Predictors of drug‐resistant epilepsy in childhood epilepsy syndromes: A subgroup analysis from a prospective cohort study

Author:

Ayoub Dana123ORCID,Jaafar Fatima4ORCID,Al‐Hajje Amal25,Salameh Pascale2567,Jost Jeremy1,Hmaimess Ghassan8,Wazne Jaafar9,Ismail‐Fawaz Zein4,Sabbagh Sandra10,Boumediene Farid1,Beydoun Ahmad4ORCID

Affiliation:

1. National Institute of Health and Medical Research, Unit 1094, Research Institute for Development, Unit 270, Université de Limoges, University Hospital Center of Limoges, EpiMaCT–Epidemiology of Chronic Diseases in Tropical Zone, Institute of Epidemiology and Tropical Neurology, OmegaHealth Limoges France

2. Clinical and Epidemiological Research Laboratory, Faculty of Pharmacy Lebanese University Beirut Lebanon

3. School of Pharmacy Lebanese International University Beirut Lebanon

4. Department of Neurology American University of Beirut Medical Center Beirut Lebanon

5. Institut National de Santé Publique, d'Épidémiologie Clinique et de Toxicologie‐Liban Beirut Lebanon

6. Department of Primary Care and Population Health University of Nicosia Medical School Nicosia Cyprus

7. School of Medicine Lebanese American University Beirut Lebanon

8. Department of Pediatrics St. George Hospital Medical University Center, University of Balamand Beirut Lebanon

9. Rafic Hariri University Hospital Beirut Lebanon

10. Department of Pediatrics Hotel Dieu de France Hospital Beirut Lebanon

Abstract

AbstractObjectivePrevious studies assessing factors associated with drug‐resistant epilepsy (DRE) were constrained by their amalgamation of all epilepsy syndromes in their analyses and the absence of uniform criteria for defining DRE. Our objective was to identify predictors of DRE among the four primary childhood epilepsy syndrome groups within a cohort of children with new onset seizures, using the International League Against Epilepsy (ILAE) definition of DRE and the recent classification of epilepsies.MethodsThis is a prospective study of 676 children with new onset seizures initiated on antiseizure medication. Patients were monitored for the occurrence of DRE according to the ILAE criteria and were categorized into one of four epilepsy groups: self‐limited focal epilepsies (SeLFEs), genetic generalized epilepsies (GGEs), developmental epileptic encephalopathies (DEEs), and focal epilepsies. Cox regression analysis was performed to identify predictors of DRE within each epilepsy group.ResultsOverall, 29.3% of children were classified as having DRE, with the highest incidence observed among children diagnosed with DEEs (77.7%), followed by focal epilepsies (31.5%). Across the entire cohort, predictors of DRE included the presence of an epileptogenic lesion, a higher pretreatment number of seizures, experiencing multiple seizure types, presence and severity of intellectual and developmental delay, myoclonus, and younger age at epilepsy onset. Within the GGEs, only a younger age at seizure onset and experiencing multiple seizure types predicted DRE. Among focal epilepsies, predictors of DRE included the presence of an epileptogenic lesion, experiencing multiple seizure types, and having a greater number of pretreatment seizures. Within the DEEs, predictors of DRE were the occurrence of tonic seizures. Predictors of DRE within SeLFEs could not be identified.SignificanceThis study indicates that different epilepsy syndromes are associated with distinct predictors of drug resistance. Anticipation of drug resistance within various groups is feasible using accessible clinical variables throughout the disease course.

Funder

American University of Beirut

Publisher

Wiley

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