Anti-ribosomal and 'P-peptide'-specific autoantibodies bind to T lymphocytes

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Abstract

Patients with systemic lupus erythematous (SLE) frequently have anti- lymphocyte autoantibodies, some of which also bind to surfaces of neurons. Since anti-ribosomal P protein autoantibodies (anti-P) from SLE patients also bind to surfaces of neurons, we hypothesized that anti-P are anti-lymphocyte antibodies. A panel of human T lymphocytes was evaluated for anti-P binding by indirect immuno-fluorescence. Affinity-purified anti-ribosomal antibodies were used as a source of anti-P. These autoantibodies bound to the surfaces of all transformed T cell lines tested. This binding was not mediated by Fe receptors. It was inhibitable by ribosomes. Anti-P bound to circulating T lymphocytes from healthy adults and children. They also bound to thymocytes and cord blood T cells from normal neonates. Circulating T cells from SLE patients with anti-P bound less anti-P than cells from healthy controls. Two patients were studied on multiple occasions. The capacity of their T cells to bind anti-P correlated inversely with titres of anti-ribosomal antibodies. Anti-ribosomal antibodies, other than anti-P, also appear to bind to T cells. The surface of T cells, contains a protein with the size and antigenicity of the ribosomal P protein, P0. We conclude that anti-ribosomal antibodies are a subset of anti-lymphocyte autoantibodies. Their possible role in the pathogenesis of lymphopenia or lymphocyte dysfunction in SLE has to be defined in further studies.

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Stafford, H. A., Chen, A. E., Anderson, C. J., Paul, A. G. A., Wyatt, E. L., Lee, L. A., & Neas, B. R. (1997). Anti-ribosomal and ’P-peptide’-specific autoantibodies bind to T lymphocytes. Clinical and Experimental Immunology, 109(1), 12–19. https://doi.org/10.1046/j.1365-2249.1997.3691261.x

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