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B-cell populations are expanded in breast cancer patients compared with healthy controls
Authors:Banri Tsuda  Asuka Miyamoto  Kozue Yokoyama  Rin Ogiya  Risa Oshitanai  Mayako Terao  Toru Morioka  Naoki Niikura  Takuho Okamura  Hirohito Miyako  Yuki Saito  Yasuhiro Suzuki  Yoshie Kametani  Yutaka Tokuda
Affiliation:1.Department of Breast and Endocrine Surgery,Tokai University School of Medicine,Kanagawa,Japan;2.Department of Breast and Endocrine Surgery,Tokai University Hachioji Hospital,Hachioji,Japan;3.Department of Surgery,Niwa Hospital,Odawara,Japan;4.Department of Molecular Life Science, Division of Basic Medical Science,Tokai University School of Medicine,Isehara,Japan
Abstract:

Background

Historically, humoral immunity was considered unimportant in anti-tumor immunity, and the differentiation and anti-tumor activity of B cells in breast cancer are poorly understood. However, it was recently discovered that B cells participate in tumor immunity through both antibody production and immunosuppressive mechanisms. We analyzed the expression of B-cell differentiation markers in detail using fluorescence-activated cell sorting to investigate the relationship between B-cell subsets and breast cancer etiology.

Methods

Blood samples were taken from breast cancer patients and healthy donors, and peripheral blood mononuclear cells were collected. B cells at various stages of differentiation were identified by the expression of combinations of the cell surface markers CD5, CD19, CD21, CD24, CD27, CD38, CD45, and IgD. Statistical analysis of the proportions of each B-cell subtype in the different patient groups was then performed.

Results

Twenty-seven breast cancer patients and 12 controls were considered. The proportion of total B cells was significantly higher in cancer patients than in controls (11.51 ± 2.059 vs 8.905 ± 0.379%, respectively; p = 0.001). Breast cancer patients were then classified as High-B or Low-B for further analysis. A significantly higher proportion of memory B cells was found in the High-B group than in the Low-B or control groups (p = 0.003 and p = 0.043, respectively).

Conclusions

Breast cancer patients generally have a higher proportion of B cells than healthy controls, but this is highly variable. Analysis of the major B-cell surface markers indicates that memory B cells in particular are significantly expanded, or more robust, in breast cancer patients.
Keywords:
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