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首页> 外文期刊>Investigative Genetics >Clinal distribution of human genomic diversity across the Netherlands despite archaeological evidence for genetic discontinuities in Dutch population history
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Clinal distribution of human genomic diversity across the Netherlands despite archaeological evidence for genetic discontinuities in Dutch population history

机译:尽管有考古证据证明荷兰人口历史中的遗传不连续性,但人类基因组多样性在整个荷兰的分布分布

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Background The presence of a southeast to northwest gradient across Europe in human genetic diversity is a well-established observation and has recently been confirmed by genome-wide single nucleotide polymorphism (SNP) data. This pattern is traditionally explained by major prehistoric human migration events in Palaeolithic and Neolithic times. Here, we investigate whether (similar) spatial patterns in human genomic diversity also occur on a micro-geographic scale within Europe, such as in the Netherlands, and if so, whether these patterns could also be explained by more recent demographic events, such as those that occurred in Dutch population history. Methods We newly collected data on a total of 999 Dutch individuals sampled at 54 sites across the country at 443,816 autosomal SNPs using the Genome-Wide Human SNP Array 5.0 (Affymetrix). We studied the individual genetic relationships by means of classical multidimensional scaling (MDS) using different genetic distance matrices, spatial ancestry analysis (SPA), and ADMIXTURE software. We further performed dedicated analyses to search for spatial patterns in the genomic variation and conducted simulations (SPLATCHE2) to provide a historical interpretation of the observed spatial patterns. Results We detected a subtle but clearly noticeable genomic population substructure in the Dutch population, allowing differentiation of a north-eastern, central-western, central-northern and a southern group. Furthermore, we observed a statistically significant southeast to northwest cline in the distribution of genomic diversity across the Netherlands, similar to earlier findings from across Europe. Simulation analyses indicate that this genomic gradient could similarly be caused by ancient as well as by the more recent events in Dutch history. Conclusions Considering the strong archaeological evidence for genetic discontinuity in the Netherlands, we interpret the observed clinal pattern of genomic diversity as being caused by recent rather than ancient events in Dutch population history. We therefore suggest that future human population genetic studies pay more attention to recent demographic history in interpreting genetic clines. Furthermore, our study demonstrates that genetic population substructure is detectable on a small geographic scale in Europe despite recent demographic events, a finding we consider potentially relevant for future epidemiological and forensic studies.
机译:背景技术在欧洲,人类遗传多样性中存在东南到西北的梯度,这是一个公认的观察结果,最近已被全基因组范围的单核苷酸多态性(SNP)数据证实。传统上,这种模式是由旧石器时代和新石器时代的主要史前人类迁徙事件解释的。在这里,我们调查了人类基因组多样性中的(相似)空间模式是否也在欧洲(如荷兰)的微观地理范围内发生,如果是的话,这些模式是否也可以用最近的人口统计学事件来解释,例如发生在荷兰人口史上的那些。方法我们使用全基因组人类SNP Array 5.0(Affymetrix)在全国54个站点的443,816个常染色体SNP上新收集了999名荷兰人的数据。我们使用不同的遗传距离矩阵,空间血统分析(SPA)和ADMIXTURE软件,通过经典多维标度(MDS)研究了个体的遗传关系。我们进一步进行了专门的分析,以寻找基因组变异中的空间模式,并进行了模拟(SPLATCHE2),以对观察到的空间模式提供历史解释。结果我们在荷兰人口中发现了一个微妙但明显的基因组人口亚结构,从而可以区分东北,中西部,中北部和南部。此外,我们在整个荷兰的基因组多样性分布中观察到了东南到西北部沿线的统计显着性,与整个欧洲的早期发现相似。模拟分析表明,这种基因组梯度可能同样是由古代以及荷兰历史上的最近事件引起的。结论考虑到荷兰遗传不连续的强大考古证据,我们将观察到的基因组多样性的临床模式解释为由荷兰人口历史中的近期事件而非古代事件引起。因此,我们建议未来的人类遗传学研究在解释遗传谱系时应更加关注最近的人口统计学历史。此外,我们的研究表明,尽管最近发生了人口统计学事件,但在欧洲较小的地理规模上仍可检测到遗传种群的亚结构,我们认为这一发现可能与未来的流行病学和法医研究有关。

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