Adolescent-onset epilepsy and deterioration associated with CAD deficiency: A case report

IF 1.4 4区医学 Q4 CLINICAL NEUROLOGY

Brain & Development Pub Date : 2024-04-18 DOI:10.1016/j.braindev.2024.04.001

Sebastián Silva , Mónica Rosas , Benjamín Guerra , Marión Muñoz , Atsushi Fujita , Masamune Sakamoto , Naomichi Matsumoto

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引用次数: 0

Abstract

Introduction

CAD (MIM*114010) encodes a large multifunctional protein with the enzymatic activity of the first three enzymes initiating and controlling the de novo pyrimidine biosynthesis pathway. Biallelic pathogenic variants in CAD cause the autosomal recessive developmental and epileptic encephalopathy 50 (MIM #616457) or CAD deficiency presenting with epilepsy, status epilepticus (SE), neurological deterioration and anemia with anisopoikilocytosis. Mortality is around 9% of patients, mainly related to the no use of its specific treatment with uridine. Majority of reported cases have an early onset during infancy, with some few starting later in childhood.

Case report

Here we report a deceased female patient with CAD deficiency whose epilepsy started at 14 years. She showed a rapid neurologic deterioration including cognitive decline, electroencephalographic background slowing which later evolved to a fatal refractory SE and supra and infratentorial atrophy on neuroimaging. Anemia developed after SE onset.

Methods and results

her post-mortem whole exome sequencing identified biallelic missense variants in CAD (NM_004341.5): c.[2944G > A];[5366G > A] p.[(Asp982Asn)];[(Arg1789Gln)]. Our review of twenty-eight reported cases (2015–2023) revealed an epilepsy age onset from neonatal period to 7 years and the SE prevalence of 46 %.

Discussion

With our case, we highlight the relevance of suspecting this treatable condition in older patients and in SE with no evident etiology.

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青少年癫痫和病情恶化与 CAD 缺乏症有关：病例报告

导言CAD（MIM*114010）编码一种大型多功能蛋白质，具有启动和控制嘧啶从头生物合成途径的前三种酶的酶活性。CAD 的双倍拷贝致病变体会导致常染色体隐性发育性和癫痫性脑病 50（MIM #616457）或 CAD 缺乏症，表现为癫痫、癫痫状态（SE）、神经系统恶化和贫血伴无异形血小板增多。患者死亡率约为 9%，主要与未使用尿苷进行特异性治疗有关。大多数报告的病例在婴儿期早期发病，也有少数病例在儿童期晚些时候发病。她的神经系统状况迅速恶化，包括认知能力下降、脑电图背景变慢，后来演变为致命的难治性癫痫，神经影像学检查显示脑室上部和下部萎缩。方法和结果尸检全外显子测序发现了 CAD（NM_004341.5）的双偶缺失变异：c. [2944G > A]; [5366G > A] p. [(Asp982Asn)];[(Arg1789Gln)]。我们对 28 个报告病例（2015-2023 年）进行了回顾，发现癫痫的发病年龄从新生儿期到 7 岁不等，SE 的发病率为 46%。讨论通过我们的病例，我们强调了在老年患者和无明显病因的 SE 中怀疑这种可治疗疾病的相关性。

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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来源期刊

Brain & Development 医学-临床神经学

CiteScore

3.60

自引率

0.00%

发文量

153

审稿时长

50 days

期刊介绍： Brain and Development (ISSN 0387-7604) is the Official Journal of the Japanese Society of Child Neurology, and is aimed to promote clinical child neurology and developmental neuroscience. The journal is devoted to publishing Review Articles, Full Length Original Papers, Case Reports and Letters to the Editor in the field of Child Neurology and related sciences. Proceedings of meetings, and professional announcements will be published at the Editor''s discretion. Letters concerning articles published in Brain and Development and other relevant issues are also welcome.