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Immunological and Biochemical Characterization of Streptococcal Pyrogenic Exotoxins I and J (SPE-I and SPE-J) from Streptococcus pyogenes

2001; American Association of Immunologists; Volume: 166; Issue: 11 Linguagem: Inglês

10.4049/jimmunol.166.11.6711

1550-6606

Thomas Proft, Vickery L. Arcus, Vanessa Handley, Edward N. Baker, John D. Fraser,

Inflammasome and immune disorders

Abstract Recently, we described the identification of novel streptococcal superantigens (SAgs) by mining the Streptococcus pyogenes M1 genome database at Oklahoma University. Here, we report the cloning, expression, and functional analysis of streptococcal pyrogenic exotoxin (SPE)-J and another novel SAg (SPE-I). SPE-I is most closely related to SPE-H and staphylococcal enterotoxin I, whereas SPE-J is most closely related to SPE-C. Recombinant forms of SPE-I and SPE-J were mitogenic for PBL, both reaching half maximum responses at 0.1 pg/ml. Evidence from binding studies and cell aggregation assays using a human B-lymphoblastoid cell line (LG-2) suggests that both toxins exclusively bind to the polymorphic MHC class II β-chain in a zinc-dependent mode but not to the generic MHC class II α-chain. The results from analysis by light scattering indicate that SPE-J exists as a dimer in solution above concentrations of 4.0 mg/ml. Moreover, SPE-J induced a rapid homotypic aggregation of LG-2 cells, suggesting that this toxin might cross-link MHC class II molecules on the cell surface by building tetramers of the type HLA-DRβ–SPE-J–SPE-J–HLA-DRβ. SPE-I preferably stimulates T cells bearing the Vβ18.1 TCR, which is not targeted by any other known SAg. SPE-J almost exclusively stimulates Vβ2.1 T cells, a Vβ that is targeted by several other streptococcal SAgs, suggesting a specific role for this T cell subpopulation in immune defense. Despite a primary sequence diversity of 51%, SPE-J is functionally indistinguishable from SPE-C and might play a role in streptococcal disease, which has previously been addressed to SPE-C.