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首页> 外文期刊>International Journal of Legal Medicine >Evaluating length heteroplasmy in the human mitochondrial DNA control region
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Evaluating length heteroplasmy in the human mitochondrial DNA control region

机译:评估人类线粒体DNA控制区中的长度异质性

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摘要

We present allelic data for three known and one new C-tract in the human mitochondrial DNA (mtDNA) control region, and we measure intergenerational mutation rates at such C-tracts. In detail, in a sample of 1,172 mtDNA sequences, we demonstrate the existence of an instability threshold of eight consecutive cytosines, at and above which the phenomenon of length heteroplasmy arises. To determine mutation rates, we draw on mtDNA sequences in up to four generations of 248 pedigrees for families living in high or low-radiation environmental conditions. The high-radiation sample gives the most conservative (fastest) mutation rate likely to be encountered in any forensic context. We find that the C-tract mutation rate is up to 6% per generation, and we observe an excess of cytosine gains over losses. Case studies and guidelines for evaluating mtDNA heteroplasmy are provided.
机译:我们提供了人类线粒体DNA(mtDNA)控制区域中三个已知和一个新的C道的等位基因数据,并且我们测量了此类C道的代际突变率。详细地,在1,172个mtDNA序列的样本中,我们证明了存在八个连续胞嘧啶的不稳定性阈值,在该阈值以上,会出现长度异质现象。为了确定突变率,我们针对生活在高辐射或低辐射环境条件下的家庭,使用多达四代的248个家系的mtDNA序列。高辐射样本给出了在任何法医背景下可能遇到的最保守(最快)的突变率。我们发现,C代突变率高达每代6%,并且我们观察到胞嘧啶的获得超过损失。提供了案例研究和评估mtDNA异质性的指南。

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