Genetic variant reanalysis reveals a case of Sandhoff disease with onset of infantile epileptic spasm syndrome.

IF 1.2 Q4 CLINICAL NEUROLOGY

Acta Epileptologica Pub Date : 2024-03-08 DOI:10.1186/s42494-024-00149-4

Qi Zhang, Liping Zou, Qian Lu, Qiuhong Wang, Shuo Dun, Jing Wang

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Abstract

Background: Sandhoff disease (SD) i s an autosomal recessive lysosomal disease with clinical manifestations such as epilepsy, psychomotor retardation and developmental delay. However, infantile SD with onset of infantile epilepsy spasm syndrome (IESS) is extremely rare.

Case presentation: The case presented here was a 22-month-old boy, who presented with IESS and psychomotor retardation/regression at 6 months of age. The patient showed progressive aggravation of seizures and excessive startle responses. The whole exome sequencing data, which initially revealed negative results, were reanalyzed and indicated a homozygous mutation at the c.1613 + 4del splice site of the HEXB gene. The activities of β-hexosaminidase A and total hexosaminidase were significantly decreased. The fundus examination showed cherry red spots at the macula.

Conclusions: IESS can be an epileptic phenotype of infantile SD. Clinical phenotypes should be adequately collected in genetic testing. In the case of negative sequencing results, gene variant reanalysis can be performed when the patients show clinically suspicious indications.

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遗传变异再分析揭示了桑德霍夫病与婴儿癫痫痉挛综合征发病的情况。

背景：山德霍夫病（Sandhoff disease， SD）是一种常染色体隐性溶酶体疾病，临床表现为癫痫、精神运动迟缓和发育迟缓。然而，婴儿SD并发婴儿癫痫痉挛综合征（IESS）是非常罕见的。病例介绍：这里的病例是一个22个月大的男孩，他在6个月大时表现为IESS和精神运动迟缓/倒退。患者表现出癫痫发作的进行性加重和过度惊吓反应。整个外显子组测序数据，最初显示阴性结果，重新分析后发现，在c.1613 + 4del剪接位点出现纯合突变。β-己糖氨酸酶A和总己糖氨酸酶活性显著降低。眼底检查显示黄斑处有樱桃红色斑点。结论：IESS可能是婴儿SD的一种癫痫表型。在基因检测中应充分收集临床表型。在测序结果为阴性的情况下，当患者出现临床可疑指征时，可进行基因变异再分析。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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