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Sequence and gene organization of mouse mitochondrial DNA.小鼠线粒体DNA的序列与基因组织
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人类线粒体DNA中的长度突变。

Length mutations in human mitochondrial DNA.

作者信息

Cann R L, Wilson A C

出版信息

Genetics. 1983 Aug;104(4):699-711. doi: 10.1093/genetics/104.4.699.

DOI:10.1093/genetics/104.4.699
PMID:6311667
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1202135/
Abstract

By high-resolution, restriction mapping of mitochondrial DNAs purified from 112 human individuals, we have identified 14 length variants caused by small additions and deletions (from about 6 to 14 base pairs in length). Three of the 14 length differences are due to mutations at two locations within the D loop, whereas the remaining 11 occur at seven sites that are probably within other noncoding sequences and at junctions between coding sequences. In five of the nine regions of length polymorphism, there is a sequence of five cytosines in a row, this sequence being comparatively rare in coding DNA. Phylogenetic analysis indicates that, in most of the polymorphic regions, a given length mutation has arisen several times independently in different human lineages. The average rate at which length mutations have been arising and surviving in the human species is estimated to be many times higher for noncoding mtDNA than for noncoding nuclear DNA. The mystery of why vertebrate mtDNA is more prone than nuclear DNA to evolve by point mutation is now compounded by the discovery of a similar bias toward rapid evolution by length mutation.

摘要

通过对从112名人类个体中纯化的线粒体DNA进行高分辨率限制图谱分析,我们鉴定出了14种由小片段插入和缺失(长度约为6至14个碱基对)引起的长度变异。这14种长度差异中的3种是由于D环内两个位置的突变所致,而其余11种发生在7个位点,这些位点可能位于其他非编码序列以及编码序列之间的连接处。在9个长度多态性区域中的5个区域,存在连续5个胞嘧啶的序列,该序列在编码DNA中相对罕见。系统发育分析表明,在大多数多态性区域中,特定的长度突变在不同的人类谱系中已经独立出现了几次。据估计,非编码线粒体DNA中长度突变产生并留存于人类物种中的平均速率比非编码核DNA高出许多倍。脊椎动物线粒体DNA为何比核DNA更容易通过点突变进化的谜团,现在又因发现了长度突变导致快速进化的类似偏向而变得更加复杂。