progression-free survival was 2.8 months (95% CI 2.6–3.9). Exploratory biomarkers revealed high levels of systemic inflammation and 60% harbored a high-risk IL-6 genotype. Pharmacodynamics demonstrated modest on-target inhibition of phosphorylated-STAT3 by ruxolitinib at a tolerable dose. Thus, ruxolitinib combined with exemestane at a tolerable dose was safe but minimally active in AI-resistant tumors of patients with high levels of systemic inflammation. These findings highlight the need for more potent and specific therapies targeting inflammation in MBC.