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A reappraisal of complete mtDNA variation in East Asian families with hearing impairment.

机译:重新评估听力障碍的东亚家庭中完整的mtDNA变异。

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摘要

In a number of recent studies, we summarized the obvious errors and shortcomings that can be spotted in many (if not most) mitochondrial DNA (mtDNA) data sets published in medical genetics. We have reanalyzed here the complete mtDNA genome data published in various recent reports of East Asian families with hearing impairment, using a phylogenetic approach, in order to demonstrate the persistence of lab-specific mistakes in mtDNA genome sequencing in cases where those caveats were (deliberately) neglected. A phylogenetic reappraisal of complete mtDNAs with mutation A1555G (or G11778A) indeed supports the suggested lack of association between haplogroup background and phenotypic presentation of these mutations in East Asians. In contrast, the claimed pathogenicity of mutation T1095C in Chinese families with hearing impairment seems unsupported, basically because this mutation is rather basal in the mtDNA phylogeny, being specific to haplogroup M11 in East Asia. The roles of other haplogroup specific or associated variants, such as A827G, T961C, T1005C, in East Asian subjects with aminoglycoside-induced and non-syndromic hearing loss are also unclear in view of the known mtDNA phylogeny.
机译:在最近的许多研究中,我们总结了医学遗传学中发表的许多(如果不是大多数)线粒体DNA(mtDNA)数据集中可以发现的明显错误和不足。我们在这里重新分析了完整的mtDNA基因组数据,这些数据已发表在东亚听力障碍东亚家庭的最新报告中,采用了系统进化方法,目的是证明在那些警告(故意的)情况下,在mtDNA基因组测序中实验室特异性错误的持续存在。 )被忽略。对具有突变A1555G(或G11778A)的完整mtDNA进行系统发育重新评估,确实支持在东亚人中,单倍体背景与这些突变的表型表现之间缺乏关联。相反,在中国有听力障碍的家庭中,声称的T1095C突变的致病性似乎不受支持,这主要是因为该突变在mtDNA系统发育中非常基础,特定于东亚单倍体M11。鉴于已知的mtDNA系统发育,还不清楚其他单体型或相关单倍体变体,例如A827G,T961C,T1005C在具有氨基糖苷诱导和非综合征性听力损失的东亚受试者中的作用。

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