Previous studies have illustrated the importance of T cellsbearing ß TCRs in the induction and development ofcollagen induced arthritis (CIA) in mice. However, the scopeof TCR usage in CIA has yet to be clearly defined. Given theinherent diversity of the TCR repertoire, the relative flexibilityof the arthritogenic TCR repertoire specific for type II collagen(CII) is not clear. Therefore, we chose to examine the influenceof a highly skewed TCR repertoire on CIA. Arthritis susceptibleB10.Q (H-2
q) mice were mated with C57L (H-2
b) animals expressingan ovalbuminspecific V
ß8.2 TCR transgene (Tg) andTg
+ offspring were further backcrossed to B10.Q. HomozygousH-2
a/q, V
ß8.2 Tg
+ mice displayed a high level of V
ß8.2
+T cells in peripheral blood. However, expression of some endogenousV
ß TCR, such as V
ß14, was still detected.Upon immunization with bovine CII in adjuvant, V
ß8.2Tg
+ mice were highly resistant to CIA when compared with Tg
–littermates. Analysis of sera demonstrated a marked reductionin antibody specific for homologous mouse CII as well as heterologousbovine CII in Tg
+ animals. Interestingly, V
ß8.2 Tg
+mice still mounted good antibody responses following immunizationwith human thyroglobulin, indicating that the skewed TCR repertoireaffected anti-CII but not antithyroglobulin responses. Thus,our findings show that constraints placed on the TCR repertoireInhibit pathogenic responses against CII and suggest that inH-2
q mice the arthritogenlc TCR repertoire bears only limitedflexibility.
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