Abstract
Objective
To evaluate antinuclear antibody (ANA) tests in established cases of systemic lupus ery-thematosus (SLE) and rheumatoid arthritis (RA) by indirect immunofluorescence microscopy (F-ANA) and enzyme-immunoassays detecting antinucleosomal antibodies (ANSA-EIA).
Methods
Sera from 50 patients with SLE and 65 patients with RA were analyzed regarding abnormal concentrations of F-ANA (serum dilution ≥ 1:200 = 95th percentile among 300 healthy blood donors). The sera were also analyzed with 2 commercial ANSA-EIA kits.
Results
An abnormal F-ANA titer occurred in 76% of the SLE sera compared to 23% in RA, and was not related to present use of antirheumatic drugs. At dilution 1:50, 84% of the SLE sera were F-ANA-positive compared to 20% of healthy women. Forty percent and 56%, respectively, of the SLE sera tested positive in the 2 ANSA-EIA kits. By the most sensitive assay, 96% of the ANSA-positive SLE sera produced a homogenous (chromosomal) F-ANA staining pattern compared to 18% of the ANSA-negative SLE sera. Ten of the 15 F-ANA-positive RA sera (63%) generated homogenous F-ANA staining and 13 (20%) tested positive in the most sensitive ANSA-EIA, but with no correlation to the F-ANA staining pattern.
Conclusion
The sensitivity of F-ANA at an abnormal titer was surprisingly low (76%) in established cases of SLE. ANSA occurred in 56% of the SLE sera, but also in a fair number (20%) of RA sera. Practically all ANSA-positive SLE sera were identified by chromosomal F-ANA staining. We conclude that the antigen-specific antinucleosomal EIA does not have high enough diagnostic specificity to justify use of this analysis for routine diagnostic purposes.
Key Indexing Terms:Footnotes
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C. Sjöwall, MD, PhD, Division of Rheumatology; M. Sturm, MD, Division of Rheumatology, Division of Clinical Immunology; C. Dahle, MD, PhD, Division of Clinical Immunology, Faculty of Health Science, Linköping University; A.A. Bengtsson, MD, PhD; A. Jönsen, MD, PhD; G. Sturfelt, MD, PhD, Department of Rheumatology, University Hospital of Lund; T. Skogh, MD, PhD, Division of Rheumatology, Faculty of Health Science, Linköping University.
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Dr. Sjöwall and Dr. Sturm contributed equally to the study.
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Supported by grants from the Swedish Research Council (grants K2006-74X-14594-04-03 and 13489), The Swedish Society Against Rheumatism, King Gustaf V 80-year Foundation, the Siv Olsson and Karin Svensson Foundations, the County Council of Östergötland, Österlund’s Foundation, and Greta and Johan Kock’s Foundation.
- Accepted for publication May 26, 2008.