[Infant glycogen storage disease type Ⅳ: a clinicopathological and genetic characteristics analysis of five cases].

Q3 Medicine 中华病理学杂志 Pub Date : 2023-12-08 DOI:10.3760/cma.j.cn112151-20230727-00032

Q Y Wang, J S Wang, L Chen

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Abstract

Objective: To investigate the clinical pathology and gene mutation characteristics of patients with glycogen storage disease type Ⅳ (GSD Ⅳ). Methods: The clinical data, liver histopathology and ultrastructural morphology, and gene sequencing results of 5 GSD Ⅳ cases diagnosed in the Children's Hospital Affiliated to Shanghai Jiaotong University School of Medicine and the Children's Hospital of Fudan University from January 2015 to February 2022 were collected and analyzed retrospectively. Results: Among the 5 cases, 3 were male and 2 were female, ranging in age from 4 months to 1 year and 9 months. The clinical manifestations included fever, hepatosplenomegaly, liver insufficiency, growth retardation and hypotonia. Four cases had liver biopsy showing ground-glass-like changes in hepatocytes with intracytoplasmic inclusion bodies and varying degrees of fibrosis. Liver electron microscopy in 2 cases showed that the level of glycogen increased to varying degrees, and the cytoplasm was filled with low electron density substances. Genetic testing revealed that 3 cases had compound heterozygous variants in GBE1 gene; 1 case had a single pathogenic variant in GBE1 gene; and 1 case was deceased with no genetic testing, but each parent was tested for a heterozygous variant in the GBE1 gene. A total of 9 GBE1 gene mutations were detected, 3 of which were reported mutations and 6 novel mutations. One case died of liver cirrhosis, and 1 case underwent autologous liver transplantation. After transplantation, the liver function basically returned to normal, and the growth and development improved; the other 3 cases were managed through diet control and symptomatic treatment. Conclusions: CSD Ⅳ is an extremely rare inherited metabolic disease caused by GBE1 gene mutation, often presenting with hepatic and neuromuscular disorders, with heterogeneous clinical manifestations. The diagnosis mainly depends on histopathology and a pedigree gene analysis.

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[婴儿糖原储存病类型Ⅳ:5例临床病理及遗传特征分析]。

目的:探讨糖原储存病Ⅳ(GSDⅣ)患者的临床病理及基因突变特点。方法:回顾性分析2015年1月至2022年2月在上海交通大学医学院附属儿童医院及复旦大学附属儿童医院诊断的5例GSDⅣ患者的临床资料、肝脏组织病理学及超微结构形态及基因测序结果。结果:5例患者中，男3例，女2例，年龄4个月~ 1岁9个月。临床表现为发热、肝脾肿大、肝功能不全、生长迟缓、低张力。4例肝活检显示肝细胞有磨玻璃样改变，胞浆内包涵体和不同程度的纤维化。2例肝脏电镜示糖原水平不同程度升高，细胞质内充满低电子密度物质。基因检测显示3例GBE1基因存在复合杂合变异;1例GBE1基因单一致病变异;1例死亡病例未进行基因检测，但对每对亲本进行了GBE1基因杂合变异检测。共检测到9个GBE1基因突变，其中3个为报道突变，6个为新突变。1例死于肝硬化，1例行自体肝移植。移植后肝功能基本恢复正常，生长发育改善;其余3例均通过饮食控制和对症治疗。结论:CSDⅣ是一种极为罕见的由GBE1基因突变引起的遗传性代谢性疾病，常表现为肝脏和神经肌肉紊乱，临床表现异质性强。诊断主要依靠组织病理学和系谱基因分析。

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