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Combined linkage disequilibrium and linkage mapping: Bayesian multilocus approach

机译:组合连锁不平衡和连锁映射:贝叶斯多场所方法

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Quantitative trait loci (QTL) affecting the phenotype of interest can be detected using linkage analysis (LA), linkage disequilibrium (LD) mapping or a combination of both (LDLA). The LA approach uses information from recombination events within the observed pedigree and LD mapping from the historical recombinations within the unobserved pedigree. We propose the Bayesian variable selection approach for combined LDLA analysis for single-nucleotide polymorphism (SNP) data. The novel approach uses both sources of information simultaneously as is commonly done in plant and animal genetics, but it makes fewer assumptions about population demography than previous LDLA methods. This differs from approaches in human genetics, where LDLA methods use LA information conditional on LD information or the other way round. We argue that the multilocus LDLA model is more powerful for the detection of phenotype-genotype associations than single-locus LDLA analysis. To illustrate the performance of the Bayesian multilocus LDLA method, we analyzed simulation replicates based on real SNP genotype data from small three-generational CEPH families and compared the results with commonly used quantitative transmission disequilibrium test (QTDT). This paper is intended to be conceptual in the sense that it is not meant to be a practical method for analyzing high-density SNP data, which is more common. Our aim was to test whether this approach can function in principle.
机译:可以使用连锁分析(LA),连锁不平衡(LD)作图或二者结合(LDLA)来检测影响目标表型的数量性状基因座(QTL)。 LA方法使用来自观察到的谱系内重组事件的信息以及来自未观察到的谱系内历史重组的LD映射。我们提出用于单核苷酸多态性(SNP)数据的组合LDLA分析的贝叶斯变量选择方法。这种新颖的方法同时使用了两种信息源,这在动植物遗传学中是很常见的,但是与以前的LDLA方法相比,它对人口人口统计学的假设更少。这与人类遗传学中的方法不同,在人类遗传学中,LDLA方法使用以LD信息为条件的LA信息,反之亦然。我们认为,多基因座LDLA模型比单基因座LDLA分析对表型-基因型关联的检测更强大。为了说明贝叶斯多基因座LDLA方法的性能,我们基于来自三代CEPH小家族的真实SNP基因型数据分析了模拟重复,并将结果与​​常用的定量透射不平衡测试(QTDT)进行了比较。本文的目的是概念性的,并不意味着它是一种分析更为常见的高密度SNP数据的实用方法。我们的目的是测试这种方法是否原则上可以起作用。

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