Abstract

ObjectiveDiseases affecting sensorimotor function impair physical independence. Reliable functional clinical biomarkers allowing early diagnosis or targeting treatment and rehabilitation could reduce this burden. Magnetoencephalography (MEG) non-invasively measures brain rhythms such as the somatomotor ‘rolandic’ rhythm which shows intermittent high-amplitude beta (14–30 Hz) ‘events’ that predict behavior across tasks and species and are altered by sensorimotor neurological diseases. MethodsWe assessed test–retest stability, a prerequisite for biomarkers, of spontaneous sensorimotor aperiodic (1/f) signal and beta events in 50 healthy human controls across two MEG sessions using the intraclass correlation coefficient (ICC). Beta events were determined using an amplitude-thresholding approach on a narrow-band filtered amplitude envelope obtained using Morlet wavelet decomposition. ResultsResting sensorimotor characteristics showed good to excellent test–retest stability. Aperiodic component (ICC 0.77–0.88) and beta event amplitude (ICC 0.74–0.82) were very stable, whereas beta event duration was more variable (ICC 0.55–0.7). 2–3 minute recordings were sufficient to obtain stable results. Analysis automatization was successful in 86%. ConclusionsSensorimotor beta phenotype is a stable feature of an individual’s resting brain activity even for short recordings easily measured in patients. SignificanceSpontaneous sensorimotor beta phenotype has potential as a clinical biomarker of sensorimotor system integrity.

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