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Quantitative Estimates of Sequence Divergence for Comparative Analyses of Mammalian Genomes

机译:序列差异的定量估计用于哺乳动物基因组的比较分析

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摘要

Comparative sequence analyses on a collection of carefully chosen mammalian genomes could facilitate identification of functional elements within the human genome and allow quantification of evolutionary constraint at the single nucleotide level. High-resolution quantification would be informative for determining the distribution of important positions within functional elements and for evaluating the relative importance of nucleotide sites that carry single nucleotide polymorphisms (SNPs). Because the level of resolution in comparative sequence analyses is a direct function of sequence diversity, we propose that the information content of a candidate mammalian genome be defined as the sequence divergence it would add relative to already-sequenced genomes. We show that reliable estimates of genomic sequence divergence can be obtained from small genomic regions. On the basis of a multiple sequence alignment of ∼1.4 megabases each from eight mammals, we generate such estimates for five unsequenced mammals. Estimates of the neutral divergence in these data suggest that a small number of diverse mammalian genomes in addition to human, mouse, and rat would allow single nucleotide resolution in comparative sequence analyses.[The multiple sequence alignment of the CFTR region and a spreadsheet with the calculations performed, will be available as supplementary information online at .]
机译:在精心挑选的哺乳动物基因组集合上进行的比较序列分析可以促进鉴定人类基因组内的功能元件,并可以量化单核苷酸水平的进化限制。高分辨率定量分析对于确定功能元件内重要位置的分布以及评估携带单核苷酸多态性(SNP)的核苷酸位点的相对重要性将是有益的。因为比较序列分析中的分辨率水平是序列多样性的直接函数,所以我们建议将候选哺乳动物基因组的信息内容定义为它将相对于已测序基因组增加的序列差异。我们表明,可以从较小的基因组区域获得可靠的基因组序列差异估计。基于来自八个哺乳动物的约1.4兆碱基的多序列比对,我们对五个未测序的哺乳动物产生了这样的估计。对这些数据中性差异的估计表明,除了人,小鼠和大鼠以外,少数多样化的哺乳动物基因组还可以在比较序列分析中实现单核苷酸解析。[CFTR区的多序列比对和带有计算完成后,将在线提供补充信息。]

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