蛋白激酶Cγ突变导致的14型脊髓小脑共济失调。
Spinocerebellar ataxia type 14 caused by a mutation in protein kinase C gamma.
作者信息
Yabe Ichiro, Sasaki Hidenao, Chen Dong-Hui, Raskind Wendy H, Bird Thomas D, Yamashita Isao, Tsuji Shoji, Kikuchi Seiji, Tashiro Kunio
机构信息
Department of Neurology, Hokkaido University Graduate School of Medicine, Sapporo, Japan.
出版信息
Arch Neurol. 2003 Dec;60(12):1749-51. doi: 10.1001/archneur.60.12.1749.
BACKGROUND
We previously discovered spinocerebellar ataxia type 14 (SCA14) in a single Japanese family with an autosomal dominant neurodegenerative disorder characterized by cerebellar ataxia and intermittent axial myoclonus. The latter manifestation is selectively observed in patients with early onset. We mapped the locus to chromosome 19q13.4-qter, but the etiologic gene was not known. Recently, a mutation in the protein kinase C gamma gene (PRKCG) was identified in a US family of English and Dutch ancestry with autosomal dominant SCA whose disease mapped to a region overlapping that of the SCA14 locus. Different PRKCG mutations were found in another family with SCA and in a sporadic case from the United States. Axial myoclonus was not observed in any of these US families.
OBJECTIVES
To determine whether a mutation in the PRKCG gene is responsible for SCA14 and to investigate the prevalence of PRKCG mutations in Japanese patients with autosomal dominant SCA.
PATIENTS AND METHODS
Direct nucleotide sequencing analysis of the 18 coding exons of the PRKCG gene was performed in the 19 members of the original Japanese family with SCA14 and in 24 Japanese probands with SCA. After identifying a PRKCG mutation, DNA samples from 72 patients with multiple system atrophy and 50 healthy individuals were examined for the mutation as controls.
RESULTS
Sequence analysis revealed a novel missense mutation, Gln127Arg, in all affected members of the family with SCA14. This mutation was not found in 122 control individuals. No mutations in the PRKCG gene were detected in the group of 24 probands with SCA of unknown type.
CONCLUSIONS
These findings document that SCA14 is caused by mutations in the PRKCG gene. The observation that all 4 PRKCG mutations identified in patients with SCA to date are located in exon 4 suggests a critical role for this region of the gene in cerebellar function. Mutations in the same region of the gene can result in myoclonus in some families but not in others.
背景
我们之前在一个日本家族中发现了14型脊髓小脑共济失调(SCA14),该家族患有一种常染色体显性神经退行性疾病,其特征为小脑共济失调和间歇性轴性肌阵挛。后者的表现仅在早发型患者中出现。我们将该基因座定位于19号染色体19q13.4 - qter,但致病基因尚不清楚。最近,在美国一个有英国和荷兰血统的常染色体显性SCA家族中,发现蛋白激酶Cγ基因(PRKCG)发生了突变,该家族疾病的基因座与SCA14基因座的区域重叠。在另一个SCA家族和一名来自美国的散发病例中发现了不同的PRKCG突变。在这些美国家族中均未观察到轴性肌阵挛。
目的
确定PRKCG基因的突变是否导致SCA14,并调查日本常染色体显性SCA患者中PRKCG突变的发生率。
患者和方法
对最初患有SCA14的日本家族的19名成员以及24名日本SCA先证者进行PRKCG基因18个编码外显子的直接核苷酸测序分析。在鉴定出PRKCG突变后,检测72例多系统萎缩患者和50名健康个体的DNA样本作为对照。
结果
序列分析在患有SCA14的家族所有患病成员中发现了一个新的错义突变,即Gln127Arg。在122名对照个体中未发现该突变。在24例不明类型SCA先证者组中未检测到PRKCG基因的突变。
结论
这些发现证明SCA14是由PRKCG基因突变引起的。迄今为止在SCA患者中鉴定出的所有4个PRKCG突变均位于第4外显子,这表明该基因的这一区域在小脑功能中起关键作用。该基因同一区域的突变在一些家族中可导致肌阵挛,而在其他家族中则不会。
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