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A T-Cell Functional Phenotype Common among Autoimmune-Prone Rodent Strains
Article first published online: 19 MAY 2002
DOI: 10.1046/j.1365-3083.2002.01086.x
1365-3083/asset/cover.gif?v=1&s=851263375540b207304bed4ad505b46ca5c4242b "Scandinavian Journal of Immunology")
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How to Cite
Lang, J. and Bellgrau, D. (2002), A T-Cell Functional Phenotype Common among Autoimmune-Prone Rodent Strains. Scandinavian Journal of Immunology, 55: 546–559. doi: 10.1046/j.1365-3083.2002.01086.x
Publication History
- Issue published online: 19 MAY 2002
- Article first published online: 19 MAY 2002
- (Received 19 September 2001; Accepted in revised form 7 February 2002)
- Abstract
- Article
- References
- Cited By
The genetic basis and familial clustering of autoimmunity suggest that common phenotypic traits predispose individuals to disease. We found a hyporesponsive T-cell phenotype that was shared by all autoimmune-prone mouse and rat strains tested, including MRL, nonobese diabetic (NOD), NZB, NZW, NZB/W F1, SJL and SWR mice, as well as DA and BB rats, but was not evident in nonautoimmune-prone rodents. This T-cell intrinsic, age-independent hyporesponsiveness is measured as an increased activation threshold for upregulation of activation markers upon T-cell receptor (TCR) cross-linking both in vitro and in vivo. Inefficient deletion of CD4 and CD8 single-positive, heat stable antigen (HSA)hi medullary thymocytes was also observed in hyporesponsive donors. We interpret these data to suggest that increased TCR-mediated signalling thresholds in autoimmune-prone individuals may contribute to the escape of autoreactive thymocytes from negative selection.