Coffin-Siris综合征3例患儿的临床表型分析和基因诊断研究

doi:10.12372/jcp.2022.21e1660

摘要/Abstract

摘要：

目的对3例Coffin-Siris综合征患儿进行临床表型分析和基因变异位点鉴定,明确其致病原因。方法采用染色体微阵列分析、家系全外显子组测序分析、家系全基因组测序分析、一代测序等多种基因检测方法进行病因学确诊。采集患儿3外周血建立永生化淋巴细胞系,用蛋白免疫印迹法检测患儿3 ARID1B蛋白表达。结果 3例患儿均因发育迟缓就诊,均合并有面容异常。患儿1伴宫内发育不全,患儿2伴反复上呼吸道感染,患儿3伴智力落后和手部异常体征。3例患儿染色体微阵列分析结果均为阴性。患儿1和患儿2采用家系全外显子组测序分析得到致病基因位点。患儿1 SMARCB1基因存在一个未见报道的新生杂合剪切变异c.363-3C>G,患儿2 ARID1B基因存在一个未见报道的新生杂合剪切变异c.3550+1(IVS13)G>A。患儿3家系全外显子组未检测到变异,经家系全基因组测序分析发现ARID1B基因携带新生杂合第11号外显子部分缺失,此位点也尚未有文献报道。蛋白免疫印迹法结果显示患儿3 ARID1B蛋白水平的表达量明显下降。结论 Coffin-siris综合征患者临床表现多样,主要以发育落后为主诉。多种基因诊断方法的综合运用,结合临床表现,可帮助确诊Coffin-Siris综合征。

关键词: Coffin-Siris综合征, 生长发育迟缓, 高通量测序

Abstract:

Objective To perform the phenotypic analysis and identify genetic variation locus in three patients with Coffin-Siris Syndrome (CSS). Methods Chromosome microarray analysis (CMA), trio-whole exome sequencing analysis (trio-WES), trio-whole genome sequencing analysis (trio-WGS), and Sanger sequencing were used for genetic diagnosis. The peripheral blood example of patient 3 was collected to establish an immortalized lymphocyte line, and the ARID1B protein expression was detected by Western Bolt (WB). Results All three patients visited the hospital for developmental retardation, and they all had facial dysmorphism. Patient 1 had intrauterine growth restriction, patient 2 was accompanied by recurrent upper respiratory tract infection, patient 3 had intellectual disability and abnormal hand manifestations. The CMA results of three patients were negative. The pathogenic gene loci of patient 1 and patient 2 were obtained by trio-WES analysis. Patient 1 has a de novo heterozygous splicing site mutation of c.363-3C>G in SMARCB1. There was a de novo heterozygous splicing site mutation of c.3550+1(IVS13) G>A in the ARID1B gene of patient 2. No pathogenic variations were identified in patient 3 by trio-WES. However, trio-WGS analysis revealed a de novo heterozygous exon 11 deletion in the ARID1B gene of patient 3. The three de novo mutations have not been reported previously. WB showed a significant decrease of ARID1B protein level in immortalized lymphocytes from patient 3. Conclusions The clinical manifestations of Coffin-Siris syndrome are diverse, and featured mainly as developmental retardation. The application of multiple genetic testing methods can help to confirm diagnosis of the Coffin-Siris syndrome.

Key words: Coffin-Siris syndrome, growth retardation, high-throughput sequencing

吴臣臣, 张惠文. Coffin-Siris综合征3例患儿的临床表型分析和基因诊断研究[J]. 临床儿科杂志, 2022, 40(5): 355-360.

WU Chenchen, ZHANG Huiwen. Clinical phenotypic and genetic analysis of three patients with Coffin-Siris syndrome[J]. Journal of Clinical Pediatrics, 2022, 40(5): 355-360.

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患儿	基因	上游引物	下游引物	产物长度/bp	退火温度/℃
患儿1	SMARCB1	TGTGTCTGGTGCCCCTACG	CCTGTTGATGGTTGTGGAGC	320	60
患儿2	ARID1B	GCAGAGGCACAAGATCCCTT	CGACAGACTGGGTTTTTGCG	203	60
患儿3	ARID1B	TGTTGGCAGGAGTACAGTCTGAC	AAATGGCTGCAAGTACCGAAA	492	60

项目	患儿1	患儿2	患儿3	正常参考值
性别	男	男	女
发病年龄	孕中晚期	出生后	出生后
就诊年龄	3月龄22天	1岁2个月	2岁8个月
确诊年龄	6月龄	1岁3个月	5岁4个月
ALT/U·L^-1	25.0	30.0	21.0	0.0~75.0
AST/U·L^-1	36.0	43.0	44.0	8.0~38.0
FT3/pmol·L^-1	6.4	6.8	7.2	3.5~6.5
FT4/pmol·L^-1	13.5	14.5	15.1	11.5~22.7
TSH/μIU·mL^-1	2.3	6.1	2.1	0.6~4.8
IGF-1/ng·mL^-1	161.0	43.1	282.0	51.0~303.0
身高/cm	60.2	77.2	91.0
体质量/kg	5.6	9.7	15.0
大运动发育迟缓	-	+	+
语言发育延迟	-	+	+
智力障碍	-	-	+
合并反复感染	-	+	-
面容异常	+	+	+
浓眉	-	-	+
长睫毛	-	-	+
多毛症	-	+	+
异常第五指/趾	-	-	+
手指指垫	-	-	+
异常脑电图	-	-	-
异常头颅MRI	+	-	-

患儿	致病基因	染色体位置(h19)	碱基改变(外显子号)	基因变异	是否为新发变异	是否为新变异	ACMG
患儿1	SMARCB1	chr22:24143128	NM_003073.3: c.363-3C>G杂合	剪切变异	是	是	LP
患儿2	ARID1B	chr6:157505570	NM_020732.3:c.3550+1(IVS13)G>A杂合	剪切变异	是	是	P
患儿3	ARID1B	chr6:157495236-157495405	NM_020732.3: EX11del 杂合	CNV	是	是	P