PLoS ONE (Jan 2017)

TGF-β3 Inhibits Antibody Production by Human B Cells.

  • Yumi Tsuchida,
  • Shuji Sumitomo,
  • Kazuyoshi Ishigaki,
  • Akari Suzuki,
  • Yuta Kochi,
  • Haruka Tsuchiya,
  • Mineto Ota,
  • Toshihiko Komai,
  • Mariko Inoue,
  • Kaoru Morita,
  • Tomohisa Okamura,
  • Kazuhiko Yamamoto,
  • Keishi Fujio

DOI
https://doi.org/10.1371/journal.pone.0169646
Journal volume & issue
Vol. 12, no. 1
p. e0169646

Abstract

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TGF-β is a pleotropic cytokine involved in various biological processes. Of the three isoforms of TGF-β, TGF-β1 has long been recognized as an important inhibitory cytokine in the immune system and has been reported to inhibit B cell function in both mice and humans. Recently, it has been suggested that TGF-β3 may play an important role in the regulation of immune system in mice. Murine CD4+CD25-LAG3+ regulatory T cells suppress B cell function through the production of TGF-β3, and it has been reported that TGF-β3 is therapeutic in a mouse model of systemic lupus erythematosus. The effect of TGF-β3 on human B cells has not been reported, and we herein examined the effect of TGF-β3 on human B cells. TGF-β3 suppressed B cell survival, proliferation, differentiation into plasmablasts, and antibody secretion. Although the suppression of human B cells by TGF-β1 has long been recognized, the precise mechanism for the suppression of B cell function by TGF-β1 remains elusive; therefore, we examined the effect of TGF-β1 and β3 on pathways important in B cell activation and differentiation. TGF-β1 and TGF-β3 inhibited some of the key molecules of the cell cycle, as well as transcription factors important in B cell differentiation into antibody secreting cells such as IRF4, Blimp-1, and XBP1. TGF-β1 and β3 also inhibited B cell receptor signaling. Our results suggest that TGF-β3 modifying therapy might be therapeutic in autoimmune diseases with B cell dysregulation in humans.