Heterogeneity of resting-state EEG features in juvenile myoclonic epilepsy and controls

on behalf of the BIOJUME Consortium, Amy Shakeshaft, Petroula Laiou, Eugenio Abela, Ioannis Stavropoulos, Mark P. Richardson, Deb K. Pal, Alessandro Orsini, Alice Howell, Alison Hyde, Alison McQueen, Almu Duran, Alok Gaurav, Amber Collingwood, Amy Kitching, Amy Shakeshaft, Anastasia Papathanasiou, Andrea Clough, Andrew Gribbin, Andrew SwainAnn Needle, Anna Hall, Anna Smith, Anne MacLeod, Asyah Chhibda, Beata Fonferko-Shadrach, Bintou Camara, Boyanka Petrova, Carmel Stuart, Caroline Hamilton, Caroline Peacey, Carolyn Campbell, Catherine Cotter, Catherine Edwards, Catie Picton, Charlotte Busby, Charlotte Quamina, Charlotte Waite, Charlotte West, Ching Ching Ng, Helen Cockerill, Holly Crudgington, Ioannis Stavropoulos, John Davis, Lisa Richardson, Mark Baker, Mark P. Richardson, Deb K. Pal, Matthew Taylor, Muhammad Khan, Rhys Thomas

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4 Citations (Scopus)

Abstract

Abnormal EEG features are a hallmark of epilepsy, and abnormal frequency and network features are apparent in EEGs from people with idiopathic generalized epilepsy in both ictal and interictal states. Here, we characterize differences in the resting-state EEG of individuals with juvenile myoclonic epilepsy and assess factors influencing the heterogeneity of EEG features. We collected EEG data from 147 participants with juvenile myoclonic epilepsy through the Biology of Juvenile Myoclonic Epilepsy study. Ninety-five control EEGs were acquired from two independent studies [Chowdhury et al. (2014) and EU-AIMS Longitudinal European Autism Project]. We extracted frequency and functional network-based features from 10 to 20s epochs of resting-state EEG, including relative power spectral density, peak alpha frequency, network topology measures and brain network ictogenicity: a computational measure of the propensity of networks to generate seizure dynamics. We tested for differences between epilepsy and control EEGs using univariate, multivariable and receiver operating curve analysis. In addition, we explored the heterogeneity of EEG features within and between cohorts by testing for associations with potentially influential factors such as age, sex, epoch length and time, as well as testing for associations with clinical phenotypes including anti-seizure medication, and seizure characteristics in the epilepsy cohort. P-values were corrected for multiple comparisons. Univariate analysis showed significant differences in power spectral density in delta (2-5Hz) (P = 0.0007, hedges' g = 0.55) and low-alpha (6-9Hz) (P = 2.9 × 10-8, g = 0.80) frequency bands, peak alpha frequency (P = 0.000007, g = 0.66), functional network mean degree (P = 0.0006, g = 0.48) and brain network ictogenicity (P = 0.00006, g = 0.56) between epilepsy and controls. Since age (P = 0.009) and epoch length (P = 1.7 × 10-8) differed between the two groups and were potential confounders, we controlled for these covariates in multivariable analysis where disparities in EEG features between epilepsy and controls remained. Receiver operating curve analysis showed low-alpha power spectral density was optimal at distinguishing epilepsy from controls, with an area under the curve of 0.72. Lower average normalized clustering coefficient and shorter average normalized path length were associated with poorer seizure control in epilepsy patients. To conclude, individuals with juvenile myoclonic epilepsy have increased power of neural oscillatory activity at low-alpha frequencies, and increased brain network ictogenicity compared with controls, supporting evidence from studies in other epilepsies with considerable external validity. In addition, the impact of confounders on different frequency-based and network-based EEG features observed in this study highlights the need for careful consideration and control of these factors in future EEG research in idiopathic generalized epilepsy particularly for their use as biomarkers.

Original languageEnglish
Article numberfcac180
JournalBrain Communications
Volume4
Issue number4
DOIs
Publication statusPublished - 2022

Keywords

  • biomarkers
  • EEG
  • epilepsy
  • heterogeneity
  • networks

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