Macrophage spatial polarity to T cells predicts prognosis in young women with luminal breast cancer

  1. Artur Mezheyeuski
  2. Garazi Serna
  3. Alfonso Martín-Bernabé
  4. Neda Hekmati
  5. Ioannis Zerdes
  6. Anna Dénes
  7. Hanna Fredholm
  8. Siarhei Mauchanski
  9. Xavier Guardia
  10. Lidia Alonso
  11. Lynn De Mey
  12. Tony Lahoutte
  13. Marleen Keyaerts
  14. Joakim Lindblad
  15. Nataša Sladoje
  16. Fredrik Wärnberg
  17. Malin Sund
  18. Gunilla Rask
  19. Charlotta Wadsten
  20. Fredrik Pontén
  21. Patrick Micke
  22. Irma Fredriksson
  23. Paolo Nuciforo
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Abstract

Purpose

The prognostic role of tumor-infiltrating lymphocytes in luminal breast cancer remains uncertain, partly because density-based metrics do not capture spatial interactions between immune cell subsets. We developed a density-independent spatial metric quantifying macrophage-T cell proximity and assessed its prognostic value.

Experimental Design

Using multiplex immunohistochemistry across three breast cancer cohorts (exploratory, n = 17; discovery, n = 687; validation, n = 305), we measured nearest-neighbor distances from T cells to M1-like and M2-like macrophages, benchmarked against a randomly subsampled total macrophage pool. We defined the Macrophage Spatial Polarity Index (MSPI) as the difference between M2-to-T cell and M1-to-T cell affinity scores, where higher values reflect an M2-dominated spatial phenotype. Cox regression was used to assess associations with distant disease-free survival (discovery) and overall survival (validation).

Results

M2-like macrophages preferentially localized near T cells, independent of cell density. Higher MSPI was associated with shorter survival in luminal cancers (discovery: HR = 1.45, p < 0.001), with the strongest effect in young women with early-stage disease (HR = 2.16, p < 0.0001). MSPI remained independently prognostic after adjustment for stage, systemic treatment, and diagnosis period (HR = 2.31, 95% CI 1.73-3.09, p < 0.0001) and was non-significant in HER2-positive and triple-negative subtypes. Validation in an independent ER-positive cohort confirmed the finding (HR = 1.30, p = 0.004). Pooled analysis yielded HR = 2.13 (95% CI 1.68-2.70, p = 3.45 x 10⁻¹⁰).

Conclusions

MSPI is a robust prognostic biomarker in luminal breast cancer, particularly in young women with early-stage disease, warranting further validation for risk stratification and therapeutic guidance.

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  1. Version published to 10.64898/2026.05.17.26352909 on medRxiv