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首页> 外文期刊>Human Biology: Official Publication of the Human Biology Council >How can we distinguish between mutational 'hot spots' and 'old sites' in human mtDNA samples?
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How can we distinguish between mutational 'hot spots' and 'old sites' in human mtDNA samples?

机译:我们如何区分人类mtDNA样本中的突变“热点”和“旧位点”?

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摘要

New research into variation in mutation rates across nucleotide positions in human mitochondrial DNA (mtDNA) calls into question population genetics models that assume a constant mutation rate for all sites in a sequence, particularly for hypervariable control region segments I and II. Related to this research is discovering the extent to which highly polymorphic sites are really mutational "hot spots" rather than "old" sites rooted early in the phylogenetic tree. This issue is addressed through the analysis of linkage disequilibrium patterns in the mtDNAs of 10 human populations. Hot spots can be expected to show little or no disequilibrium since they can be interpreted as having randomly expressed patterns. In fact, the results suggest that many highly polymorphic sites are not old sites, but instead are hot spots. Suspected hot spots are listed and compared with hypervariable sites given by Wakeley (1993) and Hasegawa et al. (1993).
机译:关于人类线粒体DNA(mtDNA)核苷酸位置突变率变异的新研究引起了人们对种群遗传学模型的质疑,该模型假定序列中所有位点,尤其是高变控制区节段I和II的突变率都是恒定的。与这项研究相关的是,发现高度多态性位点实际上是突变“热点”的程度,而不是植根于系统发生树的早期的“旧”位点。通过分析10个人的mtDNA中的连锁不平衡模式,可以解决此问题。由于热点可以解释为具有随机表达的图案,因此可以预期它们几乎不显示不平衡。实际上,结果表明许多高度多态的位点不是旧位点,而是热点。列出了可疑的热点,并与Wakeley(1993)和Hasegawa等人给出的高变位点进行了比较。 (1993)。

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