伴有眼球运动失用和低白蛋白血症的早发性共济失调： aprataxin基因突变

Early-onset ataxia with ocular motor apraxia and hypoalbuminemia: the aprataxin gene mutations.

作者信息

Shimazaki H, Takiyama Y, Sakoe K, Ikeguchi K, Niijima K, Kaneko J, Namekawa M, Ogawa T, Date H, Tsuji S, Nakano I, Nishizawa M

机构信息

Department of Neurology, Jichi Medical School, Tochigi, Japan.

出版信息

Neurology. 2002 Aug 27;59(4):590-5. doi: 10.1212/wnl.59.4.590.

DOI:10.1212/wnl.59.4.590

PMID:12196655

Abstract

BACKGROUND

Early-onset ataxia with hypoalbuminemia is regarded as a variant form of Friedreich ataxia in Japan. Early-onset ataxia with hypoalbuminemia and ataxia with ocular motor apraxia have been considered as the same clinical entity because of the recent identification of a common mutation in the aprataxin gene. A new clinical entity named early-onset ataxia with ocular motor apraxia and hypoalbuminemia (EAOH) has been proposed to explain these two diseases.

OBJECTIVE

To disclose the clinical features of EAOH and to identify the mutations in the aprataxin gene in six patients in four Japanese families with EAOH.

METHODS

The clinical features, laboratory findings, sural nerve biopsy results, and brain MRI or CT findings for these patients were evaluated, and molecular analysis was performed, which involved sequencing of the aprataxin gene directly or use of the subcloning method.

RESULTS

Cerebellar ataxia and peripheral neuropathy were noted in all six patients. Ocular motor apraxia was observed in five patients; two of these patients had obvious head thrust. Choreiform movements of the limbs and mental deterioration were observed in five patients. Although foot deformity was noted in five patients, kyphoscoliosis was noted only in one patient. In all patients, hypoalbuminemia and hypercholesterolemia were evident, and brain MRI or CT showed marked cerebellar atrophy. Nerve biopsy revealed depletion of large myelinated fibers in three of the five patients examined. Molecular analysis of the aprataxin gene revealed an insertion mutation (insT at nt167) and two missense mutations (A-to-G transition at nt80 and C-to-T transition at nt95, the former being novel).

CONCLUSION

We found clinical heterogeneity in the patients with EAOH in this study. With the disease course, the choreiform movements tended to reduce in degree, and hypoalbuminemia became evident. Molecular analysis identified one insertion and two missense mutations including a novel missense one, which was located at a highly conserved amino acid residue in the aprataxin gene product.

摘要

背景

在日本，早发性共济失调伴低白蛋白血症被视为弗里德赖希共济失调的一种变异形式。由于最近在共济失调性动眼神经失用症基因中发现了一个共同突变，早发性共济失调伴低白蛋白血症和共济失调性动眼神经失用症被认为是同一临床实体。为了解释这两种疾病，有人提出了一种名为早发性共济失调伴动眼神经失用症和低白蛋白血症（EAOH）的新临床实体。

目的

揭示EAOH的临床特征，并鉴定4个日本EAOH家系中6例患者的共济失调性动眼神经失用症基因突变情况。

方法

对这些患者的临床特征、实验室检查结果、腓肠神经活检结果以及脑MRI或CT检查结果进行评估，并进行分子分析，包括直接对共济失调性动眼神经失用症基因进行测序或采用亚克隆方法。

结果

所有6例患者均有小脑共济失调和周围神经病变。5例患者出现动眼神经失用症；其中2例患者有明显的头部前冲。5例患者出现肢体舞蹈样动作和精神衰退。虽然5例患者有足部畸形，但只有1例患者有脊柱侧凸。所有患者均有明显的低白蛋白血症和高胆固醇血症，脑MRI或CT显示明显的小脑萎缩。神经活检显示，在接受检查的5例患者中，有3例大的有髓纤维减少。对共济失调性动眼神经失用症基因的分子分析显示，有一个插入突变（第167位核苷酸处的insT）和两个错义突变（第8十位核苷酸处的A到G转换和第95位核苷酸处的C到T转换，前者为新发现的突变）。