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CCL1 and IL-2Ra differentiate Tuberculosis disease from latent infection Irrespective of HIV infection in low TB burden countries - 21/09/21

Doi : 10.1016/j.jinf.2021.07.036 
Bih H. Chendi a, b, Hallgeir Tveiten c, Candice I. Snyders b, Kristian Tonby a, d, Synne Jenum d, Susanne Dam Nielsen e, Malene Hove-Skovsgaard e, Gerhard Walzl b, Novel N. Chegou b, 1, Anne M Dyrhol-Riise a, d, 1,
a Institute of Clinical Medicine, Faculty of Medicine, University of Oslo, Oslo, Norway 
b DSI-NRF Centre of Excellence for Biomedical TB Research, South African MRC Centre for TB Research, Division of Molecular Biology and Human Genetics, Department of Biomedical Sciences, Faculty of Medicine and Health Sciences, Stellenbosch University, Cape Town, South Africa 
c Department of Pulmonary Medicine, Oslo University Hospital, Oslo, Norway 
d Department of Infectious Diseases, Oslo University Hospital, Oslo, Norway 
e Department of Infectious Diseases, University of Copenhagen, Rigshospitalet, Denmark 

Corresponding author at: Department of Infectious Diseases, Oslo University Hospital., Postal address: postbox 4952, Nydalen, 0424 Oslo, Norway.Department of Infectious Diseases, Oslo University Hospital.Postal address: postbox 4952, NydalenOslo0424Norway

Highlights

Selected plasma host biomarkers were evaluated for accuracies in differentiating tuberculosis (TB) disease from latent infection (LTBI) in HIV uninfected and infected individuals in TB low burden settings.
CCL1 and IL-2Ra were the most accurate single biomarker in differentiating TB from LTBI irrespective of HIV co-infection.
Biosignatures including 2–5 biomarkers discriminated TB from LTBI with high accuracies.
CCL1 and IL-2Ra should be included together with other selected biomarkers in larger confirmatory studies to identify biosignatures for global use in TB diagnostics.

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Summary

Objectives: To evaluate the performance of selected host immunological biomarkers in differentiating tuberculosis (TB) disease from latent TB infection (LTBI) in HIV uninfected and infected individuals enrolled in TB low-burden countries.

Design: Participants with TB disease (N = 85) and LTBI (N = 150) were recruited from prospective cohorts at hospitals in Norway and Denmark. Plasma concentrations of 54 host markers were assessed by Luminex multiplex immunoassays. Using receiver operator characteristic curves and general discriminant analysis, we determined the abilities of individual and combined biomarkers to discriminate between TB disease and LTBI including when patients were stratified according to HIV infection status.

Results: Regardless of the groups compared, CCL1 and IL-2Ra were the most accurate single biomarkers in differentiating TB disease from LTBI. Regardless of HIV status, a 4-marker signature (CCL1+RANTES+CRP+MIP-1α) derived from a training set (n = 155) differentiated TB disease from LTBI in the test set (n = 67) with a sensitivity of 56.0% (95% CI, 34.9–75.6) and a specificity of 85.7% (95% CI, 71.5–94.6). A 5-marker signature derived from the HIV uninfected group (CCL1+RANTES+MIP-1α+procalcitonin+IP-10) performed in HIV-infected individuals with a sensitivity of 75.0% and a specificity of 96.7% after leave-one-out cross validation. A 2-marker signature (CCL1+TNF-α) identified in HIV-infected persons performed in HIV-uninfected with a sensitivity and specificity of 66.7% and 100% respectively in the test set.

Conclusions: Plasma CCL1 and IL-2Ra have potential as biomarkers for differentiating TB disease from LTBI in low TB burden settings unaffected by HIV infection. Combinations between these and other biomarkers in bio-signatures for global use warrant further exploration.

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Keywords : TB disease, Latent TB infection, Diagnostics, Host biomarkers, Biosignatures, CCL1, IL-2Ra, HIV, Low endemic countries


Plan


 Running title: Host biomarkers in TB and LTBI.


© 2021  Publié par Elsevier Masson SAS.
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Vol 83 - N° 4

P. 433-443 - octobre 2021 Retour au numéro
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