Medullary thymic epithelial cell depletion leads to autoimmune hepatitis
Anthony J. Bonito, … , Matthew C. Walsh, Konstantina Alexandropoulos
Anthony J. Bonito, … , Matthew C. Walsh, Konstantina Alexandropoulos
Published July 15, 2013
Citation Information: J Clin Invest. 2013;123(8):3510-3524. https://doi.org/10.1172/JCI65414.
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Research Article Immunology

Medullary thymic epithelial cell depletion leads to autoimmune hepatitis

Abstract

TRAF6, an E3 ubiquitin protein ligase, plays a critical role in T cell tolerance by regulating medullary thymic epithelial cell (mTEC) development. mTECs regulate T cell tolerance by ectopically expressing self-antigens and eliminating autoreactive T cells in the thymus. Here we show that mice with mTEC depletion due to conditional deletion of Traf6 expression in murine thymic epithelial cells (Traf6ΔTEC mice) showed a surprisingly narrow spectrum of autoimmunity affecting the liver. The liver inflammation in Traf6ΔTEC mice exhibited all the histological and immunological characteristics of human autoimmune hepatitis (AIH). The role of T cells in AIH establishment was supported by intrahepatic T cell population changes and AIH development after transfer of liver T cells into immunodeficient mice. Despite a 50% reduction in natural Treg thymic output, peripheral tolerance in Traf6ΔTEC mice was normal, whereas compensatory T regulatory mechanisms were evident in the liver of these animals. These data indicate that mTECs exert a cell-autonomous role in central T cell tolerance and organ-specific autoimmunity, but play a redundant role in peripheral tolerance. These findings also demonstrate that Traf6ΔTEC mice are a relevant model with which to study the pathophysiology of AIH, as well as autoantigen-specific T cell responses and regulatory mechanisms underlying this disease.

Authors

Anthony J. Bonito, Costica Aloman, M. Isabel Fiel, Nichole M. Danzl, Sungwon Cha, Erica G. Weinstein, Seihwan Jeong, Yongwon Choi, Matthew C. Walsh, Konstantina Alexandropoulos

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Figure 8

Increased numbers of iTregs and cytokines in the liver of Traf6ΔTEC mice.

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Increased numbers of iTregs and cytokines in the liver of Traf6ΔTEC mice...
(A and B) Thymocytes and liver hematopoietic cell suspensions isolated from approximately 8-week-old WT and Traf6ΔTEC mice were stained with anti-CD45–Alexa Fluor 750, anti-CD3–PerCP-Cy5.5, anti-CD4–allophycocyanin, anti-CD8–Pacific Blue, anti-CD25–FITC, and anti-FOXP3–PE antibodies and analyzed by flow cytometry. n = 9 per genotype. (C) Sorted liver or spleen CD4+CD25 T cells isolated from approximately 8-week-old WT and Traf6ΔTEC mice were stimulated with TGF-β in vitro and stained with the above antibodies, and iTregs were analyzed by flow cytometry. n = 9 per genotype, run in triplicates. Data in AC are pooled results from 3 independent experiments. (D and E) Liver lysates from WT and Traf6ΔTEC mice were analyzed for the production of TGF-β and IL-10 cytokines. (D) ELISA. n ≥ 7 per genotype. Data are pooled results from 2 independent experiments run in duplicates. Red bars represent mean. (E) RT-PCR. n = 11 per genotype. Data are pooled results from 2 independent experiments run in triplicates. Bars represent mean + SEM. *P < 0.05; ***P < 0.001.