Regulatory B cells inhibit EAE initiation in mice while other B cells promote disease progression
Takashi Matsushita, … , Manabu Fujimoto, Thomas F. Tedder
Takashi Matsushita, … , Manabu Fujimoto, Thomas F. Tedder
Published September 18, 2008
Citation Information: J Clin Invest. 2008;118(10):3420-3430. https://doi.org/10.1172/JCI36030.
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Research Article

Regulatory B cells inhibit EAE initiation in mice while other B cells promote disease progression

Abstract

EAE is a mouse T cell–mediated autoimmune disease of the CNS used to model the human condition MS. The contributions of B cells to EAE initiation and progression are unclear. In this study, we have shown that EAE disease initiation and progression are differentially influenced by the depletion of B cells from mice with otherwise intact immune systems. CD20 antibody–mediated B cell depletion before EAE induction substantially exacerbated disease symptoms and increased encephalitogenic T cell influx into the CNS. Increased symptom severity resulted from the depletion of a rare IL-10–producing CD1dhiCD5+ regulatory B cell subset (B10 cells), since the adoptive transfer of splenic B10 cells before EAE induction normalized EAE in B cell–depleted mice. While transfer of regulatory B10 cells was maximally effective during early EAE initiation, they had no obvious role during disease progression. Rather, B cell depletion during EAE disease progression dramatically suppressed symptoms. Specifically, B cells were required for the generation of CD4+ T cells specific for CNS autoantigen and the entry of encephalitogenic T cells into the CNS during disease progression. These results demonstrate reciprocal regulatory roles for B cells during EAE immunopathogenesis. The therapeutic effect of B cell depletion for the treatment of autoimmunity may therefore depend on the relative contributions and the timing of these opposing B cell activities during the course of disease initiation and pathogenesis.

Authors

Takashi Matsushita, Koichi Yanaba, Jean-David Bouaziz, Manabu Fujimoto, Thomas F. Tedder

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Figure 3

CD20 mAb–induced B cell depletion in EAE mice.

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CD20 mAb–induced B cell depletion in EAE mice. B6 mice were treated with...
B6 mice were treated with CD20 or control mAb 7 days before or 14 days after MOG immunization. Representative depletion of B cells from the (A) bone marrow, (B) blood, (CF) spleen, (G) peripheral lymph nodes, and (H) peritoneal cavity 18 days after MOG immunization (n ≥ 4 mice per group) as determined by immunofluorescence staining with flow cytometry analysis. Within in the histograms, numbers indicate relative percentages of lymphocytes within the indicated gates. Bar graphs indicate (mean ± SEM) numbers of blood (per ml) and tissue B cells following mAb treatment. Within the bar graphs, numbers indicate the percentage of B cells of each phenotype found in CD20 mAb–treated mice (black bars) relative to the numbers of B cells found in control mAb–treated littermates (white bars). Significant differences between CD20 versus control mAb–treated mice are indicated; *P < 0.05, **P < 0.01. Data are representative of at least 2 independent experiments. MZ, marginal zone.