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The ability of human nuclear DNA to cause false positive low-abundance heteroplasmy calls varies across the mitochondrial genome

机译:人类核DNA引起假阳性低丰度异质性调用的能力在整个线粒体基因组中有所不同

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摘要

BackgroundLow-abundance mutations in mitochondrial populations (mutations with minor allele frequency ≤ 1%), are associated with cancer, aging, and neurodegenerative disorders. While recent progress in high-throughput sequencing technology has significantly improved the heteroplasmy identification process, the ability of this technology to detect low-abundance mutations can be affected by the presence of similar sequences originating from nuclear DNA (nDNA). To determine to what extent nDNA can cause false positive low-abundance heteroplasmy calls, we have identified mitochondrial locations of all subsequences that are common or similar (one mismatch allowed) between nDNA and mitochondrial DNA (mtDNA).
机译:背景线粒体种群的低丰度突变(等位基因频率≤1%的突变)与癌症,衰老和神经退行性疾病有关。尽管高通量测序技术的最新进展已大大改善了异质性鉴定过程,但该技术检测低丰度突变的能力可能会受到源自核DNA(nDNA)的相似序列的影响。为了确定nDNA可以在多大程度上导致假阳性的低丰度异质性调用,我们确定了nDNA和线粒体DNA(mtDNA)之间所有相同或相似(允许一个不匹配)的所有子序列的线粒体位置。

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