Clinical evaluation of autoantibodies to a novel PM/Scl peptide antigen

Anti-PM/Scl antibodies represent a specific serological marker for a subset of patients with scleroderma (Scl) and polymyositis (PM), and especially with the PM/Scl overlap syndrome (PM/Scl). Anti-PM/Scl reactivity is found in 24% of PM/Scl patients and is found in 3–10% of Scl and PM patients. The...

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Autores principales: Mahler, Michael, Raijmakers, Reinout, Dähnrich, Cornelia, Blüthner, Martin, Fritzler, Marvin J
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2005
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1174964/
https://www.ncbi.nlm.nih.gov/pubmed/15899056
http://dx.doi.org/10.1186/ar1729
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author Mahler, Michael
Raijmakers, Reinout
Dähnrich, Cornelia
Blüthner, Martin
Fritzler, Marvin J
author_facet Mahler, Michael
Raijmakers, Reinout
Dähnrich, Cornelia
Blüthner, Martin
Fritzler, Marvin J
author_sort Mahler, Michael
collection PubMed
description Anti-PM/Scl antibodies represent a specific serological marker for a subset of patients with scleroderma (Scl) and polymyositis (PM), and especially with the PM/Scl overlap syndrome (PM/Scl). Anti-PM/Scl reactivity is found in 24% of PM/Scl patients and is found in 3–10% of Scl and PM patients. The PM/Scl autoantigen complex comprises 11–16 different polypeptides. Many of those proteins can serve as targets of the anti-PM/Scl B-cell response, but most frequently the PM/Scl-100 and PM/Scl-75 polypeptides are targeted. In the present study we investigated the clinical relevance of a major alpha helical PM/Scl-100 epitope (PM1-α) using a newly developed peptide-based immunoassay and compared the immunological properties of this peptide with native and recombinant PM/Scl antigens. In a technical comparison, we showed that an ELISA based on the PM1-α peptide is more sensitive than common techniques to detect anti-PM/Scl antibodies such as immunoblot, indirect immunofluorescence on HEp-2 cells and ELISA with recombinant PM/Scl polypeptides. We found no statistical evidence of a positive association between anti-PM1-α and other antibodies, with the exception of known PM/Scl components. In our cohort a negative correlation could be found with anti-Scl-70 (topoisomerase I), anti-Jo-1 (histidyl tRNA synthetase) and anti-centromere proteins. In a multicenter evaluation we demonstrated that the PM1-α peptide represents a sensitive and reliable substrate for the detection of a subclass of anti-PM/Scl antibodies. In total, 22/40 (55%) PM/Scl patients, 27/205 (13.2%) Scl patients and 3/40 (7.5%) PM patients, but only 5/288 (1.7%) unrelated controls, tested positive for the anti-PM1-α peptide antibodies. These data indicate that anti-PM1-α antibodies appear to be exclusively present in sera from PM/Scl patients, from Scl patients and, to a lesser extent, from PM patients. The anti-PM1-α ELISA thus offers a new serological marker to diagnose and discriminate different systemic autoimmune disorders.
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spelling pubmed-11749642005-07-13 Clinical evaluation of autoantibodies to a novel PM/Scl peptide antigen Mahler, Michael Raijmakers, Reinout Dähnrich, Cornelia Blüthner, Martin Fritzler, Marvin J Arthritis Res Ther Research Article Anti-PM/Scl antibodies represent a specific serological marker for a subset of patients with scleroderma (Scl) and polymyositis (PM), and especially with the PM/Scl overlap syndrome (PM/Scl). Anti-PM/Scl reactivity is found in 24% of PM/Scl patients and is found in 3–10% of Scl and PM patients. The PM/Scl autoantigen complex comprises 11–16 different polypeptides. Many of those proteins can serve as targets of the anti-PM/Scl B-cell response, but most frequently the PM/Scl-100 and PM/Scl-75 polypeptides are targeted. In the present study we investigated the clinical relevance of a major alpha helical PM/Scl-100 epitope (PM1-α) using a newly developed peptide-based immunoassay and compared the immunological properties of this peptide with native and recombinant PM/Scl antigens. In a technical comparison, we showed that an ELISA based on the PM1-α peptide is more sensitive than common techniques to detect anti-PM/Scl antibodies such as immunoblot, indirect immunofluorescence on HEp-2 cells and ELISA with recombinant PM/Scl polypeptides. We found no statistical evidence of a positive association between anti-PM1-α and other antibodies, with the exception of known PM/Scl components. In our cohort a negative correlation could be found with anti-Scl-70 (topoisomerase I), anti-Jo-1 (histidyl tRNA synthetase) and anti-centromere proteins. In a multicenter evaluation we demonstrated that the PM1-α peptide represents a sensitive and reliable substrate for the detection of a subclass of anti-PM/Scl antibodies. In total, 22/40 (55%) PM/Scl patients, 27/205 (13.2%) Scl patients and 3/40 (7.5%) PM patients, but only 5/288 (1.7%) unrelated controls, tested positive for the anti-PM1-α peptide antibodies. These data indicate that anti-PM1-α antibodies appear to be exclusively present in sera from PM/Scl patients, from Scl patients and, to a lesser extent, from PM patients. The anti-PM1-α ELISA thus offers a new serological marker to diagnose and discriminate different systemic autoimmune disorders. BioMed Central 2005 2005-04-01 /pmc/articles/PMC1174964/ /pubmed/15899056 http://dx.doi.org/10.1186/ar1729 Text en Copyright © 2005 Mahler et al, licensee BioMed Central Ltd.
spellingShingle Research Article
Mahler, Michael
Raijmakers, Reinout
Dähnrich, Cornelia
Blüthner, Martin
Fritzler, Marvin J
Clinical evaluation of autoantibodies to a novel PM/Scl peptide antigen
title Clinical evaluation of autoantibodies to a novel PM/Scl peptide antigen
title_full Clinical evaluation of autoantibodies to a novel PM/Scl peptide antigen
title_fullStr Clinical evaluation of autoantibodies to a novel PM/Scl peptide antigen
title_full_unstemmed Clinical evaluation of autoantibodies to a novel PM/Scl peptide antigen
title_short Clinical evaluation of autoantibodies to a novel PM/Scl peptide antigen
title_sort clinical evaluation of autoantibodies to a novel pm/scl peptide antigen
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1174964/
https://www.ncbi.nlm.nih.gov/pubmed/15899056
http://dx.doi.org/10.1186/ar1729
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