STXBP1基因相关脑病患儿的临床表型和基因变异分析

doi:10.12372/jcp.2024.22e1145

摘要/Abstract

摘要：

目的探讨STXBP1基因相关脑病患儿的临床表型和基因变异情况。方法回顾性总结2015年10月至2022年5月收治的11例STXBP1基因相关脑病患儿的临床资料，分析其临床表型、基因结果、治疗及疗效情况。结果 11例患儿中男4例，女7例，10例患儿存在癫痫发作伴发育迟缓，1例患儿仅表现为发育迟缓。癫痫首发年龄为3天~1岁半，3个月以内起病者6例，3~12个月起病者3例，1岁以上起病者1例。常见的发作类型为痉挛和局灶发作。11例患儿均存在脑电图异常包括背景慢、多灶放电、爆发抑制和高度失律等。2例早期为大田原综合征，后期演变为婴儿痉挛症，5例为婴儿痉挛症，余为不能分型的癫痫综合征。4例患儿头颅MRI存在非特异性异常,包括髓鞘化发育落后、额颞部蛛网膜下隙增宽。所有患儿均存在STXBP1基因变异，共有11种突变类型，其中错义突变7例、移码突变1例、剪切突变1例、缺失突变2例，7例患儿的突变位点尚未见文献报道，分别为c.1694T>A、c.1115T>G、C.133_135del、C.1543dupG、6-17号外显子杂合缺失、C.429+1G>C、C.855C>G及c.842_843insGGACGACGGCCTGTGGATAGCACT。随访中11例患儿均存在不同程度发育迟缓，2例患儿已死亡，4例患儿存在孤独症样表现。10例癫痫患儿均应用左乙拉西坦治疗，1例为单独应用完全缓解，5例患儿部分有效，4例患儿无效。3例患儿癫痫发作完全缓解，余7例为药物难治性癫痫。结论 STXBP1脑病患儿发育迟缓相对严重，婴儿痉挛症表型最常见，癫痫治疗效果存在明显异质性，7个未报道突变位点丰富了STXBP1脑病的基因谱。

关键词: STXBP1基因, 发育性癫痫性脑病, 发育迟缓

Abstract:

Objective To investigate the clinical phenotype and genetic characteristics of children with developmental and epileptic encephalopathy(DEE) caused by syntaxin-binding protein 1(STXBP1) gene mutation. Methods The clinical data of 11 patient with STXBP1 gene-related encephalopathy admitted to the Third Affiliated Hospital of Zhengzhou University from October 2015 to May 2022 were retrospectively reviewed, and their clinical phenotypes, gene outcomes, treatment and efficacy were analyzed. Results Of the 11 children, 4 were males and 7 were females, 10 had seizures with developmental delay and 1 showed only developmental delay. The age of onset of epilepsy was 3 days to 1.5 years, with 6 cases starting at less than 3 months, 3 at 3-12 months, and 1 at more than 1 year of age. The common seizure types are epileptic spasm and focal seizure. All the 11 patients had the abnormal interictal electroencephalograms (EEG) including background slowness, multifocal discharge, suppression-burst, and hypsarrhythmia. Two cases had Otahara syndrome in the early stages, which evolved into infantile spasms in the later stages, five cases had infantile spasms, and the rest had epileptic syndromes that could not be typed. Four children had non-specific abnormalities on cranial MRI, including poor development of myelination, and widening of the subarachnoid space in the frontotemporal region.frontotemporal. All children had STXBP1 gene variants, with a total of 11 variant types, including 7 missense variants, 1 frameshift variant, 1 splicing variant, and 2 deletion variants, and the variant loci of the 7 children have not been reported in the literature, which were c.1694T>A, c.1115T>G, C.133_135del, C.1543dupG, exons 6-17 heterozygous deletion, C.429+1G>C, C.855C>G and c.842_843insGGACGACGGCCTGTGGGATAGCACT. During follow-up, 11patients had different degrees of developmental delay, 2 patients had died, and 4 patients had autistic like features. Ten patients with epilepsy were treated with levetiracetam. One patient was seizure free with levetiracetam alone, 5 patients showed partial response, and 4 patients showed no response on multitherapy. 3 patients was seizure free, the remaining 7 patients were drug resistant epilepsy. Conclusion STXBP1 gene-related epilepsy usually occur to infant, and infantile spasm is the most common phenotype. There is significant heterogeneity in the therapeutic effect of epilepsy. Seven unreported mutation sites enriched the gene spectrum of STXBP1 encephalopathy.

Key words: STXBP1 gene, developmental epileptic encephalopathy, developmental delay

李小丽, 张晓莉, 李肖, 韩瑞, 徐丹, 甘玲, 贾天明. STXBP1基因相关脑病患儿的临床表型和基因变异分析[J]. 临床儿科杂志, 2024, 42(2): 127-132.

LI Xiaoli, ZHANG Xiaoli, LI Xiao, HAN Rui, XU Dan, GAN Ling, JIA Tianming. Clinical phenotypes and gene mutations analysis of children with STXBP1 gene-related encephalopathy[J]. Journal of Clinical Pediatrics, 2024, 42(2): 127-132.

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参考文献 26

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患儿	性别	起病年龄	发作类型	脑电图	头像影像	抗癫痫治疗	治疗效果	发育情况 (随访)	其他
例1	女	生后3 d	局灶/痉挛强直阵挛	多灶放电高度失律	无异常	PB+LEV+TPM+ MP+生酮	无效	重度落后 1岁半死亡	?
例2	女	4月龄	局灶/痉挛	多灶放电高度失律	髓鞘化落后	VPA+LEV+CZP +TPM+丙球	部分有效	7岁重度落后孤独症	癫痫及智力低下家族史
例3	男	生后20 d	痉挛强直痉挛	爆发抑制高度失律	额颞部蛛网膜下隙增宽	PB+LEV+MP+ VGB+丙球+TPM+生酮	无效	4岁重度落后	?
例4	女	9月龄	局灶	背景慢广泛多量混合慢波	无异常	LEV	完全缓解	3岁半轻度落后	抽搐前存在发育落后
例5	女	生后9 d	局灶/痉挛	中央、顶、颞区尖慢波、棘慢波	额颞部蛛网膜下隙增宽	PB+TPM+LEV+ VPA+CZP	无效	2岁8月重度落后	癫痫家族史
例6	男	1个半月	强直阵挛痉挛	高度失律	无异常	VPA+LEV+ MP+TPM	部分有效	3岁9月重度落后	听力障碍视觉通路异常
例7	男	1岁半	局灶/痉挛	背景慢高度失律	无异常	OXC+MP+LEV+ VPA+LTG	完全缓解	8岁半重度落后	肌张力障碍
例8	女	2个月8 d	局灶/痉挛强直阵挛	背景慢高度失律	无异常	VPA+TPM+LEV VGB+ LTG+CZP+MP	完全缓解	3岁8月轻度落后孤独症	?
例9	女	3月龄	无发作	背景慢	髓鞘化落后	?	?	3岁8月重度落后孤独症	面容疑似歌舞伎综合征
例10	男	1个月21 d	强直痉挛痉挛	爆发抑制高度失律	无异常	PB+VPA+LEV +MP+TPM	无效	重度落后 2岁时死亡	二胎羊水穿刺无异常，现3岁
例11	女	8月龄	局灶不典型失神	背景慢多灶放电	无异常	LEV+TPM CZP+中药	显著有效	10岁重度落后孤独症	?

患儿	突变位点	氨基酸改变	突变类型	ACMG	HGMD是否收录
例1	c.1543dupG	p.A514fs	移码	p（PVS1+PS2+PM2）	无
例2	c.1651C>T	p.Arg551Cys	错义	P（PS2+PM1+PM2+PP3+PP5）	有
例3	c.875G>T	p.Arg292Leu	错义	LP(PS2+PM2_supporting+PP2+PP3+PP4）	有
例4	6-17号外显子		缺失	LP（PVS1+ PM2_supporting）	无
例5	c.133_135del	p.C45del	缺失	LP(PM2+PM4+PM6)	无
例6	c.17T>G	p.Leu6Arg	错义	LP（PM2+PM5+PP3+PS2）	有
例7	c.1694 T>A	p.Val565Glu	错义	LP（PMI+PM6+PM2_supporting+PP2+PP3）	无
例8	c.429+1G>C		剪切	P（PVS1+PS2+PM2+PP3）	无
例9	c.1115T>G	p.L372R	错义	LP（PS2+PM2_Supporting+pp2+pp3）	无
例10	c.842_843insGGACGACGGCCTGTGGATAGCACT C.855C>G	p.282_283insAspGlyLeuTrpIleAlaLeuAsp p.Asp285Glu	错义	LP（PS2+PM2_supporting+PM4+PP4） LP（PS2+PM2_supporting+PP2+PP4）	无
例11	c.734A>G	p.His245Arg	错义	P（PS1+PM1+PM2+PP3+PP5）	有