| Literature DB >> 12932358 |
Katrin Layer1, Guosheng Lin, Alessio Nencioni, Wei Hu, Adam Schmucker, Andrey N Antov, Xiaoyu Li, Satoshi Takamatsu, Timothy Chevassut, Nancy A Dower, Stacey L Stang, David Beier, Janet Buhlmann, Roderick T Bronson, Keith B Elkon, James C Stone, Luk Van Parijs, Bing Lim.
Abstract
A mouse strain was identified with a recessive genetic lesion, which spontaneously developed a lymphoproliferative autoimmune syndrome exhibiting features of systemic lupus erythematosus. Positional mapping of the disease-associated locus revealed a lesion in Rasgrp1 that prevented the translation of the RasGRP1 protein. T cells from these mice failed to activate Ras or proliferate vigorously following antigen encounter and showed defects in positive selection. Peripheral RasGRP1lag T cells spontaneously adopted a memory phenotype and were able to transfer disease to lymphopenic recipient mice. CD4+ T cells accumulated in the lymphoid tissues of older RasGRP1lag mice and were resistant to activation-induced cell death. RasGRP1lag B cells were functionally normal, but activated B cells were detected in older mice, as were autoantibodies directed against self-antigens. Our findings indicate that Ras signaling pathways are required to maintain T cell tolerance and to prevent autoimmune disease.Entities:
Mesh:
Substances:
Year: 2003 PMID: 12932358 DOI: 10.1016/s1074-7613(03)00209-7
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745