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Mitochondrial DNA Haplogroups Do Not Play a Role in the Variable Phenotypic Presentation of the A3243G Mutation

机译:线粒体DNA单倍体在A3243G突变的可变表型呈现中不起作用。

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摘要

Thirty-five mitochondrial (mt) DNAs from Spain that harbor the mutation A3243G in association with either MELAS (mitochondrial myopathy, encephalopathy, lactic acidosis, and strokelike episodes) syndrome or a wide array of disease phenotypes (ranging from diabetes and deafness to a mixture of chronic progressive external ophthalmoplegic symptoms and strokelike episodes) were studied by use of high-resolution restriction fragment length polymorphism analysis and control-region sequencing. A total of 34 different haplotypes were found, indicating that all instances of the A3243G mutation are probably due to independent mutational events. Haplotypes were distributed into 13 haplogroups whose frequencies were close to those of the general Spanish population. Moreover, there was no statistically significant difference in haplogroup distribution between patients with MELAS and those with disease phenotypes other than MELAS. Overall, these data indicate that the A3243G mutation harbors all the evolutionary features expected from a severely deleterious mtDNA mutation under strong negative selection, and they reveal that European mtDNA backgrounds do not play a substantial role in modulating the mutation's phenotypic expression.
机译:来自西班牙的35个线粒体(mt)DNA带有A3243G突变,与MELAS(线粒体肌病,脑病,乳酸性酸中毒和中风样发作)综合征或多种疾病表型(从糖尿病和耳聋到混合症)相关高分辨率限制性片段长度多态性分析和控制区测序研究了慢性进行性眼外肌麻痹症状和中风样发作的发生。总共发现了34种不同的单倍型,表明A3243G突变的所有实例都可能是由于独立的突变事件引起的。单倍型被分为13个单倍群,其频率与西班牙普通人群的频率接近。此外,MELAS患者与疾病表型不同于MELAS的患者之间的单倍型分布没有统计学上的显着差异。总体而言,这些数据表明A3243G突变具有强烈的负选择下严重有害的mtDNA突变所预期的所有进化特征,并且它们表明欧洲mtDNA背景在调节突变的表型表达中没有发挥重要作用。 < / sup>

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