Efficacy and tolerability of immediate switch from sodium channel blockers to Lacosamide

• Published in: Epilepsy & behavior Vol. 145; p. 109355
• Main Authors: Talha Özgün, Orhan, Kandemir Yılmaz, Melek, Mert Atmaca, Murat, Keskin Güler, Selda, Buluş, Eser, Duman, Arda, Çelebi, Özlem, Gürses, Candan
• Format: Journal Article
• Language: English
• Published: United States Elsevier Inc 01.08.2023
• Subjects: Anti-seizure medication; Epilepsy; Lacosamide; Switch; Switch; Epilepsy; Anti-seizure medication; Lacosamide
• ISSN: 1525-5050; 1525-5069
• DOI: 10.1016/j.yebeh.2023.109355

•Immediate switch from SCBs to LCM is safe and tolerable with good response rates in both focal- and generalized-onset seizures.•The likelihood of a successful switch is higher in patients when the reason for the switch is AEs.•Immediate switching seems like a preferable option with a decreased risk of AEs. Lacosamide (LCM) is a new-generation anti-seizure medication approved for monotherapy and add-on therapy for focal-onset epilepsy. It has novel pharmacodynamics and favorable pharmacokinetic qualities with good clinical response. This study aims to evaluate the effectiveness and tolerability of LCM when used in the immediate switch from sodium channel blockers in patients with focal-onset and generalized-onset epilepsies. This retrospective, multicenter observational study was conducted with adult patients who received LCM as mono- or polytherapy through immediate switch with 6 to 52 months follow-up. The clinical data obtained during the follow-up period were analyzed to assess retention rate, seizure freedom, more than 50% seizure reduction, and adverse effects. A total of 32 patients (eight females, 24 males) with a median age of 49.75 (range, 23–86) years, median age at epilepsy onset of 32.58 (range, 0.5–85) years, and median epilepsy duration of 17.17 (range, 1–46) years were included in this study. Seizure frequency was between 1 and 90 in the past 6 months. Seven (21.9%) of the patients had structural brain lesions and 27 (84.4%) of the patients had EEG abnormalities. The adverse effects leading to switching were hyponatremia, rash, elevated liver enzymes, pain, and erectile dysfunction. At 14.34 (range, 6–52) months follow-up, 30 (93.75%) patients in total retained LCM, 20 (66.7%) of them were seizure-free, and 13 were on LCM monotherapy. Responder rate was 81.25%. Eight (25%) of the patients experienced adverse effects after the immediate switch. One patient with generalized-onset epilepsy needed to quit LCM due to an increase in seizures. Seizure frequency did not change in three patients in the focal-onset group. Immediate switch to LCM showed favorable outcomes with a significant reduction in seizure frequency, high retention rates, and tolerable adverse effect profiles in both focal-onset and generalized-onset seizures.