Systemic lupus erythematosus (SLE) is an autoimmune disease characterized by the emergence of autoreactive Tcells. Humans and mice with SLE have reduced numbers of CD1d-restricted invariant natural killer T (iNKT) cells, suggesting a key role for these cells in its immunopathogenesis. This subset uses an invariant TCR constituted by Va14Ja281 chains paired with some Vb domains. The regulatory role for iNKT cells in non-autoimmune mice was suggested by our previous results showing that aged Ja281 knockout (KO) mice produce anti-dsDNA. Here we show that old Ja281 KO mice have proteinuria and antibodies against dsDNA and cardiolipin. Histological analysis of Ja281 KO mice revealed glomeruli damage and deposition of C3c and IgG, mainly of the IgG3 subclass. In spleens of aged Ja281 KO mice there is an increase of activated marginal zone B cells. The evolution of lesions may depend on the age-associated increase of autoantibodies production, preferentially IgG3, mainly secreted by marginal zone B cells. Our results provide the first evidence of a lupus-like syndrome in nonautoimmune mice, supporting an age-related immunoregulatory role of Ja281+ cells, probably associated with the activation of marginal zone B cells.
Immunoregulatory role of Jalpha281 T cells in aged mice developing lupus-like nephritis
Domenica Russo;
2007
Abstract
Systemic lupus erythematosus (SLE) is an autoimmune disease characterized by the emergence of autoreactive Tcells. Humans and mice with SLE have reduced numbers of CD1d-restricted invariant natural killer T (iNKT) cells, suggesting a key role for these cells in its immunopathogenesis. This subset uses an invariant TCR constituted by Va14Ja281 chains paired with some Vb domains. The regulatory role for iNKT cells in non-autoimmune mice was suggested by our previous results showing that aged Ja281 knockout (KO) mice produce anti-dsDNA. Here we show that old Ja281 KO mice have proteinuria and antibodies against dsDNA and cardiolipin. Histological analysis of Ja281 KO mice revealed glomeruli damage and deposition of C3c and IgG, mainly of the IgG3 subclass. In spleens of aged Ja281 KO mice there is an increase of activated marginal zone B cells. The evolution of lesions may depend on the age-associated increase of autoantibodies production, preferentially IgG3, mainly secreted by marginal zone B cells. Our results provide the first evidence of a lupus-like syndrome in nonautoimmune mice, supporting an age-related immunoregulatory role of Ja281+ cells, probably associated with the activation of marginal zone B cells.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.