Annals of the Child Neurology Society最新文献

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Annals of the Child Neurology Society

Pub Date : 2024-02-07 DOI: 10.1002/cns3.20056

Giusi Ferrara, G. Cutillo, Irene Peterlongo, Eleonora Minacapilli, M. Iascone, Pierangelo Veggiotti, Isabella Fiocchi

We present the cases of two sisters, both harboring the same ALDH18A1 gene mutations, who presented with a complex clinical phenotype characterized by spastic paraparesis with ataxia, epileptic encephalopathy, severe psychomotor deficits, and behavioral abnormalities.Case description of two sisters with ALDH18A1 gene mutations.The older patient, a 12‐year‐old girl, exhibited spastic paraparesis with ataxia, microcephaly, facial dysmorphisms, and severe intellectual disability, with an absence of verbal language. An electroencephalogram (EEG) revealed marked spike‐and‐wave activation during sleep (SWAS), although no clinically documented seizures were observed. The younger sister, who was 9 years old, displayed a similar clinical presentation, including spastic paraparesis with ataxia, microcephaly, dysmorphisms, however, she displayed slightly more severe intellectual deficits and polymorphic seizures. EEG revealed a SWAS pattern in this case. Magnetic resonance imaging scans in both cases showed only a thin corpus callosum. Whole exome sequencing unveiled the presence of two likely pathogenic variants in compound heterozygosity within the ALDH18A1 gene. Specifically, these variants included the splice site variant c.88 + 1c.88+1G>A of paternal origin and the variant c.1364c.1364T>C (p.Leu455Ser) of maternal origin. Both sisters displayed normal blood levels of ammonia, ornithine, citrulline, arginine, and other amino acids.These findings were compatible with ALDH18A1‐related HSP complicated with a clinical and EEG pattern reminiscent of DEE‐SWAS. We present the first report of DEE‐SWAS in ALDH18A1‐related HSP, expanding the clinical manifestations of this complex neurodevelopmental condition.

我们报告了两姐妹的病例，她们均携带相同的 ALDH18A1 基因突变，表现出以痉挛性瘫痪伴共济失调、癫痫性脑病、严重精神运动障碍和行为异常为特征的复杂临床表型。年长的患者是一名 12 岁的女孩，表现为痉挛性瘫痪伴共济失调、小头畸形、面部畸形和严重的智力障碍，并且没有口头语言。脑电图（EEG）显示她在睡眠时有明显的尖波激活现象（SWAS），但没有临床记录的癫痫发作。9 岁的妹妹也有类似的临床表现，包括痉挛性瘫痪伴共济失调、小头畸形和畸形，但她的智力缺陷和多形性癫痫发作略为严重。该病例的脑电图显示为 SWAS 模式。两个病例的磁共振成像扫描均显示胼胝体较薄。全外显子组测序发现，ALDH18A1 基因中存在两个可能的致病变体，且为复合杂合型。具体来说，这些变异包括来源于父系的剪接位点变异c.88 + 1c.88+1G>A和来源于母系的变异c.1364c.1364T>C（p.Leu455Ser）。姐妹俩的血液中氨、鸟氨酸、瓜氨酸、精氨酸和其他氨基酸水平均正常。这些发现与 ALDH18A1 相关 HSP 并发症相符，其临床和脑电图模式令人联想到 DEE-SWAS。我们首次报道了ALDH18A1相关HSP中的DEE-SWAS，从而扩展了这种复杂神经发育疾病的临床表现。

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