DRB1*0402 protects while DRB1*0401 is permissive for inducing collagen-induced arthritis in transgenic mice (130.45)

Abstract

Abstract DRB1*0401 has been associated with predisposition to rheumatoid arthritis while DRB1*0402 is associated with resistance. We have generated transgenic mice lacking endogenous H2-A and E molecules (AEo) but expressing DRB1*0401 or DRB1*0402 molecules. All transgenic mice expressed functional DR molecules which could positively and negatively select various Vβ T cell repertoire profile. Transgenic mice were studied in vivo for induction of arthritis following immunization with type II collagen. DRB1*0401 mice are susceptible to collagen-induced arthritis while DRB1*0402 mice are resistant. Presence of DR4 leads to arthritis predominantly in female mice. CIA susceptible AEo.DQ8 mice have been shown to develop arthritis without a gender bias. However, AEo mice expressing DRB1*0401.DQ8 develop arthritis in female mice with a ratio of 3F:1M, similar to that in humans. DRB1*0402 mice did not show any defect in humoral response though they demonstrated a lower cellular response to CII and an increased activation-induced cell death compared to susceptible mice. In vitro T cell response with superantigen staphylococcal enterotoxin B and Concovalin A showed that DRB1*0402 mice are not defective in generating T cell response. The resistant mice showed an increased cell death in thymus suggesting deletion of autoreactive T cells at thymic level might be one reason for protection. The data suggest that DRB1 polymorphism lead to selection of TCR in thymus thus controlling the selection of autoreactive T cells available in periphery. Thus these transgenic mice may be useful to study the reasons for gender-bias observed in human patients develop therapeutic strategies.