Shared recognition of citrullinated tenascin-C peptides by T and B cells in rheumatoid arthritis
Jing Song, … , Eddie A. James, Jane H. Buckner
Jing Song, … , Eddie A. James, Jane H. Buckner
Published January 28, 2021
Citation Information: JCI Insight. 2021;6(5):e145217. https://doi.org/10.1172/jci.insight.145217.
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Research Article Immunology

Shared recognition of citrullinated tenascin-C peptides by T and B cells in rheumatoid arthritis

Abstract

Tenascin-C (TNC), an extracellular matrix protein that has proinflammatory properties, is a recently described antibody target in rheumatoid arthritis (RA). In this study, we utilized a systematic discovery process and identified 5 potentially novel citrullinated TNC (cit-TNC) T cell epitopes. CD4+ T cells specific for these epitopes were elevated in the peripheral blood of subjects with RA and showed signs of activation. Cit-TNC–specific T cells were also present among synovial fluid T cells and secreted IFN-γ. Two of these cit-TNC T cell epitopes were also recognized by antibodies within the serum and synovial fluid of individuals with RA. Detectable serum levels of cit-TNC–reactive antibodies were prevalent among subjects with RA and positively associated with cyclic citrullinated peptide (CCP) reactivity and the HLA shared epitope. Furthermore, cit-TNC–reactive antibodies were correlated with rheumatoid factor and elevated in subjects with a history of smoking. This work confirms cit-TNC as an autoantigen that is targeted by autoreactive CD4+ T cells and autoantibodies in patients with RA. Furthermore, our findings raise the possibility that coinciding epitopes recognized by both CD4+ T cells and B cells have the potential to amplify autoimmunity and promote the development and progression of RA.

Authors

Jing Song, Anja Schwenzer, Alicia Wong, Sara Turcinov, Cliff Rims, Lorena Rodriguez Martinez, David Arribas-Layton, Christina Gerstner, Virginia S. Muir, Kim S. Midwood, Vivianne Malmström, Eddie A. James, Jane H. Buckner

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Figure 2

T cells that recognize tenascin-C epitopes are more frequent and have a distinct phenotype in patients with RA.

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T cells that recognize tenascin-C epitopes are more frequent and have a ...
The frequency and phenotype of tetramer+ cit-TNC–specific T cells was determined ex vivo using a multiplex HLA class II tetramer approach including cell surface marker antibodies to define the phenotype. Frequencies are expressed as the number of antigen-specific cells per million CD4+ memory T cells. Each symbol represents an individual subject (n = 7 for HC, n = 9 for RA), and the horizontal bar shows the median. (A) The frequencies of the combined cit-TNC–specific CD4 memory T cells were elevated in patients with RA compared with HC subjects, but the frequencies of influenza-specific CD4+ memory T cells were similar between RA and HC subjects. (B) The increased frequency of cit-TNC–specific CD4+ memory T cells appeared to be mainly due to cit-TNC45, cit-TNC50, and cit-TNC56. (C) The heatmap shows the cit-TNC T cell frequency for each epitope in each subject. Each row stands for a single epitope, and each column stands for 1 RA subject; intensity based on the number of cit-TNC T cells per million CD4+ memory T cells. (D) The frequencies of CCR4+, CCR6+, and CD38+ cit-TNC–specific CD4+ memory T cells were elevated in patients with RA compared with HC subjects. (E) The percent of CD38+ cells among total cit-TNC–specific memory CD4+ T is increased in patients with RA compared with HC subjects. (F) The lineage of cit-TNC–specific CD4+ memory T cells in RA subjects was predominantly Th2 (CCR4+CCR6CXCR3) and Th17 (CCR4+CCR6+CXCR3), but not Th1 (CXCR3+CCR4CCR6). P values were calculated using an unpaired nonparametric Mann-Whitney U test.