A novel compound heterozygous mutation in the COA7 gene responsible for a Chinese patient with spinocerebellar ataxia with axonal neuropathy type 3.

IF 0.8 4区医学 Q4 CLINICAL NEUROLOGY

Clinical Neuropathology Pub Date : 2022-05-23 DOI:10.5414/NP301457

Yuwei Tang, Meng Yu, Wei Zhang, H. Lv, Jianwen Deng, Jing Liu, Xin Shi, W. Liang, Zhi-rong Jia, Yun Yuan, Zhaoxia Wang, L. Meng

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引用次数: 0

Abstract

OBJECTIVE Spinocerebellar ataxia with axonal neuropathy type 3 (SCAN3) is a very rare autosomal recessive hereditary disease. Mutations in the COA7 gene, which encodes cytochrome c oxidase assembly factor 7, have been recently reported as the causative gene of SCAN3. So far, only five SCAN3 patients with COA7 mutations have been documented. Herein, we report the clinical, electrophysiological, histological, and genetic findings of a Chinese patient with SCAN3. MATERIALS AND METHODS The patient was a 31-year-old woman who presented with early-onset peripheral neuropathy and progressive ataxia. She was asked about her medical history and underwent electrophysiological examination, nerve and muscle biopsy, and gene detection. RESULTS Whole exome next-generation sequencing identified a novel compound heterozygous mutation of COA7 (c.17A>G p.D6G; c.554G>A, p.W185*) in this patient. Magnetic resonance imaging showed cerebellum and spinal cord atrophy. Nerve conduction studies and sural nerve biopsies revealed sensorimotor axonal neuropathy. Muscle biopsies showed mitochondrial abnormalities. Respiratory chain enzyme assay of skin fibroblasts showed normal respiratory chain complex activities. Additionally, the clinical data on previously reported SCAN patients with identified genetic causes in PubMed was summarized. Compared with SCAN1 and SCAN2 patients, SCAN3 patients had earlier onset age, less cognitive impairment, and no ocular signs. CONCLUSION We reported the first patient diagnosed with SCAN3 in China. A novel mutation in the gene COA7 (c.554G>A, p.W185*) expanded the genetic spectrum of the disease.

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COA7基因的一个新的复合杂合突变导致一名中国脊髓小脑共济失调伴3型轴索神经病变患者。

目的:脑小脑共济失调伴轴突神经病3型(SCAN3)是一种非常罕见的常染色体隐性遗传病。编码细胞色素c氧化酶组装因子7的COA7基因突变最近被报道为SCAN3的致病基因。到目前为止，仅记录了5例COA7突变的SCAN3患者。在此，我们报告了一例中国SCAN3患者的临床、电生理、组织学和遗传学结果。材料与方法患者为31岁女性，表现为早发性周围神经病变和进行性共济失调。询问病史，进行电生理检查、神经和肌肉活检、基因检测。结果新一代全外显子组测序鉴定出一种新的COA7复合杂合突变(c.17A>G . d6g;c.554G>A, p.W185*)。磁共振成像显示小脑和脊髓萎缩。神经传导检查和腓肠神经活检显示感觉运动轴索神经病变。肌肉活检显示线粒体异常。皮肤成纤维细胞呼吸链酶测定显示呼吸链复合物活性正常。此外，还总结了PubMed中先前报道的具有确定遗传原因的SCAN患者的临床数据。与SCAN1和SCAN2患者相比，SCAN3患者发病年龄更早，认知功能障碍更小，无眼部体征。结论:我们报道了中国首例被诊断为SCAN3的患者。COA7基因(c.554G>A, p.W185*)的新突变扩大了该疾病的遗传谱。

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来源期刊

Clinical Neuropathology 医学-病理学

CiteScore

1.60

自引率

0.00%

发文量

审稿时长

>12 weeks

期刊介绍： Clinical Neuropathology appears bi-monthly and publishes reviews and editorials, original papers, short communications and reports on recent advances in the entire field of clinical neuropathology. Papers on experimental neuropathologic subjects are accepted if they bear a close relationship to human diseases. Correspondence (letters to the editors) and current information including book announcements will also be published.