CDKL5基因相关早发性癫痫性脑病临床及脑电图特点

doi:10.12372/jcp.2023.22e0953

摘要/Abstract

摘要：

目的探讨CDKL5基因相关早发性癫痫性脑病的临床特征及脑电图特点。方法收集2013年3月至2021年9月确诊为早发性癫痫性脑病，并经二代基因测序筛选出CDKL5基因变异的6例患儿，回顾性分析其临床资料和脑电图特征。结果 6例患儿起病年龄为45天~1岁，中位年龄为2个月，随访时间均超过1年。所有患儿最初均为局灶性发作，经数天至4.3年相继出现痉挛发作、肌阵挛发作、强直发作和不典型失神发作，精神运动及智力严重落后或倒退。患儿脑电图由最初的正常或局灶、多灶性放电演变成高度失律图形，2岁后脑电图可呈现出伪周期性特点，其中1例男性患儿早期脑电图即呈现出高度失律图形，病程中动态演变不明显。6例患儿CDKL5基因变异类型均为新生变异，包括插入变异、错义变异、缺失变异。多种抗癫痫治疗均不能有效控制发作，3例应用促肾上腺皮质激素（ACTH）及生酮饮食，2例生长发育有进步。结论 CDKL5基因相关早发性癫痫性脑病起病早，多以局灶性发作起病，并相继出现多种发作类型。男孩临床及脑电异常更严重，5例女孩脑电图有一定演变规律。不同的基因变异位点可能有不同的早期脑电图表现。癫痫发作不易控制，部分患儿应用ACTH及生酮饮食可改善生长发育。

关键词: CDKL5基因, 早发性癫痫性脑病, 脑电图

Abstract:

Objective To investigate the clinical and electroencephalographic (EEG) features of CDKL5 gene-related early onset epileptic encephalopathy. Methods A total of 6 children diagnosed with early-onset epileptic encephalopathy from March 2013 to September 2021 and screened with CDKL5 gene variation by next-generation gene sequencing were collected. Their clinical data and EEG characteristics were analyzed retrospectively. Results The median onset age of six children was 2 months (45days-1 years), and the follow-up time was more than 1 year. All children initially had focal seizures that successively progressed to spasms, myoclonic seizures, tonic seizures, and atypical absence seizures over a period of days to 4.3 years. All the children had serious psychomotor and intellectual retardation or regression. The EEG of the children also evolved from the initial normal or focal or multifocal discharge into a highly irregular pattern, and the EEG showed a pseudo-periodic feature after 2 years of age. Among them, the EEG of one male child showed a highly irregular pattern in the early stage, and the dynamic evolution was not obvious in the course of the disease. All the CDKL5 gene variants in the 6 children were de novo variants, including insertion variants, missense variants and deletion variants. Several antiepileptic treatments failed to control seizures effectively. Adrenocorticotropic hormone (ACTH) and ketogenic diet were used in 3 patients, and growth and development were improved in 2 patients. Conclusions CDKL5-related early onset epileptic encephalopathy has early onset and mostly begins with focal seizures, and a variety of seizure types occur successively. The clinical and EEG abnormalities are more serious in boys, and the EEG of 5 girls shows a certain pattern of evolution. Different gene variation sites may have different early EEG manifestations. Epileptic seizures are not easy to control. The growth and development of some patients can be improved by administration of ACTH and ketogenic diet.

Key words: CDKL5 gene, early onset epileptic encephalopathy, electroencephalogram

李鹤婷, 罗小青, 江军. CDKL5基因相关早发性癫痫性脑病临床及脑电图特点[J]. 临床儿科杂志, 2023, 41(4): 272-277.

LI Heting, LUO Xiaoqing, JIANG Jun. Clinical and electroencephalographic characteristics of CDKL5 gene-related early onset epileptic encepha-lopathy[J]. Journal of Clinical Pediatrics, 2023, 41(4): 272-277.

图/表 3

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6例CDKL5基因相关早发性癫痫性脑病患儿临床及脑电图资料"

病例	性别	起病/ 随访年龄	癫痫发作	运动及语言发育	伴随症状	VEEG	基因变异	头颅MRI	治疗
1	女	2月/ 8岁	局灶性发作、痉挛、不典型失神、肌阵挛、强直发作	4月抬头，不会走、说话，不认人，互动差	肌张力低下、刻板搓手、双手失用、呼吸急促、睡眠障碍	背景慢波、发作间期小棘波→高度失律样图形→伪周期样放电	c.1794ins A	正常	TPM/LEV/VPA/PB/CZP/ACTH/CLB，效果差，发育无进步
2	女	50 d/ 1岁9个月	局灶性发作、痉挛发作	7月抬头，不会坐，眼神交流少	肌张力低下	背景及间期正常→高度失律样图形→多灶性放电,枕、颞区突出	c.211A>G p.Asn71Asp	正常	PB/VPA/TPM/ACTH/VGB，仍有发作，发育无进步
3	女	45 d/ 1岁2个月	局灶性发作、痉挛发作、强直痉挛发作	9月抬头、11月翻身，不会坐，不认人、互动差	肌张力低下，双手主动抓物差	背景正常，间期局灶性放电→高度失律样图形→多灶性放电，左颞区突出	Xp22.13区段390k缺失	正常	LEV/TPMVPA/VGB、生酮饮食，仍有发作，发育无进步
4	女	6月/ 2岁7个月	局灶、痉挛发作	2月抬头，后倒退，能短暂独坐，不会走、不会说，互动差	肌张力低下，四肢过度运动	背景正常、间期多灶、广泛性放电→高度失律样图形→伪周期样放电	c.2774-2775del	正常	LEV/ACTH/TPM/NZP/VGB/LTG/生酮饮食，仍有发作，ACTH及生酮后生长发育有进步
5	女	1岁/ 2岁	局灶、部分接痉挛发作、肌阵挛发作	4月抬头，8月独坐，1岁扶站，抽搐发作后独坐不稳	肌张力低下，不自主动作多，双手失用，睡眠障碍	背景、间期正常→高度失律样图形→多灶性放电，左颞突出	c.180G>T p.Glu60Asp	双侧额部脑外间隙稍宽	VPA/TPM/ACTH/LTG/生酮饮食，仍有发作，生酮饮食后生长发育较前进步
6	男	2月/ 2岁5个月	局灶、痉挛、强直	抬头不稳，不会说话及走路	肌张力低下	高度失律→高度失律→高度失律，睡眠期伪周期样放电	c.120-124del	胼胝体体部形态略纤细，双侧视神经眶后段及视交叉未完整显示	LEV/ACTH/VGB/生酮饮食/TPM/VPA/LTG/CLB/LCS，仍有发作，发育无进步

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