Evaluation of the fully automated LIAISON®XL chemiluminescence analyzer for QuantiFERON®-CMV testing in transplant recipients

Sarah Mafi; Sophie Alain; Sébastien Hantz

doi:10.1016/j.jcv.2023.105550

Evaluation of the fully automated LIAISON®XL chemiluminescence analyzer for QuantiFERON®-CMV testing in transplant recipients

J Clin Virol. 2023 Sep:166:105550. doi: 10.1016/j.jcv.2023.105550. Epub 2023 Jul 20.

Authors

Sarah Mafi¹, Sophie Alain², Sébastien Hantz³

Affiliations

¹ French National Reference Center for Herpesviruses, Bacteriology, Virology, Hygiene Department, CHU Limoges, F-87000 Limoges, France; INSERM, RESINFIT, U1092, F-87000, Limoges, France. Electronic address: sarah.mafi@unilim.fr.
² French National Reference Center for Herpesviruses, Bacteriology, Virology, Hygiene Department, CHU Limoges, F-87000 Limoges, France; INSERM, RESINFIT, U1092, F-87000, Limoges, France.
³ French National Reference Center for Herpesviruses, Bacteriology, Virology, Hygiene Department, CHU Limoges, F-87000 Limoges, France; INSERM, RESINFIT, U1092, F-87000, Limoges, France. Electronic address: sebastien.hantz@unilim.fr.

PMID: 37527584
DOI: 10.1016/j.jcv.2023.105550

Abstract

Background: Monitoring CMV-specific cell-mediated immunity by the QuantiFERON®-CMV (QF-CMV) may be useful in predicting the risk of CMV infection in transplant recipients (TR).

Objectives: As the QuantiFERON-Tuberculosis (QFT®-Plus) became available on the fully automated LIAISON®XL chemiluminescence (CLIA) analyzer, we evaluated the performance of the QF-CMV on the LIAISON®XL analyzer using the QuantiFERON®-TB Gold Plus reagent.

Study design: Between 2018 and 2022, 81 samples from TR were collected at the Department of Virology of Limoges Hospital, France. Whole blood was collected into each of the three QF-CMV collection tubes: a CMV-antigen tube (QF-Ag), a mitogen tube (QF-Mg) (positive control), and a nil tube (negative control). The QF-CMV was performed on the LIAISON®XL analyzer, and results were compared with those obtained by conventional microplate ELISA.

Results: Intra- and inter-assay coefficients of variation were inferior to 20%. No inter-sample contamination was found (p=0.366). The level of concordance between CLIA and the commonly used ELISA method was 88.9%. Positive and negative percent agreements were 92.3% and 85.7%, respectively, with a very good agreement between assays (κ=0.818). Most discordances were due to indeterminate- or negative-ELISA/positive-CLIA results (most of ELISA results were borderline). Linear regression analyses demonstrated a strong correlation between both assays (QF-Ag Pearson's r=0.978, QF-Mg Pearson's r=0.963). No significant difference was observed in median QF-CMV values between both assays (QF-Ag p=0.776; QF-Mg p=0.853; Mann-Whitney U test). The Bland-Altman plots showed a minor difference in IFN-γ release (QF-Ag -0.069 IU/ml, 95% limits of agreement (LoA): -1.589; 1.451; QF-Mg 0.190 IU/ml, 95% LoA: -2.070; 2.450).

Conclusion: Automated QF-CMV with CLIA is comparable to QF-CMV performed by ELISA with a presumably higher sensitivity for IFN-γ detection that may result in the conversion of samples close to the ELISA cut-off into positive results. Moreover, the use of a random-access analyzer allows to optimize the follow-up of TR.

Keywords: LIAISON®XL; QuantiFERON®-CMV; Transplant recipients.

MeSH terms

Cytomegalovirus Infections*
Humans
Interferon-gamma
Interferon-gamma Release Tests / methods
Luminescence
Transplant Recipients
Tuberculosis* / diagnosis

Substances

Interferon-gamma