Oda Masaya, Maruyama Hirofumi, Komure Osamu, Morino Hiroyuki, Terasawa Hideo, Izumi Yuishin, Imamura Tohru, Yasuda Minoru, Ichikawa Keiji, Ogawa Masafumi, Matsumoto Masayasu, Kawakami Hideshi
Department of Clinical Neuroscience and Therapeutics, Graduate School of Biomedical Sciences, Hiroshima University, Hiroshima, Japan.
Arch Neurol. 2004 Feb;61(2):209-12. doi: 10.1001/archneur.61.2.209.
Spinocerebellar ataxia type 17 (SCA17) is an autosomal dominant cerebellar ataxia caused by expansion of CAG/CAA trinucleotide repeats in the TATA-binding protein (TBP) gene. Because the number of triplets in patients with SCA17 in previous studies ranged from 43 to 63, the normal number of trinucleotide units has been considered to be 42 or less. However, some healthy subjects in SCA17 pedigrees carry alleles with the same number of expanded repeats as patients with SCA17.
To investigate the minimum number of CAG/CAA repeats in the TBP gene that causes SCA17.
We amplified the region of the TBP gene containing the CAG/CAA repeat by means of polymerase chain reaction and performed fragment and sequence analyses.
The subjects included 734 patients with SCA (480 patients with sporadic SCA and 254 patients with familial SCA) without CAG repeat expansions at the SCA1, SCA2, Machado-Joseph disease, SCA6, SCA7, or dentatorubral-pallidolluysian atrophy loci, with 162 healthy subjects, 216 patients with Parkinson disease, and 195 with Alzheimer disease as control subjects.
Eight patients with SCA possessed an allele with more than 43 CAG/CAA repeats. Among the non-SCA groups, alleles with 43 to 45 repeats were seen in 3 healthy subjects and 2 with Parkinson disease. In 1 SCA pedigree, a patient with possible SCA17 and her healthy sister had alleles with 45 repeats. A 34-year-old man carrying alleles with 47 and 44 repeats (47/44) had developed progressive cerebellar ataxia and myoclonus at 25 years of age, and he exhibited dementia and pyramidal signs. He was the only affected person in his pedigree, although his father and mother carried alleles with mildly expanded repeats (44/36 and 47/36, respectively). In another pedigree, 1 patient carried a 43-repeat allele, whereas another patient had 2 normal alleles, indicating that the 43-repeat allele may not be pathologic in this family.
We estimate that 44 CAG/CAA repeats is the minimum number required to cause SCA17. However, the existence of unaffected subjects with mildly expanded triplets suggests that the TBP gene mutation may not penetrate fully. Homozygosity of alleles with mildly expanded triplet repeats in the TBP gene might contribute to the pathologic phenotype.
17型脊髓小脑共济失调(SCA17)是一种常染色体显性遗传性小脑共济失调,由TATA结合蛋白(TBP)基因中CAG/CAA三核苷酸重复序列的扩增引起。由于先前研究中SCA17患者的三联体数量范围为43至63,因此三核苷酸单位的正常数量被认为是42个或更少。然而,SCA17家系中的一些健康受试者携带与SCA17患者相同数量的扩增重复序列的等位基因。
研究导致SCA17的TBP基因中CAG/CAA重复序列的最小数量。
我们通过聚合酶链反应扩增了包含CAG/CAA重复序列的TBP基因区域,并进行了片段和序列分析。
研究对象包括734例无SCA1、SCA2、马查多-约瑟夫病、SCA6、SCA7或齿状核红核苍白球路易体萎缩位点CAG重复序列扩增的脊髓小脑共济失调患者(480例散发性SCA患者和254例家族性SCA患者),162名健康受试者、216例帕金森病患者和195例阿尔茨海默病患者作为对照。
8例脊髓小脑共济失调患者拥有一个CAG/CAA重复序列超过43个的等位基因。在非脊髓小脑共济失调组中,3名健康受试者和2名帕金森病患者携带43至45个重复序列的等位基因。在一个SCA家系中,一名可能患有SCA17的患者及其健康姐妹携带45个重复序列的等位基因。一名携带47和44个重复序列(47/44)等位基因的34岁男性在25岁时出现进行性小脑共济失调和肌阵挛,并表现出痴呆和锥体束征。他是其家系中唯一受影响的人,尽管他的父亲和母亲携带轻度扩增重复序列的等位基因(分别为44/36和47/36)。在另一个家系中,一名患者携带一个43个重复序列的等位基因,而另一名患者有两个正常等位基因,这表明该家系中43个重复序列的等位基因可能无致病性。
我们估计44个CAG/CAA重复序列是导致SCA17所需的最小数量。然而,存在三联体轻度扩增的未受影响受试者表明TBP基因突变可能未完全外显。TBP基因中三联体重复序列轻度扩增的等位基因纯合性可能导致病理表型。
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