AI Article Synopsis

  • Tumor-associated macrophages (TAMs) play a crucial role in breast cancer, with M1 macrophages promoting inflammation and immune response, while M2 macrophages support tumor growth and immune suppression.
  • The study analyzed 367 invasive breast cancer cases using immunohistochemistry to evaluate markers CD68, CD11c, and CD163 and their relation to various tumor characteristics and patient outcomes.
  • Findings show that higher levels of CD163+ (M2) macrophages correlate with worse survival outcomes, while CD11c+ (M1) macrophages are associated with better survival, highlighting the complex role of TAMs as both unfavorable and favorable prognostic factors in invasive breast cancer.

Article Abstract

Purpose: Tumor-associated macrophages (TAMs) are activated macrophages associated with tumor progression in various cancers. TAMs can polarize M1 or M2 type. M1 has a pro-inflammatory function and kills pathogens. Conversely, M2 shows immunosuppressive action and promotes tumor growth. There are various markers of TAMs. CD11c is considered as a specific marker of M1. CD163 is an optimal marker for M2. CD68 is known as a pan-macrophage marker. We evaluated the relationship between the clinicopathological parameters and immunohistochemical expressions of CD11c, CD163, and CD68 in invasive breast cancer (IBC), and the prognostic value of macrophage localization within the tumor stroma (TS) and tumor nest (TN).

Methods: Immunohistochemistry of CD68, CD11c, and CD163 was analyzed on tissue microarrays of 367 IBCs. The number of CD68+, CD11c+, or CD163+ macrophages in TN vs. TS was counted by 2 pathologists. The correlations between the degree of macrophage (CD68+, CD11c+, or CD163+) infiltration and the clinicopathological parameters were analyzed. We also assessed the impact of macrophages (CD68+, CD11c+, or CD163+) on disease free survival (DFS) and overall survival (OS).

Results: High numbers of macrophages (CD68+, CD11c+, or CD163+) were associated with higher histologic grade, higher Ki-67 proliferating index, estrogen receptor negativity, and progesterone receptor negativity. High numbers of macrophages (CD11c+ or CD163+) in TS were associated with a larger tumor size. Furthermore, CD163+ macrophages in TN were an independent prognostic marker of reduced OS and DFS. Conversely, CD11c+ macrophages in TS were an independent prognostic marker for higher OS and DFS.

Conclusion: TAMs, including M2 type, are associated with tumor progression in IBC. They can also act as a significant unfavorable or favorable prognostic factor. In addition to simply analyzing the degree of TAM infiltration, it is also important to analyze the location of TAMs.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6438840PMC
http://dx.doi.org/10.4048/jbc.2019.22.e5DOI Listing

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