Context-dependent induction of autoimmunity by TNF signaling deficiency
Tam D. Quach, … , Yong-Rui Zou, Anne Davidson
Tam D. Quach, … , Yong-Rui Zou, Anne Davidson
Published February 1, 2022
Citation Information: JCI Insight. 2022;7(5):e149094. https://doi.org/10.1172/jci.insight.149094.
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Research Article Immunology

Context-dependent induction of autoimmunity by TNF signaling deficiency

Abstract

TNF inhibitors are widely used to treat inflammatory diseases; however, 30%–50% of treated patients develop new autoantibodies, and 0.5%–1% develop secondary autoimmune diseases, including lupus. TNF is required for formation of germinal centers (GCs), the site where high-affinity autoantibodies are often made. We found that TNF deficiency in Sle1 mice induced TH17 T cells and enhanced the production of germline encoded, T-dependent IgG anti-cardiolipin antibodies but did not induce GC formation or precipitate clinical disease. We then asked whether a second hit could restore GC formation or induce pathogenic autoimmunity in TNF-deficient mice. By using a range of immune stimuli, we found that somatically mutated autoantibodies and clinical disease can arise in the setting of TNF deficiency via extrafollicular pathways or via atypical GC-like pathways. This breach of tolerance may be due to defects in regulatory signals that modulate the negative selection of pathogenic autoreactive B cells.

Authors

Tam D. Quach, Weiqing Huang, Ranjit Sahu, Catherine M.M. Diadhiou, Chirag Raparia, Roshawn Johnson, Tung Ming Leung, Susan Malkiel, Peta Gay Ricketts, Stefania Gallucci, Çagla Tükel, Chaim O. Jacob, Martin L. Lesser, Yong-Rui Zou, Anne Davidson

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Figure 2

Inflammatory effector T cells are enhanced in TNF-deficient mice.

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Inflammatory effector T cells are enhanced in TNF-deficient mice. (A–C) ...
(AC) Bar graphs show the percentage of Tregs (TR — CD3+CD4+Foxp3+) (A), TFH cells (CD3+CD4+PSGL1CD44+PD1hiBcl6hi) (B), and TFR cells (CD3+CD4+PSGL1CD44+PD1hiBcl6hiFoxp3+) (C) in CD4+ T cells of Sle1 and Sle1 TNF–/– mice (y, young, 2–3 months old; o, old, >8 months old). ANOVA Kruskal-Wallis with Dunn’s multiple comparisons test, *P < 0.05: **P < 0.01, ***P < 0.001. (DF) Summary results of TR, TFH, and TFR cell counts in old mice, Mann-Whitney nonparametric test, *P < 0.05. (G) Plots show IL-17 expression in CD4+ T cells with (+)/without (-) PMA stimulation from Sle1 and Sle1 TNF–/– mice. (H) Summary bar plot shows the percentage of IL-17+ T cells in total CD3+ and indicated T cell subsets with/without PMA stimulation. Sle1 mice are shown in unfilled symbols, and Sle1 TNF–/– mice are shown in filled symbols. Ordinary 2-way ANOVA with Tukey’s multiple comparisons test, *P < 0.05: **P < 0.01, ****P < 0.0001. DP, CD4+CD8+; DN, CD4CD8.