Tumor‐associated lymphocytes and macrophages are related to stromal elastosis and vascular invasion in breast cancer

Ying Chen; Tor Audun Klingen; Hans Aas; Elisabeth Wik; Lars A Akslen

doi:10.1002/cjp2.226

The Journal of Pathology: Clinical Research (Sep 2021)

Tumor‐associated lymphocytes and macrophages are related to stromal elastosis and vascular invasion in breast cancer

Ying Chen,
Tor Audun Klingen,
Hans Aas,
Elisabeth Wik,
Lars A Akslen

Affiliations

Ying Chen: Centre for Cancer Biomarkers CCBIO, Department of Clinical Medicine University of Bergen Bergen Norway
Tor Audun Klingen: Centre for Cancer Biomarkers CCBIO, Department of Clinical Medicine University of Bergen Bergen Norway
Hans Aas: Department of Surgery Vestfold Hospital Tønsberg Norway
Elisabeth Wik: Centre for Cancer Biomarkers CCBIO, Department of Clinical Medicine University of Bergen Bergen Norway
Lars A Akslen: Centre for Cancer Biomarkers CCBIO, Department of Clinical Medicine University of Bergen Bergen Norway

DOI: https://doi.org/10.1002/cjp2.226
Journal volume & issue: Vol. 7, no. 5
pp. 517 – 527

Abstract

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Abstract The tumor microenvironment plays a critical role in breast cancer progression. Here, we investigated tumor‐infiltrating lymphocytes (TILs) and associations with macrophage numbers, tumor stromal elastosis, vascular invasion, and tumor detection mode. We performed a population‐based retrospective study using data from The Norwegian Breast Cancer Screening Program in Vestfold County (2004–2009), including 200 screen‐detected and 82 interval cancers. The number of TILs (CD45+, CD3+, CD4+, CD8+, and FOXP3+) and tumor‐associated macrophages (CD163+) was counted using immunohistochemistry on tissue microarray slides. Lymphatic and blood vessel invasion (LVI and BVI) were recorded using D2‐40 and CD31 staining, and the amount of elastosis (high/low) was determined on regular HE‐stained slides. High numbers of all TIL subsets were associated with LVI (p ≤ 0.04 for all), and high counts of several TIL subgroups (CD8+, CD45+, and FOXP3+) were associated with BVI (p ≤ 0.04 for all). Increased levels of all TIL subsets, except CD4+, were associated with estrogen receptor‐negative tumors (p < 0.001) and high tumor cell proliferation by Ki67 (p < 0.001). Furthermore, high levels of all TIL subsets were associated with high macrophage counts (p < 0.001) and low‐grade stromal elastosis (p ≤ 0.02). High counts of CD3+, CD8+, and FOXP3+ TILs were associated with interval detected tumors (p ≤ 0.04 for all). Finally, in the luminal A subgroup, high levels of CD3+ and FOXP3+ TILs were associated with shorter recurrence‐free survival, and high counts of FOXP3+ were linked to reduced breast cancer‐specific survival. In conclusion, higher levels of different TIL subsets were associated with stromal features such as high macrophage counts (CD163+), presence of vascular invasion, absence of stromal elastosis, as well as increased tumor cell proliferation and interval detection mode. Our findings support a link between immune cells and vascular invasion in more aggressive breast cancer. Notably, presence of TIL subsets showed prognostic value within the luminal A category.

Published in The Journal of Pathology: Clinical Research

ISSN: 2056-4538 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Pathology
Website: http://onlinelibrary.wiley.com/journal/10.1002/(ISSN)2056-4538

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