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Two-locus sampling distributions and their application.两位点抽样分布及其应用。
Genetics. 2001 Dec;159(4):1805-17. doi: 10.1093/genetics/159.4.1805.
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Linkage disequilibrium in humans: models and data.人类中的连锁不平衡:模型与数据。
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Local rates of recombination are positively correlated with GC content in the human genome.人类基因组中局部重组率与GC含量呈正相关。
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Why is there so little intragenic linkage disequilibrium in humans?为什么人类基因内的连锁不平衡如此之少?
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Linkage disequilibrium in the human genome.人类基因组中的连锁不平衡。
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Comparison of human genetic and sequence-based physical maps.人类遗传图谱与基于序列的物理图谱的比较。
Nature. 2001 Feb 15;409(6822):951-3. doi: 10.1038/35057185.
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Worldwide genetic analysis of the CFTR region.CFTR区域的全球基因分析。
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Linkage disequilibria and the site frequency spectra in the su(s) and su(w(a)) regions of the Drosophila melanogaster X chromosome.黑腹果蝇X染色体上su(s)和su(w(a))区域的连锁不平衡及位点频率谱
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Short tandem-repeat polymorphism/alu haplotype variation at the PLAT locus: implications for modern human origins.PLAT基因座处的短串联重复多态性/Alu单倍型变异:对现代人类起源的影响。
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When did the human population size start increasing?人类人口规模何时开始增长?
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基因转换和不同的群体历史可能解释多态性与连锁不平衡水平之间的差异。

Gene conversion and different population histories may explain the contrast between polymorphism and linkage disequilibrium levels.

作者信息

Frisse L, Hudson R R, Bartoszewicz A, Wall J D, Donfack J, Di Rienzo A

机构信息

Department of Human Genetics, University of Chicago, Chicago, IL 60637, USA.

出版信息

Am J Hum Genet. 2001 Oct;69(4):831-43. doi: 10.1086/323612. Epub 2001 Aug 29.

DOI:10.1086/323612
PMID:11533915
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1226068/
Abstract

To characterize linkage disequilibrium (LD) levels in human populations, we have analyzed 10 independent noncoding segments in three population samples from the major ethnic groups--that is, Africans, Asians, and Europeans. Descriptive statistics show that LD decays much faster in the African samples than in the non-African ones. With the assumption of an equilibrium model, we estimated the population crossing-over parameter (4N(e)r(bp), where N(e) is the effective population size and r(bp) is the crossing-over rate per generation between adjacent base pairs) in the presence of gene conversion. In the African sample, LD and polymorphism levels lead to similar estimates of effective population size, as expected under an equilibrium model. Conversely, in both non-African samples, LD levels suggest a smaller effective population size than that implied by polymorphism levels. This observation is paralleled by significant departures from an equilibrium model in the spectrum of allele frequencies of the non-African samples. Besides ruling out the possibility that non-African populations are at equilibrium, these results suggest different demographic history (temporal and spatial) of these groups. Interestingly, the African sample fits the expectations of an equilibrium model based on polymorphism and divergence levels and on frequency spectrum. For this sample, the estimated ratio of gene conversion to crossing-over rates is 7.3 for a mean tract length of 500 bp, suggesting that gene conversion may be more frequent than previously thought. These findings imply that disease-association studies will require a much denser map of polymorphic sites in African than in non-African populations.

摘要

为了描绘人类群体中的连锁不平衡(LD)水平,我们分析了来自主要族群(即非洲人、亚洲人和欧洲人)的三个群体样本中的10个独立非编码片段。描述性统计表明,非洲样本中的LD衰减速度比非非洲样本快得多。在基因转换存在的情况下,基于平衡模型,我们估计了群体交叉参数(4N(e)r(bp),其中N(e)是有效群体大小,r(bp)是相邻碱基对之间每代的交叉率)。在非洲样本中,LD和多态性水平导致了有效群体大小的相似估计,这正如平衡模型所预期的那样。相反,在两个非非洲样本中,LD水平表明有效群体大小比多态性水平所暗示的要小。非非洲样本的等位基因频率谱显著偏离平衡模型,这与上述观察结果一致。这些结果除了排除非非洲群体处于平衡状态的可能性外,还表明了这些群体不同的人口历史(时间和空间)。有趣的是,非洲样本符合基于多态性和分化水平以及频率谱的平衡模型预期。对于这个样本,平均片段长度为500 bp时,估计的基因转换与交叉率之比为7.3,这表明基因转换可能比以前认为的更频繁。这些发现意味着,与疾病关联的研究在非洲人群中需要比在非非洲人群中更密集的多态性位点图谱。