Autoimmune-Mediated Intestinal Inflammation–Impact and Regulation of Antigen-Specific CD8 + T Cells
Background & Aims: Few data exist regarding mechanisms of mucosal CD8 + T-cell reactivity to epithelial-specific antigen. To dissect the immunologic mechanisms underlying CD8 + T-cell dysregulation, reactivity to a self-antigen expressed in intestinal epithelium of mice bearing a major histocomp...
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Veröffentlicht in: | Gastroenterology (New York, N.Y. 1943) N.Y. 1943), 2006-08, Vol.131 (2), p.510-524 |
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Zusammenfassung: | Background & Aims:
Few data exist regarding mechanisms of mucosal CD8
+ T-cell reactivity to epithelial-specific antigen. To dissect the immunologic mechanisms underlying CD8
+ T-cell dysregulation, reactivity to a self-antigen expressed in intestinal epithelium of mice bearing a major histocompatibility complex class I–restricted T-cell receptor specific for this antigen was studied. In addition, antigen-specific regulatory CD4
+ T cells induced in vivo were tested to control these autoreactive CD8
+ T cells.
Methods:
Transgenic VILLIN-HA mice were mated with CL4-TCR transgenic mice. Alternatively, adoptive transfer of CL4-TCR transgenic CD8
+ T cells into VILLIN-HA transgenic mice was performed to mimic spontaneous encounter of neoantigen. Mucosal CD8
+ T cells were characterized under different conditions of tolerance, immunopathology, and active immunosuppression.
Results:
Transgenic CD8
+ T cells from VILLIN-HA × CL4-TCR transgenic mice preferentially migrated and expanded in mucosal lymphoid tissues. Although transgenic CD8
+ T cells showed signs of T-cell activation, they failed to cause tissue damage. This was accompanied by the induction/expansion of CD4
+ and CD8
+, Foxp3-expressing T cells. In contrast, adoptive transfer of naive transgenic CD8
+ T cells from CL4-TCR transgenic mice into VILLIN-HA transgenic mice induced severe intestinal inflammation with poor clinical course of disease. Transgenic CD8
+ T cells secreted vigorous amounts of proinflammatory cytokines like interferon γ/tumor necrosis factor α. Strikingly, this acute wasting disease was significantly ameliorated by cotransfer of antigen-specific regulatory CD4
+ T cells.
Conclusions:
Epithelial-specific antigen expression is sufficient to trigger severe antigen-specific CD8
+ T-cell–mediated intestinal inflammation; this might be controlled by antigen-specific regulatory T cells under physiological conditions. |
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ISSN: | 0016-5085 1528-0012 |
DOI: | 10.1053/j.gastro.2006.05.015 |