Troponin-Specific Autoantibody Interference in Different Cardiac Troponin I Assay Configurations

Author:

Savukoski Tanja1,Engström Emilia1,Engblom Janne2,Ristiniemi Noora1,Wittfooth Saara1,Lindahl Bertil3,Eggers Kai M3,Venge Per3,Pettersson Kim1

Affiliation:

1. Department of Biotechnology, University of Turku, Turku, Finland

2. Turku School of Economics, Turku, Finland

3. Department of Medical Sciences, Clinical Chemistry, University of Uppsala, Uppsala, Sweden

Abstract

AbstractBACKGROUNDAutoantibodies to cardiac troponins (cTnAAb) can interfere with the measurement of cardiac troponin I (cTnI) by immunoassays. The aim of this study was to explore the degree of cTnAAb interference in different cTnI assay configurations.METHODSTernary troponin complex was added into samples (serum or plasma, n = 132, 68% cTnAAb positive) from individuals without known cardiac conditions. The recovery of cTnI was then measured with 6 investigational cTnI assays (2, 3, or 4 antibodies per assay). Three of these assays were then selected for further comparison by use of samples (plasma, n = 210, 33% cTnAAb positive) from non–ST-elevation acute coronary syndrome patients in the FRISC-II (FRagmin/Fast Revascularisation during InStability in Coronary artery disease) cohort. Finally, these results were compared to those obtained with 3 commercial cTnI assays.RESULTSAnalytical recoveries varied widely among the 6 investigational assays. Notably the low recoveries (median 9%) of the midfragment-targeting reference assay were normalized (median 103%) with the use of the 4-antibody assay construct (3 capture, 1 tracer antibody) with only 1 antibody against a midfragment epitope. Reduced analytical recoveries correlated closely with measured autoantibody amounts. cTnI concentrations from cTnAAb-positive patient samples determined with 3 investigational assays confirmed the reduced concentrations expected from the low analytical recoveries. The results from the commercial cTnI assays with antibody selections representative for contemporary assay constructs revealed a similar underestimation (up to 20-fold) of cTnI in cTnAAb-positive samples.CONCLUSIONSA novel cTnI assay deviating from the conventional IFCC-recommended midfragment approach substantially improves cTnI detection in samples containing cTnAAbs.

Funder

Erlangen Graduate School of Advanced Optical Technologies

Publisher

Oxford University Press (OUP)

Subject

Biochemistry (medical),Clinical Biochemistry

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