Deciphering the Natural History of SCN8A-Related Disorders.

IF 7.7 1区医学 Q1 CLINICAL NEUROLOGY

Neurology Pub Date : 2025-04-14 DOI:10.1212/wnl.0000000000213533

Jan H Magielski,Stacey Cohen,Michael C Kaufman,Shridhar Parthasarathy,Julie Xian,Elise Brimble,Nasha Fitter,Francesca Furia,Elena Gardella,Rikke Steensbjerre Møller,Ingo Helbig,Jillian L McKee

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Abstract

BACKGROUND AND OBJECTIVES SCN8A-related disorders encompass a range of neurodevelopmental and epilepsy phenotypes. However, despite representing one of the most common epilepsy-associated channelopathies, its longitudinal phenotypes remain largely uncharacterized. METHODS In this study, we harmonized electronic medical record data from 82 individuals with SCN8A-related disorders to reconstruct the natural history of the disorder in comparison with a cohort of 2,833 individuals with known or presumed genetic epilepsies. RESULTS Compared with the cohort of other known or presumed genetic epilepsies, those with SCN8A-related disorders (mean age = 8.3 years, 52% female) had >10-fold odds of bilateral tonic-clonic seizures as early as at 1 year (p = 1.70 × 10-14, OR 10.56, CI 5.85-18.90). Individuals carrying gain-of-function (GOF) SCN8A variants had particularly high seizure risk at 6 months (p = 0.007/pthreshold = 4.25 × 10-4, OR 4.71, CI 1.36-21.25) and an increased risk of global developmental delay as early as at 3 months (p = 0.002/pthreshold = 4.72 × 10-5, OR 5.67, CI 1.74-20.23) when compared with the broader SCN8A cohort. Individuals with loss-of-function variants were more likely to have atypical absence seizures, most prominently at 4.25 years (p = 0.013/pthreshold = 7.08 × 10-4, OR 32.71, CI 1.44-2,193.51). Compared with the broader SCN8A cohort, individuals with the recurrent p.Arg850Gln variant were more likely to have infantile spasms at 6 months and those with variants at the p.Arg1872Trp/Gln/Leu hotspot were more likely to have neonatal seizures. Individuals with the recurrent p.Gly1475Arg variant were more likely to have active epilepsy after 5 years of age. In later childhood, focal seizures were more prominent in individuals with the recurrent p.Arg1617Gln variant while generalized-onset seizures were more prominent with the p.Asn1877Ser variant. We also established the effectiveness of sodium channel blockers in managing SCN8A epilepsy in individuals carrying GOF variants and those whose variants have not been functionally characterized, suggesting that many unstudied SCN8A variants may have GOF mechanisms. DISCUSSION SCN8A-related disorders distinguish themselves from other genetic epilepsies by the frequent bilateral tonic-clonic seizures in infancy, prominent early epileptic and developmental features in GOF variant carriers, and unique seizure phenotypes in those with recurrent variants. Our study provides a longitudinal perspective on SCN8A-related disorders, paving the way for future precision medicine approaches.

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背景和目的SCN8A 相关疾病包括一系列神经发育和癫痫表型。方法在这项研究中，我们整合了 82 名 SCN8A 相关疾病患者的电子病历数据，与 2833 名已知或推测患有遗传性癫痫的患者进行比较，重建了该疾病的自然史。结果与其他已知或推测的遗传性癫痫队列相比，SCN8A相关疾病患者（平均年龄=8.3岁，52%为女性）早在1岁时出现双侧强直阵挛发作的几率就超过了10倍（P = 1.70 × 10-14，OR 10.56，CI 5.85-18.90）。与更广泛的SCN8A队列相比，携带功能增益（GOF）SCN8A变异的个体在6个月时癫痫发作的风险特别高（p = 0.007/pthreshold = 4.25 × 10-4，OR 4.71，CI 1.36-21.25），而且早在3个月时全面发育迟缓的风险就会增加（p = 0.002/pthreshold = 4.72 × 10-5，OR 5.67，CI 1.74-20.23）。功能缺失变异个体更有可能出现不典型失神发作，在4.25岁时最为明显（p = 0.013/pthreshold = 7.08 × 10-4，OR 32.71，CI 1.44-2,193.51）。与更广泛的SCN8A队列相比，具有复发性p.Arg850Gln变异的个体更有可能在6个月时出现婴儿痉挛，而具有p.Arg1872Trp/Gln/Leu热点变异的个体更有可能出现新生儿癫痫发作。具有复发性p.Gly1475Arg变异的个体更有可能在5岁后出现活动性癫痫。在儿童后期，具有复发性 p.Arg1617Gln 变异的个体局灶性癫痫发作更为突出，而具有 p.Asn1877Ser 变异的个体全身性癫痫发作更为突出。我们还确定了钠通道阻滞剂在控制SCN8A癫痫方面对携带GOF变异体和变异体功能尚未定性的个体的有效性，这表明许多未研究的SCN8A变异体可能具有GOF机制。讨论SCN8A相关疾病区别于其他遗传性癫痫的特点是：婴儿期双侧强直阵挛发作频繁，GOF变异体携带者的早期癫痫和发育特征突出，复发性变异体携带者的癫痫发作表型独特。我们的研究为 SCN8A 相关疾病提供了一个纵向视角，为未来的精准医疗方法铺平了道路。

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来源期刊

Neurology 医学-临床神经学

CiteScore

12.20

自引率

4.00%

发文量

1973

审稿时长

2-3 weeks

期刊介绍： Neurology, the official journal of the American Academy of Neurology, aspires to be the premier peer-reviewed journal for clinical neurology research. Its mission is to publish exceptional peer-reviewed original research articles, editorials, and reviews to improve patient care, education, clinical research, and professionalism in neurology. As the leading clinical neurology journal worldwide, Neurology targets physicians specializing in nervous system diseases and conditions. It aims to advance the field by presenting new basic and clinical research that influences neurological practice. The journal is a leading source of cutting-edge, peer-reviewed information for the neurology community worldwide. Editorial content includes Research, Clinical/Scientific Notes, Views, Historical Neurology, NeuroImages, Humanities, Letters, and position papers from the American Academy of Neurology. The online version is considered the definitive version, encompassing all available content. Neurology is indexed in prestigious databases such as MEDLINE/PubMed, Embase, Scopus, Biological Abstracts®, PsycINFO®, Current Contents®, Web of Science®, CrossRef, and Google Scholar.