Endogenous antigens shape the transcriptome and TCR repertoire in an autoimmune arthritis model
Elizabeth E. McCarthy, … , Arthur Weiss, Judith F. Ashouri
Elizabeth E. McCarthy, … , Arthur Weiss, Judith F. Ashouri
Published November 26, 2024
Citation Information: J Clin Invest. 2025;135(2):e174647. https://doi.org/10.1172/JCI174647.
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Research Article Autoimmunity Immunology

Endogenous antigens shape the transcriptome and TCR repertoire in an autoimmune arthritis model

Abstract

The development of pathogenic autoreactive CD4+ T cells, particularly in the context of impaired signaling, remains poorly understood. Unraveling how defective signaling pathways contribute to their activation and persistence is crucial for identifying new therapeutic targets. We performed bulk and single-cell RNA-Seq (scRNA-Seq) and single-cell T cell receptor sequencing (scTCR-Seq) to profile a highly arthritogenic subset of naive CD4+ T cells from BALB/c-Zap70*W163C (SKG) mice, which develop CD4+ T cell–mediated autoimmune arthritis driven by a hypomorphic mutation in Zap70 — a key TCR signaling kinase. Despite impaired signaling, these cells exhibited heightened expression of T cell activation and cytokine signaling genes but diminished expression of a subset of tolerogenic markers (Izumo1r, Tnfrsf9, Cd5, S100a11) compared with WT cells. The arthritogenic cells showed an enrichment for TCR variable β (Vβ) chains targeting superantigens (Sags) from the endogenous mouse mammary tumor virus (MMTV) but exhibited diminished induction of tolerogenic markers following peripheral antigen encounter, contrasting with the robust induction of the negative regulators seen in WT cells. In arthritic joints, cells expressing Sag-reactive Vβs expanded alongside detectable MMTV proviruses. Antiretroviral treatment and Sag-reactive T cell depletion curtailed SKG arthritis, suggesting that endogenous retroviruses disrupted peripheral tolerance and promoted the activation and differentiation of autoreactive CD4+ T cells into pathogenic effector cells.

Authors

Elizabeth E. McCarthy, Steven Yu, Noah Perlmutter, Yuka Nakao, Ryota Naito, Charles Lin, Vivienne Riekher, Joe DeRisi, Chun Jimmie Ye, Arthur Weiss, Judith F. Ashouri

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Figure 5

SKG CD4+ T cells harbor a biased TCR Vβ gene repertoire.

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SKG CD4+ T cells harbor a biased TCR Vβ gene repertoire. (A and B) Scatt...
(A and B) Scatterplot of the mean frequency of cells expressing each TRBV (A) or TRAV (B) gene for the SKGNur GFPhi samples versus the WTNur GFPhi samples. Dots for each TRBV and TRAV genes are sized according to the FDR using a 1-sided, 1-tailed paired t test with B-H correction comparing frequencies in SKGNur GFPhi versus SKGNur GFPlo cells. Dots are colored as either significantly enriched (FDR <0.1) in SKGNur GFPhi cells (dark blue), significantly enriched in SKGNur GFPlo cells (light blue), or not significantly enriched in either cell subgroup (black). Dots for significant TRBV genes are labeled with the TRBV gene name. Labels for TRBV genes that were significantly enriched in SKGNur GFPhi cells and were also more highly expressed in SKGNur GFPhi samples versus WTNur GFPhi samples are bolded. (C) Bar plot of the mean value of cells expressing each TRBV gene as a percentage of all cells in each sample with an assigned TRBV. Bars are colored according to subgroup and ordered with the TRBV genes enriched in SKGNur GFPhi cells from A, followed by the other TRBV genes ordered by increasing overall frequency. (D) Bar plots of the frequency of cells for each of the 2 replicate mice in each subgroup expressing the indicated TRBV genes which were significantly enriched in SKGNur GFPhi. (E and F) Representative FACS plots (E) of naive peripheral CD4+ T cells with the indicated TCR Vβ protein usage determined by flow cytometry in GFPlo and GFPhi T cells from LNs of WTNur and SKGNur mice prior to arthritis induction and quantification (F), where bar graphs depict the mean frequency (± SEM). n = 3–4 mice per group. The experiment was repeated at least 3 times. *P < 0.05 and **P < 0.01, for FDR (2-tailed paired Student’s t test with B-H correction) or P value (exact permutation test).