Communications Medicine (Feb 2024)

S100A8/A9 predicts response to PIM kinase and PD-1/PD-L1 inhibition in triple-negative breast cancer mouse models

  • Lauren R. Begg,
  • Adrienne M. Orriols,
  • Markella Zannikou,
  • Chen Yeh,
  • Pranathi Vadlamani,
  • Deepak Kanojia,
  • Rosemary Bolin,
  • Sara F. Dunne,
  • Sanjeev Balakrishnan,
  • Roman Camarda,
  • Diane Roth,
  • Nicolette A. Zielinski-Mozny,
  • Christina Yau,
  • Athanassios Vassilopoulos,
  • Tzu-Hsuan Huang,
  • Kwang-Youn A. Kim,
  • Dai Horiuchi

DOI
https://doi.org/10.1038/s43856-024-00444-8
Journal volume & issue
Vol. 4, no. 1
pp. 1 – 17

Abstract

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Abstract Background Understanding why some triple-negative breast cancer (TNBC) patients respond poorly to existing therapies while others respond well remains a challenge. This study aims to understand the potential underlying mechanisms distinguishing early-stage TNBC tumors that respond to clinical intervention from non-responders, as well as to identify clinically viable therapeutic strategies, specifically for TNBC patients who may not benefit from existing therapies. Methods We conducted retrospective bioinformatics analysis of historical gene expression datasets to identify a group of genes whose expression levels in early-stage tumors predict poor clinical outcomes in TNBC. In vitro small-molecule screening, genetic manipulation, and drug treatment in syngeneic mouse models of TNBC were utilized to investigate potential therapeutic strategies and elucidate mechanisms of drug action. Results Our bioinformatics analysis reveals a robust association between increased expression of immunosuppressive cytokine S100A8/A9 in early-stage tumors and subsequent disease progression in TNBC. A targeted small-molecule screen identifies PIM kinase inhibitors as capable of decreasing S100A8/A9 expression in multiple cell types, including TNBC and immunosuppressive myeloid cells. Combining PIM inhibition and immune checkpoint blockade induces significant antitumor responses, especially in otherwise resistant S100A8/A9-high PD-1/PD-L1-positive tumors. Notably, serum S100A8/A9 levels mirror those of tumor S100A8/A9 in a syngeneic mouse model of TNBC. Conclusions Our data propose S100A8/A9 as a potential predictive and pharmacodynamic biomarker in clinical trials evaluating combination therapy targeting PIM and immune checkpoints in TNBC. This work encourages the development of S100A8/A9-based liquid biopsy tests for treatment guidance.