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Likelihood analysis of disequilibrium mapping and related problems.

机译:不平衡映射的可能性分析以及相关问题。

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摘要

In this paper a theory is developed that provides the sampling distribution of alleles at a diallelic marker locus closely linked to a low-frequency allele that arose as a single mutant. The sampling distribution provides a basis for maximum-likelihood estimation of either the recombination rate, the mutation rate, or the age of the allele, provided that the two other parameters are known. This theory is applied to (1) the data of Hästbacka et al., to estimate the recombination rate between a locus associated with diastrophic dysplasia and a linked RFLP marker; (2) the data of Risch et al., to estimate the age of a presumptive allele causing idiopathic distortion dystonia in Ashkenazi jews; and (3) the data of Tishkoff et al., to estimate the date at which, at the CD4 locus, non-African lineages diverged from African lineages. We conclude that the extent of linkage disequilibrium can lead to relatively accurate estimates of recombination and mutation rates and that those estimates are not very sensitive to parameters, such as the population age, whose values are not known with certainty. In contrast, we also conclude that, in many cases, linkage disequilibrium may not lead to useful estimates of allele age, because of the relatively large degree of uncertainly in those estimates.
机译:在本文中,发展了一种理论,该理论提供了在与单个等位基因出现的低频等位基因紧密相关的,在拨号标记位点上的等位基因的采样分布。如果已知其他两个参数,则采样分布为重组率,突变率或等位基因的年龄的最大似然估计提供了基础。该理论适用于(1)Hästbacka等人的数据,以估计与非典型增生相关的基因座与连锁的RFLP标记之间的重组率; (2)Risch等人的数据,以估计引起阿什肯纳兹族犹太人特发性变形肌张力障碍的等位基因年龄。 (3)Tishkoff等人的数据,以估计在CD4位点上非非洲血统与非洲血统发生分歧的日期。我们得出结论,连锁不平衡的程度可以导致相对准确的重组和突变率估计,并且这些估计对参数(例如人口年龄)不是很敏感,这些参数的值尚不确定。相反,我们还得出结论,在许多情况下,连锁不平衡可能无法得出等位基因年龄的有用估计值,因为这些估计值的不确定性相对较高。

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