中国 SCN8A 相关疾病患儿的表型和基因型谱。

Phenotypic and genetic spectrum in Chinese children with SCN8A-related disorders.

机构信息

Department of Neurology, Children's Hospital of Fudan University, Shanghai 201102, China.

出版信息

Seizure. 2022 Feb;95:38-49. doi: 10.1016/j.seizure.2021.12.011. Epub 2021 Dec 25.

DOI:10.1016/j.seizure.2021.12.011

PMID:34979445

Abstract

BACKGROUND

Pathogenic variants in SCN8A have been demonstrated with a wide spectrum of epilepsy phenotypes, ranging from benign infantile epilepsy (BIE), to early onset developmental and epileptic encephalopathy (DEE) with moderate to severe developmental delay. In order to provide further insight on the spectrum of SCN8A-related epilepsy, we aimed to explore the clinical and genetic phenotype in Chinese children.

METHODS

A cohort of fifty Chinese patients with SCN8A-related disorders was included in the retrospective study. Genetic and clinical features and treatment effect of patients were further assessed based on phenotype parameters. The pathogenicity of variants was classified using the next-generation sequencing variation study.

RESULTS

We found 50 patients who presented with severe developmental and epileptic encephalopathy (DEE, 70%), benign infantile epilepsy (BIE, 12%), developmental encephalopathy with epilepsy (16%), and severe developmental delay without epilepsy (2%). The seizure onset age ranged from 1 day to 1 year and 11 months. After anti-seizure treatment, 28% of patients obtained seizure control. Sodium channel blockers showed good prognosis in 26% of patients with severe DEE. Oxcarbazepine (OXC) monotherapy was obviously effective in patients with BIE and developmental encephalopathy with epilepsy, most importantly, 87.5% received the anti-seizure therapy with sodium channel blockers in combination. All the variants were de novo missense with exception of one splice site variant. We reported three new variants, Asn1887Ser, Ile1605Thr, and Met1869Thr, which were associated with SCN8A-BIE.

CONCLUSION

The phenotypic spectrum of SCN8A-related disorders in Chinese children ranged from severe developmental delay without epilepsy to severe DEE. Three new variants were associated with SCN8A-BIE. Sodium channel blockers were effective in treating seizures for some SCN8A-related disorders however may not be relevant to the mutant location.

摘要

背景

SCN8A 中的致病性变异与广泛的癫痫表型相关，从良性婴儿癫痫（BIE）到伴有中度至重度发育迟缓的早发性发育性和癫痫性脑病（DEE）。为了进一步了解 SCN8A 相关癫痫的谱，我们旨在探索中国儿童的临床和遗传表型。

方法

我们回顾性研究了 50 名 SCN8A 相关疾病的中国患者队列。根据表型参数进一步评估患者的遗传和临床特征以及治疗效果。使用下一代测序变异研究对变体的致病性进行分类。

结果

我们发现 50 名患者表现为严重发育性和癫痫性脑病（DEE，70%）、良性婴儿癫痫（BIE，12%）、伴癫痫的发育性脑病（16%）和严重发育迟缓而无癫痫（2%）。癫痫发作年龄从 1 天到 1 年 11 个月不等。抗癫痫治疗后，28%的患者癫痫得到控制。钠通道阻滞剂对 26%的严重 DEE 患者有良好的预后。奥卡西平（OXC）单药治疗对 BIE 和伴癫痫的发育性脑病患者明显有效，最重要的是，87.5%的患者接受了钠通道阻滞剂联合抗癫痫治疗。所有变体均为新生错义，除一个剪接位点变体外。我们报道了三个新的变体，Asn1887Ser、Ile1605Thr 和 Met1869Thr，它们与 SCN8A-BIE 相关。