SEMA6B基因变异致进行性肌阵挛性癫痫1例报告

doi:10.12372/jcp.2022.21e1029

Abstract

Abstract:

A 15-year-old female patient was admitted to the hospital due to developmental retardation for 14 years and significant motor and cognitive regression for more than 1 year. The clinical features of this patient were myoclonus, intention tremor, ataxia, tendon hyperreflexia, hypertonia, dysarthria, speech regression, intellectual disability and multifocal seizures. Electroencephalogram showed typical epileptic discharge and the epilepsy was refractory. The patient had developmental retardation since childhood. Walking gait instability gradually aggravated, and eventually developed into walking difficulties with tremor of limbs. In addition of seizures, language and cognitive regression of the patient was evident. Genetic testing found a variation of SEMA6B gene in the child, which was determined as a pathogenic variation combined with genetic characteristics and clinical phenotype, and the child was diagnosed as progressive myoclonic epilepsy (PME). Treatment of PME is generally anti-seizure, as well as palliative support and rehabilitation measures. Most patients have poor prognosis. Genetic testing contributes to the diagnosis and treatment of patients with refractory epilepsy. SEMA6B gene variation can lead to PME phenotype. The gene variation C.2149 (exon17) C>T has not been reported before, which expands the gene variation spectrum of PME.

Key words: progressive myoclonic epilepsy, SEMA6B gene, genetic variation, adolescent

ZHAO Jinhua, TANG Jihong, HUANG Jing, XIAO Xiao, ZHANG Bingbing, XING Yujiao, SHI Xiaoyan. Progressive myoclonic epilepsy caused by SEMA6B gene variations: a case report[J].Journal of Clinical Pediatrics, 2022, 40(9): 705-709.

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References 9

[1]	Orsini A, Valetto A, Bertini V, et al. The best evidence for progressive myoclonic epilepsy: a pathway to precision therapy[J]. Seizure, 2019, 71: 247-257. doi: 10.1016/j.seizure.2019.08.012
[2]	Hamanaka K, Imagawa E, Koshimizu E, et al. De novo truncating variants in the last exon of SEMA6B cause progressive myoclonic epilepsy[J]. Am J Hum Genet, 2020, 106(4): 549-558. doi: S0002-9297(20)30053-7 pmid: 32169168
[3]	Xiaozhen S, Fan Y, Fang Y, et al. Novel truncating and missense variants in SEMA6B in patients with early-onset epilepsy[J]. Front Cell Dev Biol, 2021, 9: 633819. doi: 10.3389/fcell.2021.633819
[4]	Bhat S, Ganesh S. New discoveries in progressive myoclonus epilepsies: a clinical outlook[J]. Expert Rev Neurother, 2018, 18(8): 649-667. doi: 10.1080/14737175.2018.1503949
[5]	张静, 张月华. 进行性肌阵孪癫痫研究进展[J]. 中华儿科杂志, 2018, 56(4): 316-319.
[6]	Nita DA, Mole SE, Minassian BA. Neuronal ceroid lipofuscinoses[J]. Epileptic Disord, 2016, 18(S2): 73-88.
[7]	Malek N, Stewart W, Greene J. The progressive myoclonic epilepsies[J]. Pract Neurol, 2015, 15(3): 164-171. doi: 10.1136/practneurol-2014-000994
[8]	张静, 张月华, 陈娇阳, 等. 进行性肌阵挛癫痫患儿26例致病基因及临床表型特点[J]. 中华儿科杂志, 2019, 57(6): 458-463.
[9]	Riva A, Guglielmo A, Balagura G, et al. Emerging treatments for progressive myoclonus epilepsies[J]. Expert Rev Neurother, 2020, 20(4): 341-350. doi: 10.1080/14737175.2020.1741350

时间	事件
6岁前	运动发育较同龄儿稍落后,语言、智力发育也落后,但能跟同龄儿一起玩耍及交流。
6岁左右	出现第一次抽搐,表现为全面性强直-阵挛性发作,后反复发作,在当地医院诊断为癫痫,予丙戊酸钠抗癫痫治疗。治疗后无抽搐发作,但有时会出现不自主肢体抖动,意向性震颤。
13岁左右	担心丙戊酸钠相关副作用,换用左乙拉西坦抗癫痫治疗,但效果欠佳,反复出现身体抖动,甚至偶尔出现全面性强直-阵挛性发作,每次约2~4min。
14岁左右	停用抗癫痫药物,停药后反复抽搐发作。出现四肢抖动明显,双手持物不稳,步态不稳、宽步,易摔倒,逐渐丧失独立行走能力,外出时需要坐轮椅。时有不自主肢体抽动、耸肩及躯体扭动。能回答简单问题,但思维迟缓,构音障碍,言语不清,计算能力倒退。
15岁	入院奥拉西坦、复合维生素口服。完善检查。
入院5天	有睡眠障碍,予艾司唑仑口服。
入院13天	基因检测发现SEMA6B基因有一无义变异,结合临床表现确诊为PME11型。家属拒绝使用抗癫痫药物及康复治疗,自动出院。

序号	性别	起病年龄	首发症状	小脑共济失调	智力运动落后	小脑畸形	变异位点	氨基酸变异	难治癫痫
1	男	6岁	癫痫、发育落后	有	有	无	c.1950_1969dup	p.Arg657Profs*35	是
2	女	11月	癫痫	有	有	有	c.1976_1982del	p.Ala659Valfs*24	是
3	男	2岁	癫痫	有	有	有	c.1991del	p.Gly664Alafs*21	否
4	女	4岁	癫痫、发育落后	有	有	有	c.1991del	p.Gly664Alafs*21	是
5	女	4岁	癫痫、发育落后	有	有	无	c.2056(exon17)C>T	p.Gln686?	是
6	男	3岁	癫痫	有	无	无	c.1483(exon14)G>T	p.Gly495Trp	否
7本例	女	6岁	癫痫、发育落后	有	有	无	c.2149(exon17)C>T	p.Q717*,172	是

Progressive myoclonic epilepsy caused by SEMA6B gene variations: a case report

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