Suppression of allograft rejection by regulatory B cells induced via TLR signaling
Kang Mi Lee, Qiang Fu, Guoli Huai, Kevin Deng, Ji Lei, Lisa Kojima, Divyansh Agarwal, Peter van Galen, Shoko Kimura, Naoki Tanimine, Laura Washburn, Heidi Yeh, Ali Naji, Charles G. Rickert, Christian LeGuern, James F. Markmann
Kang Mi Lee, Qiang Fu, Guoli Huai, Kevin Deng, Ji Lei, Lisa Kojima, Divyansh Agarwal, Peter van Galen, Shoko Kimura, Naoki Tanimine, Laura Washburn, Heidi Yeh, Ali Naji, Charles G. Rickert, Christian LeGuern, James F. Markmann
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Research Article Immunology Transplantation

Suppression of allograft rejection by regulatory B cells induced via TLR signaling

Abstract

B lymphocytes have long been recognized for their critical contributions to adaptive immunity, providing defense against pathogens through cognate antigen presentation to T cells and Ab production. More recently appreciated is that B cells are also integral in securing self-tolerance; this has led to interest in their therapeutic application to downregulate unwanted immune responses, such as transplant rejection. In this study, we found that PMA- and ionomycin-activated mouse B cells acquire regulatory properties following stimulation through TLR4/TLR9 receptors (Bregs-TLR). Bregs-TLR efficiently inhibited T cell proliferation in vitro and prevented allograft rejection. Unlike most reported Breg activities, the inhibition of alloimmune responses by Bregs-TLR relied on the expression of TGF-β and not IL-10. In vivo, Bregs-TLR interrupted donor-specific T cell expansion and induced Tregs in a TGF-β–dependent manner. RNA-Seq analyses corroborated the involvement of TGF-β pathways in Breg-TLR function, identified potential gene pathways implicated in preventing graft rejection, and suggested targets to foster Breg regulation.

Authors

Kang Mi Lee, Qiang Fu, Guoli Huai, Kevin Deng, Ji Lei, Lisa Kojima, Divyansh Agarwal, Peter van Galen, Shoko Kimura, Naoki Tanimine, Laura Washburn, Heidi Yeh, Ali Naji, Charles G. Rickert, Christian LeGuern, James F. Markmann

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Figure 6

Impact of suppressive Bregs on cytokine-producing T cells.

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Impact of suppressive Bregs on cytokine-producing T cells. In vitro freq...
In vitro frequencies and numbers of cytokine-producing T cells in cocultures of OTII CD4+ (A) or OTI CD8+ T cells (B) stimulated by irradiated OVA splenocytes (OVA/SPC) and incubated for 3 days with OVA-specific OBI Bregs-TLR or control OBI Bregs-CpG cells (T cells: Bregs ratios of 1:1 and 1:2). (C) B cell–deficient μMT B6 mice were injected with purified 1 × 106 OTII CD4+ T cells and 5 × 106 Bregs-TLR or Bregs-CpG at day –1. Transplantation of OVA skin grafts was done at day 0, and the in vivo frequencies of OTII T cells producing cytokines were evaluated at day 14 (≥ 4 independent experiments). Data are expressed as mean ± SD. P value (1-way ANOVA): *P < 0.05, **P < 0.01, ***P < 0.001, and ****P < 0.0001.