Measurement of antinuclear antibodies and their fine specificities: time for a change in strategy?

CTD公司 IIf公司 医学 抗核抗体 自身抗体 结缔组织病 内科学 抗体 免疫学 病理 疾病 自身免疫性疾病 海洋学 地质学
作者
Henny G. Otten,Walter J. Brummelhuis,Ruth Fritsch‐Stork,Helen L. Leavis,Bram W. Wisse,J.M. van Laar,Ronald H. W. M. Derksen
出处
期刊:PubMed 卷期号:35 (3): 462-470 被引量:13
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The current strategy for antinuclear antibody (ANA) analysis involves screening for presence with a subsequent detailed analysis of their specificity. The aim of this study is to compare the clinical and financial efficacy of this strategy between different commercial tests in a large cohort of unselected patients.In all consecutive 1030 patients associations were defined between results from different ANA test systems and the pre-test probability for connective tissue disease (CTDs). Test systems were used for screening (ANA-IIF vs. CTD screen) and definition of their fine specificity (profile 3 line blot vs. CTD single analytes).Positive ANA-IIF and/or CTD screen results were found in 304 sera. Further analysis for ANA-specificity by profile 3 line blot and CTD single analytes showed 86 discrepant results of which more than a third are clinically relevant, with the CTD single analyte assay performing better than the line blot in supporting or confirming the presence of a CTD. Autoantigens present in one test but absent in the other were of minor practical use. The ANA screening and identification strategies currently employed are not cost-effective as 83% of tests were performed in order to find specific autoantibodies in patients without the fitting clinical signs or symptoms. This causes many unexpected positive results and subsequent confusion with regard to interpretation.We advocate that some autoantigens should be excluded from the line blot and CTD assays and propose the use of a cost-effective and selective ANA specificity testing purely based on clinical guidance.

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