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Novel PRNP mutation in a patient with a slow progressive dementia syndrome

机译:缓慢进行性痴呆综合征患者的新型PRNP突变

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Background Creutzfeldt-Jakob disease is a rare neurodegenerative disorder with a worldwide incidence of 1.5 per million inhabitants. About 10-15% of all cases of Creutzfeldt-Jakob disease are of genetic origin and display a large variety in clinical presentation (regarding disease duration, age at onset, and others). The goal of this report was to describe the clinical features and diagnostic tests in a patient with a novel prion protein gene (PRNP) D202G mutation. Material and Method A 71-year-old patient had all the clinical signs of Creutzfeldt-Jakob disease (CJD) but an extremely prolonged disease duration of 16 years. The 14-3-3 protein test was positive, while MRI and EEG did not show CJD typical changes. Family history was positive for cerebellar and dementia disorders without definite diagnoses. Full-length sequencing of the prion protein gene (PRNP) showed a new D202G mutation associated with valine on codon 129 of unknown significance. Methionine/valine heterozygosity at codon 129 was found. Results Conclusions These findings highlight the value of 14-3-3 and gene analysis in unclear neurological disorders to detect possibly atypical presentations of prion disorders. The significance of this new mutation will remain unclear until further such patients are reported.
机译:背景技术Creutzfeldt-Jakob病是一种罕见的神经退行性疾病,全世界每百万居民中有1.5例发病。 Creutzfeldt-Jakob疾病的所有病例中约有10-15%是遗传起源的,并且在临床表现上表现出多种多样(关于疾病持续时间,发病年龄等)。本报告的目的是描述患有新型病毒蛋白基因(PRNP)D202G突变的患者的临床特征和诊断测试。材料和方法一名71岁的患者患有克雅氏病(CJD)的所有临床体征,但病程极其延长,为16年。 14-3-3蛋白测试呈阳性,而MRI和EEG未显示CJD典型变化。没有明确诊断的小脑和痴呆症家族史为阳性。 ion病毒蛋白基因(PRNP)的全长测序表明,新的D202G突变与129位密码子上的缬氨酸有关,但意义不明。发现第129密码子的蛋氨酸/缬氨酸杂合性。结果结论这些发现强调了14-3-3和基因分析在不清楚的神经系统疾病中的价值,以发现可能是非典型的病毒疾病。直到有进一步的此类患者报道,这种新突变的意义仍不清楚。

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