Cenobamate as add-on treatment for SCN8A developmental and epileptic encephalopathy.

IF 6.6 1区医学 Q1 CLINICAL NEUROLOGY

Epilepsia Pub Date : 2025-01-15 DOI:10.1111/epi.18257

Cathrine E Gjerulfsen, Madeleine J Oudin, Francesca Furia, Sopio Gverdtsiteli, Cecilie Johannessen Landmark, Marina Trivisano, Simona Balestrini, Renzo Guerrini, Angel Aledo-Serrano, Ricardo Morcos, Roberto Previtali, Pierangelo Veggiotti, Emilia Ricci, Guido Rubboli, Elena Gardella, Rikke S Møller

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引用次数: 0

Abstract

Objectives: Developmental and epileptic encephalopathies (DEEs) caused by pathogenic variants in SCN8A are associated with difficult-to-treat and early-onset seizures, developmental delay/intellectual disability, impaired quality of life, and increased risk of early mortality. High doses of sodium channel blockers are typically used to treat SCN8A-DEE caused by gain-of-function (GoF) variants. However, seizures are often drug resistant, and only a few patients achieve seizure freedom. In this retrospective study, the effect of cenobamate was assessed in patients with SCN8A-DEE.

Methods: Across multiple centers and through collaborations with SCN8A patient advocacy organizations, patients with SCN8A-DEE treated with cenobamate for ≥6 months were identified. Data were obtained from patients' caregivers or treating physicians through a (Research Electronic Data Capture) REDCap survey. The functional effect of the SCN8A variants was obtained from the literature or assessed by prediction tools.

Results: Twelve patients (3-25 years of age (median 8 years), 9 females) with presumed GoF SCN8A variants were treated with cenobamate for a mean period of 17 months (range 6-42 months). Countable motor seizures were meaningfully reduced in 10 of 12 patients (83%). Six patients experienced a seizure reduction above 70%, of which two achieved seizure freedom. In addition, two patients achieved a reduction in seizures ranging between 50% and 70%. An increase in seizure-free days per patient was also reported. Rescue medication was decreased in six of seven patients (85%) in need. Furthermore, 80% of patients reported non-seizure-related improvements, which included increased alertness, better sleep, and improved muscle tone. Adverse effects were reported by 50% of patients, and half resolved spontaneously or through the reduction of concomitant antiseizure medications.

Significance: Our data suggest that cenobamate is a promising and safe treatment for SCN8A-DEE, even during early childhood. As a potential precision approach to treatment, cenobamate significantly reduced seizure burden and improved non-seizure-related symptoms. These positive outcomes may also be achieved in patient cohorts with GoF variants in other voltage-gated sodium channel genes.

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塞诺巴马特作为 SCN8A 发育和癫痫性脑病的附加治疗。

目的：由SCN8A致病性变异引起的发育性和癫痫性脑病（dei）与难以治疗和早发性癫痫发作、发育迟缓/智力残疾、生活质量受损和早期死亡风险增加相关。高剂量的钠通道阻滞剂通常用于治疗由功能获得（GoF）变异引起的SCN8A-DEE。然而，癫痫发作往往是耐药的，只有少数患者实现了癫痫发作的自由。在这项回顾性研究中，评估了cenobamate对SCN8A-DEE患者的影响。方法：通过多个中心和与SCN8A患者倡导组织的合作，确定了使用cenobamate治疗≥6个月的SCN8A- dee患者。数据通过REDCap（研究电子数据采集）调查从患者护理人员或主治医生处获得。SCN8A变异的功能影响从文献中获得或通过预测工具进行评估。结果：12例假定为GoF SCN8A变异的患者（年龄3-25岁（中位8岁），9例女性）接受了cenobamate治疗，平均时间为17个月（范围6-42个月）。12例患者中有10例（83%）可计数运动癫痫发作明显减少。6例患者癫痫发作减少超过70%，其中2例实现了癫痫发作自由。此外，两名患者的癫痫发作减少了50%至70%。据报道，每位患者无癫痫发作天数也有所增加。有需要的7名患者中有6名（85%）减少了抢救用药。此外，80%的患者报告了与癫痫无关的改善，包括警觉性提高、睡眠质量改善和肌肉张力改善。50%的患者报告了不良反应，其中一半自发消退或通过减少伴随的抗癫痫药物。意义：我们的数据表明，对于SCN8A-DEE， cenobamate是一种有前景且安全的治疗方法，即使在儿童早期也是如此。作为一种潜在的精确治疗方法，cenobamate显著减轻了癫痫发作负担并改善了非癫痫相关症状。这些积极的结果也可能在其他电压门控钠通道基因中具有GoF变异的患者队列中实现。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Epilepsia 医学-临床神经学

CiteScore

10.90

自引率

10.70%

发文量

319

审稿时长

2-4 weeks

期刊介绍： Epilepsia is the leading, authoritative source for innovative clinical and basic science research for all aspects of epilepsy and seizures. In addition, Epilepsia publishes critical reviews, opinion pieces, and guidelines that foster understanding and aim to improve the diagnosis and treatment of people with seizures and epilepsy.