4.6 Article

Differences in the Immune Response of the Nonmetastatic Axillary Lymph Nodes between Triple-Negative and Luminal A Breast Cancer Surrogate Subtypes

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AMERICAN JOURNAL OF PATHOLOGY
卷 191, 期 3, 页码 545-554

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ELSEVIER SCIENCE INC
DOI: 10.1016/j.ajpath.2020.11.008

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资金

  1. Institute of Health Carlos III [PI11/0488, PI13/02501]
  2. European Union European Regional Development Fund
  3. AIDPATH FP7-PEOPLE Project [612471]
  4. Oncology Master Plan for Catalonia (Pla Director d'Oncologia de Catalunya)

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This study aimed to determine the differences in immune populations between primary tumors and ALNs(-) associated with luminal A or TNBC subtypes. The findings showed that TNBC samples had higher levels of immune markers in both primary tumors and ALNs(-) compared to luminal A, which partially explains the worse prognosis of TNBC patients.
Breast cancer (BC) comprises four immunohistochemical surrogate subtypes of which triple-negative breast cancer (TNBC) has the highest risk of mortality. Axillary lymph nodes (ALNs) are the regions where BC cells first establish before distant metastasis, and the presence of tumor cells in the ALN causes an immune tolerance profile that contrasts with that of the nonmetastatic ALN (ALN(-)). However, few studies have compared the immune components of the ALNs(-) in BC subtypes. The present study aimed to determine whether differences between immune populations in the primary tumor and ALNs(-) were associated with the luminal A or TNBC subtype. We evaluated a retrospective cohort of 144 patients using paraffin-embedded biopsies. The TNBC samples tended to have a higher histologic grade and proliferation index and had higher levels of immune markers compared with luminal A in primary tumors and ALNs(-). Two methods for validating the multivariate analysis found that histologic grade, intratumoral S100 dendritic cells, and CD8 T lymphocytes and CD57 natural killer cells in the ALNs(-) were factors associated with TNBC, whereas CD83 dendritic cells in the ALNs(-) were associated with the luminal A subtype. In conclusion, we found that intratumoral regions and ALNs(-) of TNBC contained higher concentrations of markers related to immune tolerance than luminal A. This finding partially explains the worse prognosis of patients with TNBC.

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