TCR1+ large granular lymphocyte proliferation in rheumatoid arthritis |
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Authors: | J. G. Kuipers R. Jacobs A. Kemper H. Zeidler R. E. Schmidt |
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Affiliation: | (1) Department of Clinical Immunology, Hannover Medical School, Konstanty-Gutschow-Strasse 8, D-30625 Hannover, Germany;(2) Department of Rheumatology, Hannover Medical School, Hannover, Germany |
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Abstract: | The T-lymphoproliferative syndrome is characterized by a proliferation of large granular lymphocytes (LGL). It is often associated with neutropenia, and in 30% of cases with rheumatoid arthritis (RA). Phenotypic analysis has demonstrated that in most cases of RA with T-proliferative disease, the LGL represent T cells with a clonal rearrangement of the / T cell receptor (TCR2). Here, three patients with / TCR1+ LGL proliferation suffering from long-standing arthritis and neutropenia are described. The first patient with RA showed an expansion of a heterogeneous CD2+ CD16+ CD56- LGL population, of which 30% coexpressed TCR1 with V1 rearrangement. The second patient with ankylosing spondylitis and RA was suffering from proliferation of TCR1+ (V9-, V1-), CD2+ CD16- CD56- LGL with low coexpression of CD8. The third patient with RA was suffering from a proliferation of TCR1+ (V1+, V9-) CD4- CE8- CD16- CD56- lymphocytes. On the basis of these unusual findings, the pathogenetic role of TCR1+ T cells in RA is discussed. |
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Keywords: | T /content/l8360115255j0745/xxlarge947.gif" alt=" gamma" align=" MIDDLE" BORDER=" 0" >-lymphoproliferative syndrome Large granular lymphocytes Rheumatoid arthritis /content/l8360115255j0745/xxlarge945.gif" alt=" agr" align=" BASELINE" BORDER=" 0" >/ /content/l8360115255j0745/xxlarge946.gif" alt=" beta" align=" MIDDLE" BORDER=" 0" > T cell receptor (TCR2) /content/l8360115255j0745/xxlarge947.gif" alt=" gamma" align=" MIDDLE" BORDER=" 0" >/ /content/l8360115255j0745/xxlarge948.gif" alt=" delta" align=" BASELINE" BORDER=" 0" > TCR1+ |
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