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利用古人类基因组分析人类加速区 DNA。

Analysis of human accelerated DNA regions using archaic hominin genomes.

机构信息

Max Planck Institute for Evolutionary Anthropology, Leipzig, Germany.

出版信息

PLoS One. 2012;7(3):e32877. doi: 10.1371/journal.pone.0032877. Epub 2012 Mar 7.

Abstract

Several previous comparisons of the human genome with other primate and vertebrate genomes identified genomic regions that are highly conserved in vertebrate evolution but fast-evolving on the human lineage. These human accelerated regions (HARs) may be regions of past adaptive evolution in humans. Alternatively, they may be the result of non-adaptive processes, such as biased gene conversion. We captured and sequenced DNA from a collection of previously published HARs using DNA from an Iberian Neandertal. Combining these new data with shotgun sequence from the Neandertal and Denisova draft genomes, we determine at least one archaic hominin allele for 84% of all positions within HARs. We find that 8% of HAR substitutions are not observed in the archaic hominins and are thus recent in the sense that the derived allele had not come to fixation in the common ancestor of modern humans and archaic hominins. Further, we find that recent substitutions in HARs tend to have come to fixation faster than substitutions elsewhere in the genome and that substitutions in HARs tend to cluster in time, consistent with an episodic rather than a clock-like process underlying HAR evolution. Our catalog of sequence changes in HARs will help prioritize them for functional studies of genomic elements potentially responsible for modern human adaptations.

摘要

先前有几项将人类基因组与其他灵长类和脊椎动物基因组进行比较的研究,确定了在脊椎动物进化中高度保守但在人类谱系中快速进化的基因组区域。这些人类加速区 (HARs) 可能是人类过去适应性进化的区域。或者,它们可能是非适应性过程的结果,例如偏向性基因转换。我们使用来自伊比利亚尼安德特人的 DNA 从先前发表的 HAR 集合中捕获和测序 DNA。将这些新数据与尼安德特人和丹尼索瓦人草图基因组的鸟枪法序列相结合,我们确定了至少一个古老人类的等位基因,占 HAR 内所有位置的 84%。我们发现,8%的 HAR 替换在古老人类中没有观察到,因此从衍生等位基因尚未在现代人与古老人类的共同祖先中达到固定这一意义上说,它们是新近出现的。此外,我们发现 HAR 中的近期替换往往比基因组其他部位的替换更快地达到固定,并且 HAR 中的替换往往会随着时间的推移而聚集,这与 HAR 进化背后的偶发性而不是时钟样过程一致。我们在 HAR 中对序列变化的编目将有助于为潜在负责现代人类适应性的基因组元件的功能研究确定优先级。

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