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Detecting Population Growth, Selection and Inherited Fertility From Haplotypic Data in Humans

机译:从人类单倍型数据检测人口增长,选择和继承的生育力

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The frequency of a rare mutant allele and the level of allelic association between this allele and one or several closely linked markers are frequently measured in genetic epidemiology. Both quantities are related to the time elapsed since the appearance of the mutation in the population and the intrinsic growth rate of the mutation (which may be different from the average population growth rate). Here, we develop a method that uses these two kinds of genetic data to perform a joint estimation of the age of the mutation and the minimum growth rate that is compatible with its present frequency. In absence of demographic data, it provides a useful estimate of population growth rate. When such data are available, contrasts among estimates from several loci allow demographic processes, affecting all loci similarly, to be distinguished from selection, affecting loci differently. Testing these estimates on populations for which data are available for several disorders shows good congruence with demographic data in some cases whereas in others higher growth rates are obtained, which may be the result of selection or hidden demographic processes.
机译:罕见的突变等位基因的频率以及该等位基因与一个或几个紧密相连的标记之间的等位基因缔合水平经常在遗传流行病学中进行测量。这两个数量都与自群体中出现突变以来经过的时间和突变的固有增长率(可能与平均群体增长率不同)有关。在这里,我们开发了一种使用这两种遗传数据对突变年龄和与其当前频率兼容的最小增长率进行联合估计的方法。在没有人口统计学数据的情况下,它可以提供有用的人口增长率估算值。当此类数据可用时,来自多个基因座的估计之间的对比允许将人口统计学过程(类似地影响所有基因座)与选择过程区分开来,从而将其影响不同。在某些情况下,对可获得几种疾病数据的人群进行这些估计值的检验,可以看出与人口统计数据具有很好的一致性,而在另一些情况下,则可以得到较高的增长率,这可能是选择或隐藏人口统计学过程的结果。

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