Tumor-infiltrating B cells signal functional humoral immune responses in breast cancer
Soizic Garaud, Laurence Buisseret, Cinzia Solinas, Chunyan Gu-Trantien, Alexandre de Wind, Gert Van den Eynden, Celine Naveaux, Jean-Nicolas Lodewyckx, Anaïs Boisson, Hughes Duvillier, Ligia Craciun, Lieveke Ameye, Isabelle Veys, Marianne Paesmans, Denis Larsimont, Martine Piccart-Gebhart, Karen Willard-Gallo
Soizic Garaud, Laurence Buisseret, Cinzia Solinas, Chunyan Gu-Trantien, Alexandre de Wind, Gert Van den Eynden, Celine Naveaux, Jean-Nicolas Lodewyckx, Anaïs Boisson, Hughes Duvillier, Ligia Craciun, Lieveke Ameye, Isabelle Veys, Marianne Paesmans, Denis Larsimont, Martine Piccart-Gebhart, Karen Willard-Gallo
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Research Article Immunology Oncology

Tumor-infiltrating B cells signal functional humoral immune responses in breast cancer

Abstract

Tumor-infiltrating B cells (TIL-B) in breast cancer (BC) have previously been associated with improved clinical outcomes; however, their roles in tumor immunity are not currently well known. This study confirms and extends the correlation between higher TIL-B densities and positive outcomes through an analysis of HER2+ and triple-negative BC patients from the BIG 02-98 clinical trial (10-year median follow-up). Fresh tissue analyses identify an increase in TIL-B density in untreated primary BC compared with normal breast tissues, which is associated with global, CD4+, and CD8+ tumor infiltrating lymphocytes (TIL); higher tumor grades; higher proliferation; and hormone receptor negativity. All B cell differentiation stages are detectable, but significant increases in memory TIL-B are consistently present. BC with higher infiltrates are specifically characterized by germinal center TIL-B, which in turn are correlated with T follicular helper (TFH) TIL and antibody-secreting TIL-B principally located in tertiary lymphoid structures. Some TIL-B also interact directly with tumor cells. Functional analyses reveal that TIL-B are responsive to B cell receptor (BCR) stimulation ex vivo, express activation markers, and produce cytokines and Igs despite reduced expression of the antigen-presenting molecules HLA-DR and CD40. Overall, these data support the concept that ongoing humoral immune responses are generated by TIL-B and help to promote effective antitumor immunity at the tumor site.

Authors

Soizic Garaud, Laurence Buisseret, Cinzia Solinas, Chunyan Gu-Trantien, Alexandre de Wind, Gert Van den Eynden, Celine Naveaux, Jean-Nicolas Lodewyckx, Anaïs Boisson, Hughes Duvillier, Ligia Craciun, Lieveke Ameye, Isabelle Veys, Marianne Paesmans, Denis Larsimont, Martine Piccart-Gebhart, Karen Willard-Gallo

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Figure 2

B cell infiltration in breast cancer tissues.

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B cell infiltration in breast cancer tissues. (A–H) B cell infiltration ...
(AH) B cell infiltration was determined as an absolute number normalized to the weight (mg) of the tissue sample (A, C, E, and G) and as a percentage (B, D, F, and H) of CD45+ TIL in the tissue by FACS. B cell infiltration was analyzed according to breast tissue type and cancer histology (A and B), BC stage (C and D), and global TIL infiltration in IDC (E and F) and in ILC (G and H). Data represent a combination of experiments involving individual patients and are displayed as the mean ± SEM by 1-way ANOVA with Dunn’s multiple comparisons test (normal, n = 62; NANT, n = 312; benign, n = 21; IDC, n = 241; ILC, n = 62; stage I–III, n = 241; stage IV, n = 6, local recurrence (rec.), n = 9; IDC TILneg, n = 78; IDC TILint, n = 84; IDC TILhi, n = 79; ILC TILneg, n = 21; ILC TILint, n = 16; ILC TILhi, n = 14). *P < 0.05; **P < 0.01; ***P < 0.001; ****P < 0.0001. NANT, nonadjacent nontumor; IDC, invasive ductal carcinoma; ILC, invasive lobular carcinoma; TIL, tumor-infiltrating lymphocytes. See also Supplemental Table 3 and Supplemental Figure 1.