Literature DB >> 14988508

Structural availability influences the capacity of autoantigenic epitopes to induce a widespread lupus-like autoimmune response.

Micah T McClain1, Carol S Lutz, Kenneth M Kaufman, Ofer Z Faig, Timothy F Gross, Judith A James.   

Abstract

A subset of lupus patients with severe nephritis and anti-nRNP reactivity produces autoantibodies primarily against two major epitopes of the nRNP A (also known as U1A) protein. These sequences span amino acids 44-56 (A3) and amino acids 103-115 (A6). These two epitopes represent structurally different regions of the protein, as both epitopes are located on the surface, but the A6 epitope is functionally masked in vivo by binding between nRNP A and the U1 RNA. Rabbits were immunized with either the A3 or A6 peptides constructed on a branching polylysine backbone. Rabbits immunized with each of these peptides first developed antibodies directed against the peptide of immunization. With boosting, the immune response of rabbits immunized with the A3 peptide spread to other common antigenic regions of nRNP A. These regions of nRNP A bound by A3 immunized rabbits are very similar to common epitopes in human systemic lupus erythematosus. These A3 immunized rabbits also develop antibodies to common antigenic regions of nRNP 70K, nRNP C, Sm B/B', and Sm D1 proteins, as well as clinical symptoms of systemic lupus erythematosus such as leukopenia and renal insufficiency. On the other hand, rabbits immunized with the A6 peptide only develop antibodies to the peptide of immunization. Anti-A3, but not anti-A6, antibodies are capable of immunoprecipitating native small nuclear ribonucleoprotein complexes. Immunization with the A3 peptide of nRNP A (a surface epitope), but not the A6 peptide (masked), induces an extensive, varied immune response against multiple small nuclear ribonucleoprotein autoantigens similar to that seen in human systemic lupus erythematosus.

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Year:  2004        PMID: 14988508      PMCID: PMC373500          DOI: 10.1073/pnas.0306267101

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  42 in total

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Authors:  J A James; J B Harley
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Authors:  M Mattioli; M Reichlin
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4.  Selective small antigenic structures are capable of inducing widespread autoimmunity which closely mimics the humoral fine specificity of human SLE.

Authors:  M T McClain; R H Scofield; B T Kurien; T F Gross; J A James
Journal:  Scand J Immunol       Date:  2002-10       Impact factor: 3.487

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Authors:  T P Gordon; G Kinoshita; D Cavill; C Keech; A Farris; K Kaufman; J McCluskey; A Purcell
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8.  Temporal shifts from Sm to ribonucleoprotein reactivity in systemic lupus erythematosus.

Authors:  D E Fisher; W H Reeves; R Wisniewolski; R G Lahita; N Chiorazzi
Journal:  Arthritis Rheum       Date:  1985-12

9.  Novel specificity of anti-U1A autoimmune patient sera.

Authors:  O Z Faig; C S Lutz
Journal:  Scand J Immunol       Date:  2003-01       Impact factor: 3.487

10.  Autoantibodies against small nuclear ribonucleoprotein components.

Authors:  W J van Venrooij
Journal:  J Rheumatol Suppl       Date:  1987-06
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4.  Identification of T-cell epitopes on U1A protein in MRL/lpr mice: double-negative T cells are the major responsive cells.

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6.  Epstein Barr virus nuclear antigen 1 (EBNA-1) peptides recognized by adult multiple sclerosis patient sera induce neurologic symptoms in a murine model.

Authors:  Neelakshi R Jog; Micah T McClain; Latisha D Heinlen; Timothy Gross; Rheal Towner; Joel M Guthridge; Robert C Axtell; Gabriel Pardo; John B Harley; Judith A James
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7.  Most nuclear systemic autoantigens are extremely disordered proteins: implications for the etiology of systemic autoimmunity.

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9.  B cell epitope of human cytomegalovirus phosphoprotein 65 (HCMV pp65) induced anti-dsDNA antibody in BALB/c mice.

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