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Genetic evidence for unequal effective population sizes of human females and males

机译:男女有效人口规模不平等的遗传证据

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The time to the most recent common ancestor (TMRCA) of the human mitochondria (mtDNA) is estimated to be older than that of the nonrecombining portion of the Y chromosome (NRY). Surveys of variation in globally distributed humans typically result in mtDNA TMRCA values just under 200 thousand years ago (kya), whereas those for the NRY range between 46 and 110 kya. A favored hypothesis for this finding is that natural selection has acted on the NRY, leading to a recent selective sweep. An alternate hypothesis is that sex-biased demographic processes are responsible. Here, we re-examine the disparity between NRY and mtDNA TMRCAs using data collected from individual human populations-a sampling strategy that minimizes the confounding influence of population subdivision in global data sets. We survey variation at 782 bp of the mitochondrial cytochrome c oxidase subunit 3 gene as well as at 26.5 kb of noncoding DNA from the NRY in a sample of 25 Khoisan, 24 Mongolians, and 24 Papua New Guineans. Data from both loci in all populations are best described by a model of constant population size, with the exception of Mongolian mtDNA, which appears to be experiencing rapid population growth. Taking these demographic models into account, we estimate the TMRCAs for each locus in each population. A pattern that is remarkably consistent across all three populations is an approximately twofold deeper coalescence for mtDNA than for the NRY. The oldest TMRCAs are observed for the Khoisan (73.6 kya for the NRY and 176.5 kya for mtDNA), whereas those in the non-African populations are consistently lower (averaging 47.7 kya for the NRY and 92.8 kya for mtDNA). Our data do not suggest that differential natural selection is the cause of this difference in TMRCAs. Rather, these results are most consistent with a higher female effective population size.
机译:估计到人类线粒体(mtDNA)的最近共同祖先(TMRCA)的时间比Y染色体(NRY)的非重组部分的时间更长。在全球分布的人类中进行的变异调查通常会导致mtDNA TMRCA值低于20万年前(kya),而NRY的值介于46至110 kya之间。该发现的一个有利假设是自然选择作用于NRY,导致最近的选择性扫描。另一种假设是,性别偏向的人口统计过程是负责任的。在这里,我们使用从单个人群中收集的数据重新检查NRY与mtDNA TMRCA之间的差异-一种抽样策略,该策略最大程度地减少了人口细分在全球数据集中的混淆影响。我们调查了25名Khoisan,24名蒙古人和24名巴布亚新几内亚人的样本中,线粒体细胞色素C氧化酶亚基3基因的782 bp以及NRY的26.5 kb非编码DNA的变异。用恒定种群规模模型最好地描述所有种群中两个基因座的数据,蒙古的mtDNA除外,蒙古的mtDNA似乎正在快速增长。考虑到这些人口模型,我们估计了每个人群中每个基因座的TMRCAs。在所有三个种群中,一个非常一致的模式是mtDNA的结合深度大约是NRY的两倍。 Khoisan观察到最古老的TMRCA(NRY为73.6 kya,mtDNA为176.5 kya),而非非洲人群的TMRCA始终较低(NRY平均为47.7 kya,mtDNA为92.8 kya)。我们的数据并不表明差异自然选择是TMRCA中差异的原因。相反,这些结果与更高的女性有效人口规模最一致。

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