PIGN mutation multiple congenital anomalies-hypotonia-seizures syndrome 1:A case report

BACKGROUND Multiple congenital anomalies-hypotonia-seizures syndrome 1(MCAHS1)associated with mutations in PIGN gene.CASE SUMMARY The authors report 1 case of a 16 years old girl who was presented with epilepsy,developmental delay and cerebellar atrophy.She harbors a compound heterozygous variant in the PIGN gene,include a nonsense splice site mutation(c.2557A>C)which was inherited from her mother,and a novel site mutation(c.980del)which was inherited from her father.CONCLUSION This case report expands the mutation spectrum found in PIGN gene,and strengthens the association between PIGN mutation and MCAHS1.Mutations in PIGN gene may be an underestimated cause of epilepsy.The authors recommend that,for patients with epilepsy or prenatal diagnosis of highly suspicious fetus,gene sequencing should be the preferred detection method.

1例多发先天畸形-肌张力低下-癫痫综合征1临床及遗传学分析

目的分析多发先天畸形-肌张力低下-癫痫综合征1(MCAHS1)的临床及遗传学特征。方法回顾2018年4月确诊的1例MCAHS1患儿的临床资料;应用全外显子测序及Sanger验证行基因检测;采用流式细胞术分析患儿外周血粒细胞表面糖基磷脂酰肌醇(GPI)锚定蛋白FLAER、CD16、CD24、CD58、CD59表达量。结果男性患儿,4月龄,因阵发性双眼上翻,发育落后就诊;患儿有特殊面容、肌张力低下。全外显子测序发现患儿PIGN基因存在2个杂合变异,c.343G>C和c.1694G>T,分别来自于临床表型正常的母亲和父亲,为复合杂合变异。该变异尚未见报道,经美国医学遗传学与基因组学学会(ACMG)指南评级为疑似致病性变异。该复合杂合变异导致粒细胞表面GPI锚定蛋白的表达量下降。随访发现患儿10月龄出现发热抽搐,15月龄出现癫痫,口服丙戊酸钠后发作控制。经康复治疗患儿仍发育缓慢。文献检索已经报道MCAHS1患者18例,基因变异以错义变异最常见,多数患儿预后不佳。结论该MCAHS1患儿的基因测序扩充了MCAHS 1基因变异谱。

PIGN基因变异所致多发先天畸形-肌张力低下-癫痫综合征1例患儿的遗传学分析

目的分析1例多发先天畸形-肌张力低下-癫痫综合征1(MCAHS1)患儿的临床表型及遗传学病因。方法收集2023年3月因"间断肢体抽动2年"就诊于青岛大学附属医院的1例MCAHS1患儿的临床资料。采集患儿及其父母的外周血样,对患儿进行全外显子组测序。对候选变异进行Sanger测序家系验证。根据美国医学遗传学与基因组学学会(ACMG)相关指南对变异进行致病性分析。结果患儿为2岁男性,表现为特殊面容、肢体畸形、肌张力低下、运动智力发育落后及癫痫发作。全外显子组测序发现其携带PIGN基因复合杂合变异:c.963G>A(p.Q321=)和c.994A>T(p.I332F),分别遗传自表型正常的母亲与父亲。根据ACMG相关指南,c.963G>A变异判定为致病性(PVS1+PM2_Supporting+PM3),c.994A>T变异判定为意义未明(PM2_Supporting+PP3)。结论本研究发现的PIGN基因变异位点扩展了MCAHS1的变异谱,有助于明确其基因型与表型的对应关系。