Rh. Scofield et al., Immunization of mice with human 60-kd Ro peptides results in epitope spreading if the peptides are highly homologous between human and mouse, ARTH RHEUM, 42(5), 1999, pp. 1017-1024
Objective. Immunization with peptide fragments of autoantigens may lead to
an immune response at both the T and B cell level that is directed not only
at the immunogen, but also at the autoantigen from which the peptide came.
In addition, a complex multicomponent particle may become the target of th
is expanded immune response. The purpose of this study was to determine the
ability of several different peptides from 60-kd Ro to induce expansion of
the immune response to the Ro/La RNP particle.
Methods. We immunized BALB/c mice with 3 different oligopeptides from human
60-kd Ro (or, SSA),
Results, Animals immunized with peptides either identical to or differing b
y only 1 amino acid developed autoimmunity to the entire Ro RNP particle. A
nimals immunized with a human peptide highly divergent from the correspondi
ng mouse sequence developed an immune response to the immunogen only and sh
owed little evidence of epitope spreading. Furthermore, these mice did not
have antibodies that bound the poorly conserved mouse homolog peptide, and
the antibody response to this peptide did not include IgG1.
Conclusion. These data indicate that B lymphocytes specific for the self-pe
ptide that is homologous to the immunogen are a critical determinant for sp
reading of the immune response to other components of self.