| Literature DB >> 31408436 |
Soizic Garaud1, Laurence Buisseret1, Cinzia Solinas1, Chunyan Gu-Trantien1, Alexandre de Wind2, Gert Van den Eynden3, Celine Naveaux1, Jean-Nicolas Lodewyckx1, Anaïs Boisson1, Hughes Duvillier1,4, Ligia Craciun2, Lieveke Ameye5, Isabelle Veys6, Marianne Paesmans5, Denis Larsimont2, Martine Piccart-Gebhart7, Karen Willard-Gallo1.
Abstract
Tumor-infiltrating B-cells (TIL-B) in breast cancer (BC) have previously been associated with improved clinical outcomes; however, their role(s) in tumor immunity is not currently well known. This study confirms and extends the correlation between higher TIL-B densities and positive outcomes through an analysis of HER2-positive and triple-negative BC patients from the BIG 02-98 clinical trial (10yr mean follow-up). Fresh tissue analyses identify an increase in TIL-B density in untreated primary BC compared to normal breast tissues, which is associated with global, CD4+ and CD8+ 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 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 TIL-B are responsive to BCR stimulation ex vivo, express activation markers and produce cytokines and immunoglobulins 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 generate effective anti-tumor immunity at the tumor site.Entities:
Keywords: Adaptive immunity; B cells; Breast cancer; Immunology; Oncology
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Year: 2019 PMID: 31408436 PMCID: PMC6795287 DOI: 10.1172/jci.insight.129641
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708