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强直性肌营养不良:临床症状与CTG三核苷酸重复序列大小的相关性。

Myotonic dystrophy: correlation of clinical symptoms with the size of the CTG trinucleotide repeat.

作者信息

Jaspert A, Fahsold R, Grehl H, Claus D

机构信息

Department of Neurology, University of Erlangen-Nürnberg, Germany.

出版信息

J Neurol. 1995 Jan;242(2):99-104. doi: 10.1007/BF00887824.

Abstract

An unstable DNA sequence of a gene encoding a protein kinase has been identified as the molecular basis of myotonic dystrophy. The correlation between different symptoms of myotonic dystrophy and the size of this unstable base triplet (CTG)n repeat was investigated in 14 patients. DNA was prepared from whole blood by standard procedures. Detailed clinical, psychological, electrophysiological (quantified measurement of myotonia, electrocardiography) and other laboratory examinations (muscle biopsy in 4 patients, slit lamp examination) were performed. Triplet size correlated significantly with muscular disability and inversely with age at onset of the disease. A greater frequency of mental and gonadal dysfunction could be observed in patients with a larger repeat size. Other symptoms, however, such as cataract, myotonia, gastrointestinal dysfunction and cardiac abnormalities were not correlated with repeat size. Somatic mosaicism with different amplification rates in various tissues might be one possible explanation for the variable phenotypes. Furthermore, other factors such as different expression of the myotonic dystrophy gene might contribute to the clinical variability of the disease at a given triplet size.

摘要

编码蛋白激酶的基因中一段不稳定的DNA序列已被确定为强直性肌营养不良的分子基础。在14名患者中研究了强直性肌营养不良的不同症状与这种不稳定的三碱基重复序列(CTG)n大小之间的相关性。采用标准程序从全血中提取DNA。进行了详细的临床、心理、电生理(肌强直定量测量、心电图)和其他实验室检查(4例患者进行了肌肉活检、裂隙灯检查)。三碱基重复序列大小与肌肉功能障碍显著相关,与疾病发病年龄呈负相关。在重复序列较大的患者中可观察到更高频率的精神和性腺功能障碍。然而,其他症状,如白内障、肌强直、胃肠功能障碍和心脏异常与重复序列大小无关。不同组织中具有不同扩增率的体细胞镶嵌现象可能是表型变异的一种可能解释。此外,其他因素,如强直性肌营养不良基因的不同表达,可能在给定的三碱基重复序列大小情况下导致该疾病的临床变异性。

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