Erschienen in:
29.04.2023 | Original Communication
The phenotypic spectrum of epilepsy associated with periventricular nodular heterotopia
verfasst von:
Karina Paliotti, Christelle Dassi, Saoussen Berrahmoune, Marlin Liz Bejaran, Carlos Eduardo Valera Davila, Ariadna Borràs Martinez, Maria Carme Fons Estupiñà, Maria Margherita Mancardi, Antonella Riva, Thea Giacomini, Mariasevina Severino, Romina Romaniello, François Dubeau, Myriam Srour, Kenneth A. Myers
Erschienen in:
Journal of Neurology
|
Ausgabe 8/2023
Einloggen, um Zugang zu erhalten
Abstract
Background
Periventricular nodular heterotopia (PVNH) is a congenital brain malformation often associated with seizures. We aimed to clarify the spectrum of epilepsy phenotypes in PVNH and the significance of specific brain malformation patterns.
Methods
In this retrospective cohort study, we recruited people with PVNH and a history of seizures, and collected data via medical record review and a standardized questionnaire.
Results
One hundred individuals were included, aged 1 month to 61 years. Mean seizure onset age was 7.9 years. Ten patients had a self-limited epilepsy course and 35 more were pharmacoresponsive. Fifty-five had ongoing seizures, of whom 23 met criteria for drug resistance. Patients were subdivided as follows: isolated PVNH (“PVNH-Only”) single nodule (18) or multiple nodules (21) and PVNH with additional brain malformations (“PVNH-Plus”) single nodule (8) or multiple nodules (53). Of PVNH-Only single nodule, none had drug-resistant seizures. Amongst PVNH-Plus, 55% with multiple unilateral nodules were pharmacoresponsive, compared to only 21% with bilateral nodules. PVNH-Plus with bilateral nodules demonstrated the highest proportion of drug resistance (39%). A review of genetic testing results revealed eight patients with pathogenic or likely pathogenic single-gene variants, two of which were FLNA. Five had copy number variants, two of which were pathogenic.
Conclusions
The spectrum of epilepsy phenotypes in PVNH is broad, and seizure patterns are variable; however, epilepsy course may be predicted to an extent by the pattern of malformation. Overall, drug-resistant epilepsy occurs in approximately one quarter of affected individuals. When identified, genetic etiologies are very heterogeneous.