4.7 Article

Functional network dynamics revealed by EEG microstates reflect cognitive decline in amyotrophic lateral sclerosis

Journal

HUMAN BRAIN MAPPING
Volume -, Issue -, Pages -

Publisher

WILEY
DOI: 10.1002/hbm.26536

Keywords

cognitive-behavioural impairments; EEG microstates; motor neuron disease; neurodegeneration; resting-state EEG; temporal dynamics; transition probabilities

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Recent EEG studies have found that analyzing EEG microstates can help differentiate ALS from control groups and detect signal abnormalities in ALS. The properties of microstates, such as coverage, occurrence, duration, and transition probabilities, show differences between ALS and control groups and correlate with functional decline in limbs and cognitive decline. Microstate characteristics also change over the course of the disease and may reflect abnormalities within sensory and higher-order networks. Furthermore, microstate properties can predict symptom progression in those with cognitive impairments.
Recent electroencephalography (EEG) studies have shown that patterns of brain activity can be used to differentiate amyotrophic lateral sclerosis (ALS) and control groups. These differences can be interrogated by examining EEG microstates, which are distinct, reoccurring topographies of the scalp's electrical potentials. Quantifying the temporal properties of the four canonical microstates can elucidate how the dynamics of functional brain networks are altered in neurological conditions. Here we have analysed the properties of microstates to detect and quantify signal-based abnormality in ALS. High-density resting-state EEG data from 129 people with ALS and 78 HC were recorded longitudinally over a 24-month period. EEG topographies were extracted at instances of peak global field power to identify four microstate classes (labelled A-D) using K-means clustering. Each EEG topography was retrospectively associated with a microstate class based on global map dissimilarity. Changes in microstate properties over the course of the disease were assessed in people with ALS and compared with changes in clinical scores. The topographies of microstate classes remained consistent across participants and conditions. Differences were observed in coverage, occurrence, duration, and transition probabilities between ALS and control groups. The duration of microstate class B and coverage of microstate class C correlated with lower limb functional decline. The transition probabilities A to D, C to B and C to B also correlated with cognitive decline (total ECAS) in those with cognitive and behavioural impairments. Microstate characteristics also significantly changed over the course of the disease. Examining the temporal dependencies in the sequences of microstates revealed that the symmetry and stationarity of transition matrices were increased in people with late-stage ALS. These alterations in the properties of EEG microstates in ALS may reflect abnormalities within the sensory network and higher-order networks. Microstate properties could also prospectively predict symptom progression in those with cognitive impairments.

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