JOINT-DERIVED T-CELLS IN RHEUMATOID-ARTHRITIS PROLIFERATE TO ANTIGENS PRESENT IN AUTOLOGOUS SYNOVIAL-FLUID

被引:0
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作者
MAURICE, MM
RES, PCM
LEOW, A
VANHALL, T
DAHA, MR
STRUYK, L
VANDENELSEN, P
BREEDVELD, FC
VERWEIJ, CL
机构
[1] UNIV LEIDEN HOSP,DEPT RHEUMATOL,2300 RC LEIDEN,NETHERLANDS
[2] UNIV LEIDEN HOSP,DEPT NEPHROL,2300 RC LEIDEN,NETHERLANDS
[3] UNIV LEIDEN HOSP,DEPT IMMUNOHAEMATOL & BLOODBANK,2300 RC LEIDEN,NETHERLANDS
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中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
The histopathological features of rheumatoid joint-inflammation suggest that an antigen-driven activation of T cells plays a central role in the onset and/or perpetuation of the inflammatory process. However, the disease-associated antigens responsible for the activation of T cells in the joint are unknown. In this project we study the response of IL-2 expanded T-cell lines from the synovial fluid (SF) of rheumatoid arthritis (RA) patients against autologous SF in a proliferation assay. Sixteen out of 32 RA patients were found to have CD4+ T cells that proliferate in response to autologous SF. The presence of T cells able to respond to SF antigens in inflamed joints suggests that these T cells play an active role in the pathogenesis of RA. T cell clones reactive to autologous SF were isolated from SF-derived T-cell lines of two RA patients. All clones were of the CD4(+), CD8(-), alpha/beta(+) phenotype. SF-reactivity of T-cell clones from the DR4/DR12-positive RA patient was restricted via the Dw4 subtype of DR4. SF reactivity of T cells of the DR12/DR15 patient was DP-restricted. Some of the T-cell clones responded specifically to autologous and not to allogeneic SF, whereas others revealed responsiveness against a limited number of allogeneic SF samples. The (restricted) specificity of T cells towards autologous SF antigens is indicative for heterogeneity of the epitopes recognized and argues against ubiquitous nonpolymorphic joint constituents as the relevant antigens recognized by the SF-autoreactive T cells.
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页码:169 / 177
页数:9
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