Immunoglobulin epitope spreading and autoimmune disease after peptide immunization: Sm B/B'-derived PPPGMRPP and PPPGIRGP induce spliceosome …

JA James, T Gross, RH Scofield… - The Journal of …, 1995 - rupress.org
The Journal of experimental medicine, 1995rupress.org
Autoantibodies from many patients with systemic lupus erythematosus bind the Sm
autoantigen B/B'polypeptide. The binding of serial serum specimens to the 233 overlapping
octapeptides of Sm B/B'have shown that of the B/B'-derived octapeptides, PPPGMRPP and
PPPGIRGP are early targets of the autoimmune response in some lupus patients. Rabbits
immunized with PPPGMRPP and PPPGIRGP develop antibodies which not only bind these
octapeptides, but also subsequently bind many other octapeptides of Sm B/B'. Eventually …
Autoantibodies from many patients with systemic lupus erythematosus bind the Sm autoantigen B/B' polypeptide. The binding of serial serum specimens to the 233 overlapping octapeptides of Sm B/B' have shown that of the B/B'-derived octapeptides, PPPGMRPP and PPPGIRGP are early targets of the autoimmune response in some lupus patients. Rabbits immunized with PPPGMRPP and PPPGIRGP develop antibodies which not only bind these octapeptides, but also subsequently bind many other octapeptides of Sm B/B'. Eventually, the rabbits immunized with one octapeptide develop autoantibodies that bind other spliceosomal proteins including D, 70K, A, and C. Any mechanisms that operate to maintain tolerance or anergy for the spliceosome are thus overcome. Features considered typical of human systemic lupus erythematosus are also found in these peptide-immunized animals, such as antinuclear antibodies, anti-Sm precipitins, anti-double-stranded DNA, thrombocytopenia, seizures, and proteinuria. This disease model provides access to a mechanism for the development of humoral autoimmunity and may provide a basis to explain the immunopathogenesis of lupus in humans.
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