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DNA 滑动发生在人类微卫星位点,没有最小阈值长度:一种比较基因组学方法。

DNA slippage occurs at microsatellite loci without minimal threshold length in humans: a comparative genomic approach.

机构信息

Centre d'Ecologie Fonctionnelle et d'Evolution, UMR 5175 CNRS, 1919 route de Mende, 34095 Montpellier cedex 5, France.

出版信息

Genome Biol Evol. 2010 Jul 12;2:325-35. doi: 10.1093/gbe/evq023.

Abstract

The dynamics of microsatellite, or short tandem repeats (STRs), is well documented for long, polymorphic loci, but much less is known for shorter ones. For example, the issue of a minimum threshold length for DNA slippage remains contentious. Model-fitting methods have generally concluded that slippage only occurs over a threshold length of about eight nucleotides, in contradiction with some direct observations of tandem duplications at shorter repeated sites. Using a comparative analysis of the human and chimpanzee genomes, we examined the mutation patterns at microsatellite loci with lengths as short as one period plus one nucleotide. We found that the rates of tandem insertions and deletions at microsatellite loci strongly deviated from background rates in other parts of the human genome and followed an exponential increase with STR size. More importantly, we detected no lower threshold length for slippage. The rate of tandem duplications at unrepeated sites was higher than expected from random insertions, providing evidence for genome-wide action of indel slippage (an alternative mechanism generating tandem repeats). The rate of point mutations adjacent to STRs did not differ from that estimated elsewhere in the genome, except around dinucleotide loci. Our results suggest that the emergence of STR depends on DNA slippage, indel slippage, and point mutations. We also found that the dynamics of tandem insertions and deletions differed in both rates and size at which these mutations take place. We discuss these results in both evolutionary and mechanistic terms.

摘要

微卫星或短串联重复(STR)的动力学在长、多态性位点上有很好的记录,但在较短的位点上则知之甚少。例如,DNA 滑动的最小阈值长度问题仍然存在争议。模型拟合方法通常得出结论,只有在大约 8 个核苷酸的阈值长度上才会发生滑动,这与在较短重复位点上观察到的串联重复直接观察结果相矛盾。我们使用人类和黑猩猩基因组的比较分析,研究了长度短至一个重复单元加一个核苷酸的微卫星位点的突变模式。我们发现,微卫星位点的串联插入和缺失率与人类基因组其他部分的背景率强烈偏离,并随 STR 大小呈指数增长。更重要的是,我们没有检测到滑动的下限长度。未重复位点的串联重复率高于随机插入的预期值,为全基因组插入滑动(产生串联重复的另一种机制)提供了证据。紧邻 STR 的点突变率与基因组其他区域的估计值没有差异,除了二核苷酸位点附近。我们的结果表明,STR 的出现取决于 DNA 滑动、插入和缺失滑动以及点突变。我们还发现,串联插入和缺失的动力学在发生这些突变的速率和大小上存在差异。我们从进化和机制的角度讨论了这些结果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bdf1/2997547/a01c0087d629/gbeevq023f01_ht.jpg

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