Threshold tracking transcranial magnetic stimulation and neurofilament light chain as diagnostic aids in ALS

Author:

Jacobsen Anna B.1ORCID,Bostock Hugh2,Howells James3,Cengiz Bülent4,Samusyte Gintaute56,Koltzenburg Martin27ORCID,Pia Hossein1,Fuglsang‐Frederiksen Anders1,Blicher Jakob8,Obál Izabella8,Andersen Henning9,Tankisi Hatice1ORCID

Affiliation:

1. Department of Clinical Neurophysiology Aarhus University Hospital Aarhus N 8200 Denmark

2. UCL Queen Square Institute of Neurology Queen Square London WC1N 3BG UK

3. Central Clinical School, Faculty of Medicine and Health University of Sydney Sydney NSW 2006 Australia

4. Department of Neurology Gazi University Faculty of Medicine Beşevler 06570 Ankara Turkey

5. Department of Neurology, Medical Academy Lithuanian University of Health Sciences Kaunas 44307 Lithuania

6. Department of Neurology Lithuanian University of Health Sciences Hospital Kauno Klinikos Kaunas 50161 Lithuania

7. Department of Clinical Neurophysiology National Hospital for Neurology and Neurosurgery Queen Square London WC1N 3BG UK

8. Department of Neurology Aalborg University Hospital Aalborg 9000 Denmark

9. Department of Neurology Aarhus University Hospital Aarhus N 8200 Denmark

Abstract

AbstractObjectiveThere is a need for sensitive biomarkers in amyotrophic lateral sclerosis (ALS), to enable earlier diagnosis and to help assess potential treatments. The main objective of this study was to compare two potential biomarkers, threshold‐tracking short‐interval cortical inhibition (T‐SICI), which has shown promise as a diagnostic aid, and neurofilament light chains (NfL).MethodsNinety‐seven patients with ALS (mean age 67.1 ± 11.5 years) and 53 ALS mimics (aged 62.4 ± 12.9) were included. Mean disease duration was 14 months ±14.1. Patients were evaluated with revised ALS functional rating score (ALSFRS‐R), Penn upper motor neuron score (UMNS), muscle strength using the Medical Research Council (MRC) score and examined with T‐SICI, quantitative electromyography (EMG), and NfL measured in spinal fluid.ResultsNfL increased with increasing UMNS (rho = 0.45, p = 8.2 × 10−6) whereas T‐SICI at 2.5 ms paradoxically increased toward normal values (rho = 0.53, p = 1.9 × 10−7). However, these two measures were uncorrelated. Discrimination between ALS patients and mimics was best for NfL (area under ROC curve 0.842, sensitivity 84.9%, specificity 83.5%), compared with T‐SICI (0.675, 39.6%, 91.8%). For the patients with no UMN signs, NfL also discriminated best (0.884, 89.3%, 82.6%), compared with T‐SICI (0.811, 71.4%, 82.6%). However, when combining NfL and T‐SICI, higher AUCs of 0.854 and 0.922 and specificities of 93.8 and 100 were found when considering all patients and patients with no UMN signs, respectively.InterpretationBoth T‐SICI and NfL correlated with UMN involvement and combined, they provided a strong discrimination between ALS patients and ALS mimics.

Funder

Sundhedsvidenskabelige Fakultet, Aarhus Universitet

Lundbeck Foundation

William Demant Fonden

Familien Hede Nielsens Fond

Aage og Johanne Louis-Hansens Fond

Publisher

Wiley

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