Autoreactive helper T cells alleviate the need for intrinsic TLR signaling in autoreactive B cell activation
Josephine R. Giles, Adriana Turqueti Neves, Ann Marshak-Rothstein, Mark J. Shlomchik
Josephine R. Giles, Adriana Turqueti Neves, Ann Marshak-Rothstein, Mark J. Shlomchik
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Research Article Immunology

Autoreactive helper T cells alleviate the need for intrinsic TLR signaling in autoreactive B cell activation

Abstract

T cells play a significant role in the pathogenesis of systemic autoimmune diseases, including systemic lupus erythematosus; however, there is relatively little information on the nature and specificity of autoreactive T cells. Identifying such cells has been technically difficult because they are likely to be rare and low affinity. Here, we report a method for identifying autoreactive T cell clones that recognize proteins contained in autoantibody immune complexes, providing direct evidence that functional autoreactive helper T cells exist in the periphery of normal mice. These T cells significantly enhanced autoreactive B cell proliferation and altered B cell differentiation in vivo. Most importantly, these autoreactive T cells were able to rescue many aspects of the TLR-deficient AM14 (anti-IgG2a rheumatoid factor) B cell response, suggesting that TLR requirements can be bypassed. This result has implications for the efficacy of TLR-targeted therapy in the treatment of ongoing disease.

Authors

Josephine R. Giles, Adriana Turqueti Neves, Ann Marshak-Rothstein, Mark J. Shlomchik

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Figure 3

13C2 T cells alleviate the need for intrinsic TLR signaling for AM14 proliferation but not Ab production.

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13C2 T cells alleviate the need for intrinsic TLR signaling for AM14 pro...
VPD450-labeled AM14 B cells (WT, Tlr7–/–, Tlr9–/–, Tlr7/9–/–) were cultured with VPD450-labeled T cells from DO11.10 BALB/c mice (top, AC) or 13C2 Rg BALB/c mice (bottom, AC, and D–F) in the presence of PL2-3 (1 μg/ml) or BWR4 (10 μg/ml). Analysis was performed on day 4. (A) The percentage of divided 4-44+ cells was determined by flow cytometry. (B) Total 4-44+ IgM and (C) IgG2a concentration in the culture supernatant. (D) The percentage of divided 13C2 T cells was determined by flow cytometry. (E) Concentrations of IL-2 in the culture supernatant. Data are represented as the percentage of maximum for each of 4 independent experiments; mean ± SEM. Statistics were calculated with 3-way ANOVA (A–C) or 2-way ANOVA (D–F); multiple testing was corrected with Holm-Sidak’s. *P < 0.05; **P < 0.01; ***P < 0.001; ****P < 0.0001.