4.6 Article

Atypical EEG abnormalities in genetic generalized epilepsies

Journal

CLINICAL NEUROPHYSIOLOGY
Volume 127, Issue 1, Pages 214-220

Publisher

ELSEVIER IRELAND LTD
DOI: 10.1016/j.clinph.2015.05.031

Keywords

Paroxysmal fast; Generalized epilepsy; Spike-wave; Seizure; Topography; Morphology; Atypical

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Objective: Bilateral, symmetric and synchronous generalized epileptiform activity is considered to be the typical electroencephalographic (EEG) abnormality in genetic generalized epilepsy (GGE). We sought to study atypical EEG abnormalities in a systematic way based on 24-h ambulatory EEG recordings. Methods: The diagnosis of GGE was validated and classified into syndromes according to the International League against Epilepsy criteria. All participants underwent 24-h ambulatory EEG recording. Epileptiform discharges were counted and detailed information was entered into an electronic database. Amplitude asymmetry, focal onset/offset of paroxysms, focal discharges, atypical morphology and generalized paroxysmal fast rhythm were defined as atypical abnormalities. Results: Of the total of 120 patients, 107 had abnormal EEGs, of which 66.4% had at least one atypical epileptiform abnormality on EEG. Atypical morphology was the most frequent abnormality in 93.4% of patients, followed by amplitude asymmetry (28.0%), focal discharges (21.5%), focal onset of paroxysms (13.1%), focal offset of paroxysms (8.2%) and generalized paroxysmal fast rhythm (1.9%). The analysis of individual discharges revealed that 76% of paroxysms were of atypical morphology. Significant associations were found between (a) amplitude asymmetry and state of arousal (p < 0.001) as well as seizure-free duration (p 0.013); (b) atypical morphology and state of arousal (p < 0.001). Conclusion: In GGE, there are both common and rare atypical epileptiform EEG abnormalities that may vary according to the state of arousal and seizure-free duration. Significance: Awareness of these variations is important to avoid misdiagnosis. Crown Copyright (C) 2015 Published by Elsevier Ireland Ltd. on behalf of International Federation of Clinical Neurophysiology. All rights reserved.

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