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Mutation analysis of the spastin gene (SPG4) in patients with hereditary spastic paraparesis

机译:遗传性痉挛性轻瘫的患者spastin基因(SPG4)突变分析

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摘要

Background-Hereditary spastic paraparesis is a genetically heterogeneous condition. Recently, mutations in the spastin gene were reported in families Linked to the common SPG4 locus on chromosome 2p21-22. Objectives-To study a population of patients with hereditary spastic paraparesis for mutations in the spastin gene (SPG4) on chromosome 2p21-22. Methods-DNA from 32 patients (12 from families known to be linked to SPG4) was analysed for mutations in the spastin gene by single strand conformational polymorphism analysis and sequencing. All patients were also examined clinically. Results-Thirteen SPG4 mutations were identified, 11 of which are novel. These mutations include missense, nonsense, frameshift, and splice site mutations, the majority of which affect the AAA cassette. We also describe a nucleotide substitution outside this conserved region which appears to behave as a recessive mutation. Conclusions-Recurrent mutations in the spastin gene are uncommon. This reduces the ease of mutation detection as a part of the diagnostic work up of patients with hereditary spastic paraparesis. Our findings have important implications for the presumed function of spastin and schemes for mutation detection in HSP patients.
机译:背景-遗传性痉挛性轻瘫是一种遗传异质性疾病。最近,在与2p21-22号染色体上的常见SPG4基因座相关的家族中报告了spastin基因的突变。目的-研究遗传性痉挛性轻瘫的患者群体中2p21-22染色体上spastin基因(SPG4)突变的情况。方法:通过单链构象多态性分析和测序分析了32例患者(12例已知与SPG4有联系的家庭)的DNA中spastin基因的突变。所有患者均接受了临床检查。结果-鉴定出13个SPG4突变,其中11个是新突变。这些突变包括错义,无意义,移码和剪接位点突变,其中大多数会影响AAA盒。我们还描述了这个保守区域外的核苷酸取代,该取代似乎表现为隐性突变。结论spastin基因的反复突变并不常见。这降低了作为遗传性痉挛性轻瘫的患者进行诊断检查的一部分的突变检测的难度。我们的发现对HSP患者中spastin的推测功能和突变检测方案具有重要意义。

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