CTNNB1基因变异致伴有痉挛性双瘫和视觉缺陷的神经发育障碍5例报告并文献复习

doi:10.12372/jcp.2022.21e1421

摘要/Abstract

摘要：

目的探讨伴有痉挛性双瘫和视觉缺陷的神经发育障碍(NEDSDV)患儿的临床特征和基因变异特点。方法回顾性分析2014—2020年在南京市儿童医院康复科确诊的5例NEDSDV患儿的临床表现、实验室检查及基因检测结果,结合文献复习总结NEDSDV患儿的临床及基因特点。结果 5例患儿均表现出全面性发育迟缓、小头畸形、痉挛性双瘫特征,其中例1、例2、例3、例5均有斜视,例5有严重的先天性视网膜渗出性病变。基因检测鉴定5例患儿均为新发的CTNNB1基因杂合变异,且均为截短变异（包括无义和移码变异）,其中c.478_479insTAAATGA、c.1973dupT和c.625G>T为新发现的变异。除1例患儿胼胝体压部略薄外余4例患儿均未见显著的脑影像学异常,而视网膜病变亦相对少见。结论全面性发育迟缓伴有小头畸形和痉挛性双瘫可作为疑诊NEDSDV的指征,而眼病变及脑影像学异常并非该病的必要表型,确诊有赖于基因检测。CTNNB1的3个新变异的鉴定扩展了NEDSDV的致病性变异谱。

关键词: 全面性发育迟缓, 痉挛性双瘫, 视觉缺陷, CTNNB1基因

Abstract:

Objective To investigate the clinical characteristics and genetic variants of children with neurodevelopmental disorder with spastic diplegia and visual defects (NEDSDV). Methods A retrospective analysis was performed on the clinical manifestations, laboratory examinations, and genetic testing of 5 NEDSDV children diagnosed in the rehabilitation department of Nanjing Children's Hospital from 2014 to 2020, and the clinical manifestations and genetic characteristics of the patients were summarized together with literature review. Results All the five patients showed features of global developmental delay, microcephaly and spastic diplegia. Among them, patients 1, 2, 3, and 5 all had strabismus, and patient 5 had severe congenital retinal exudative abnormalities. Genetic testing identified de novo heterozygous mutations of CTNNB1 gene in all of the five patients, and all of them were truncated mutations (including nonsense and frameshift mutations), of which c.478_479insTAAATGA, c.1973dupT and c.625G>T were newly discovered mutations. Compared with 39 cases of genetically diagnosed patients reported abroad from 2001 to 2020 (including 5 adult cases), all but one child in this study had a slightly thinner corpus callosum, the other four cases showed no significant brain imaging abnormalities, and retinopathy was relatively rare. Conclusions Global developmental delay accompanied by microcephaly and spastic diplegia can be an indication for the suspected diagnosis of NEDSDV, while ocular lesions and brain imaging abnormalities are not necessary phenotypes for clinical diagnosis, and confirmation of diagnosis depends on genetic testing. The identification of three novel variants of CTNNB1 expands the pathogenic variants spectrum of NEDSDV.

Key words: global developmental delay, spastic diplegia, visual defects, CTNNB1 gene

庞可心, 王培, 朱敏, 陆芬, 汤健, 张丽. CTNNB1基因变异致伴有痉挛性双瘫和视觉缺陷的神经发育障碍5例报告并文献复习[J]. 临床儿科杂志, 2022, 40(8): 616-622.

PANG Kexin, WANG Pei, ZHU Min, LU Fen, TANG Jian, ZHANG Li. Neurodevelopmental disorder with spastic diplegia and visual defects by CTNNB1 gene mutation: a report of 5 Chinese cases with literature review[J]. Journal of Clinical Pediatrics, 2022, 40(8): 616-622.

图/表 2

表1

5例NEDSDV患儿临床资料及基因检测结果"

项目	例1	例2	例3	例4	例5
性别	男	男	女	男	男
就诊年龄	6月	9月	1岁6月	1岁7月	1岁8月
头围（就诊时）	39cm (<-3SD)	41.5cm (-3SD~-2SD)	42cm （<-3SD）	44cm (-3SD~-2SD)	44cm (-2SD~-1SD)
视力缺陷（远视）	+	-	-	-	+
斜视	+	+	+	-	-
渗出性玻璃体视网膜病变	-	-	-	-	+
长人中、薄上唇、高腭弓	+	+	+	+	+
小鼻翼	-	-	-	+	-
白皙皮肤	+	+	+	-	-
头发异常	-	+	-	-	-
认知、运动发育迟缓	6月龄不能竖头,不会翻身,不能独坐,不能注意到玩具	9月龄不能独坐,不会翻身,仅能无意识发出“ma”	1岁6月可独坐,不可独站独走,仅会喊“爸爸、妈妈”	1岁7月可独坐,不能独站、独走,仅有简单称呼	1岁8月不能独坐,不会喊“爸爸、妈妈”,不会欢迎再见
语言障碍	+	+	+	+	+
进行性痉挛性截瘫	+	+	+	+	+
康复治疗策略	患儿入院后分别予运动疗法、肌兴奋、肌力训练、脑超声、生物反馈、针灸等综合康复训练
疗程	5个疗程（1月/疗程）	间断,约每1~3月1次	间断	间断	间断治疗3次,约每月1次
最后随访年龄	2岁1月	2岁10月	9岁	3岁9月	4岁6月
最后一次随访时认知、运动发展	可弓背屈膝独坐,但不会独站、独走,仅有简单称呼	可独坐、扶走,但不可独站、独走,会讲约10个词	独坐稳定,但不可独站、独走,可进行简单对话	可独坐,独走2-3步,但步态不稳,仅有简单称呼	不可独站
头颅MRI	-	-	-	-	胼胝体压部略薄
其他异常表现	眼裂小,双足趾长	上眼睑下垂,左手通贯掌	-	-	双眼家族性渗出性玻璃体视网膜病变,双眼渗出性视网膜脱离
CTNNB1 （NM_001904）核苷酸改变	c.1420C>T (p.R474X)	c.1543C>T (pR515X)	c.478_479insT AAATGA (p.E163Kfs*2)	c.1973dupT (p.L659Ffs*6)	c.625G>T (p.E209X)
变异类型	无义变异	无义变异	移码变异	移码变异	无义变异
变异来源	Denovo	Denovo	Denovo	Denovo	Denovo
gnomAD频率	未收录	未收录	未收录	未收录	未收录
软件预测（CADD）	37（有害）	36（有害）	-	-	37（有害）
ACMG评级	P:PVS1+PM2+PS2	P:PVS1+PM2+PS2	P:PVS1+PM2+PS2	P:PVS1+PM2+PS2	P:PVS1+PM2+PS2
dbSNP	rs1553631860	Rs397514554	未收录	未收录	未收录

表1

图1

参考文献 19

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