CXCL13 as a biomarker in the diagnostics of European lyme Neuroborreliosis - A prospective multicentre study in Austria

Author:

Waiß Christoph1ORCID,Ströbele Barbara2,Graichen Uwe3ORCID,Klee Sascha3,Gartlehner Joshua1,Sonntagbauer Estelle1,Hirschbichler Stephanie1,Tinchon Alexander1,Kacar Emrah4,Wuchty Bianca5,Novotna Bianka5,Kühn Zofia6,Sellner Johann5ORCID,Struhal Walter4,Bancher Christian7,Schnider Peter6,Asenbaum-Nan Susanne8,Oberndorfer Stefan19

Affiliation:

1. Department of Neurology, Karl-Landsteiner-Private University of Health Sciences (KLPU), University Hospital St. Poelten, St Polten, Austria

2. Institute of Hygiene and Microbiology, Karl-Landsteiner-Private University of Health Sciences (KLPU), University Hospital St. Poelten, St Polten, Austria

3. Department for Health Sciences, Biostatistics and Data Science, Karl-Landsteiner-Private University of Health Sciences (KLPU), Krems an der Donau, Austria

4. Department of Neurology, Karl-Landsteiner-Private University of Health Sciences (KLPU), University Hospital Tulln, Tulln, Austria

5. Department of Neurology, Hospital Mistelbach, Mistelbach, Austria

6. Department of Neurology, Hospital Wr. Neustadt, Wiener Neustadt, Austria

7. Department of Neurology, Hospital Horn, Horn, Austria

8. Department of Neurology, Hospital Amstetten, Amstetten, Austria

9. Karl Landsteiner Institute for Neurology and Neuropsychology St. Poelten, Krems an der Donau, Austria

Abstract

Background ‘Definite Neuroborreliosis (NB)’ is diagnosed with the presence of NB-specific symptoms, cerebrospinal fluid (CSF) pleocytosis and an elevated Borrelia Burgdorferi antibody index. However, some diagnostic uncertainties exist. The B-cell chemokine CXCL13 represents an emerging biomarker for the diagnosis and treatment of NB because its intrathecal concentration rises prior to the Borrelia antibody index and drops rapidly after antibiotic therapy. Nevertheless, due to lacking prospective data, a definite CXCL13 cut-off for the diagnosis of NB is still pending. Objective Definition of a CSF CXCL13 cut-off for the diagnosis of acute and untreated NB in a prospective study setting. Design and methods This multicentre prospective study involved 6 neurological departments treating patients in the Lower Austria district (1.7 million inhabitants). The controls were patients scheduled for a spinal tap but not clinically diagnosed with NB. Demographic data, clinical characteristics and blood counts, as well as inflammatory CSF values and CSF CXCL13-concentration were analysed. Results We recruited 440 adult patients, of whom 42 have been diagnosed as having an acute and untreated ‘definite NB’. Three hundred ninety-eight patients were assigned to the control group. The median intrathecal CXCL13 concentration was 2384 pg/ml for patients with NB and 0 pg/ml for controls. The difference was highly statistically significant ( P ≤ .001). A CSF CXCL13 cut-off of 271 pg/ml resulted in a sensitivity of 95.2% and a specificity of 97.2% for the confirmation or exclusion of NB. Conclusion Based on our results, we propose a CSF CXCL13 cut-off of 271 pg/ml with Euroimmun-Elisa for the diagnosis of acute and untreated NB. Due to its high sensitivity and specificity, CXCL13 is a strong candidate biomarker for routine NB assessment, especially in clinically unclear cases.

Funder

Forschungsimpulse

Federal Government of Lower Austria

Publisher

SAGE Publications

Reference38 articles.

1. Cerebrospinal fluid CXCL13 in Lyme neuroborreliosis and asymptomatic HIV infection

2. The NeBoP score - a clinical prediction test for evaluation of children with Lyme Neuroborreliosis in Europe

3. Rauer SKSea, Neuroborreliose, S3-Leitlinie. Deutsche Gesellschaft für Neurologie (Hrsg.), Leitlinien für Diagnostik und Therapie in der Neurologie, 2018.

4. The chemokine CXCL13 in acute neuroborreliosis

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