首页> 外文会议>Eighth Pacific Symposium on Biocomputing (PSB), Jan 3-7, 2003, Kauai, Hawaii >JOINT BAYESIAN ESTIMATION OF MUTATION LOCATION AND AGE USING LINKAGE DISEQUILIBRIUM
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JOINT BAYESIAN ESTIMATION OF MUTATION LOCATION AND AGE USING LINKAGE DISEQUILIBRIUM

机译:使用链接不平衡性的突变位置和年龄的联合贝叶斯估计

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摘要

Associations between disease and marker alleles on chromosomes in populations can arise as a consequence of historical forces such as mutation, selection and genetic drift, and is referred to as "linkage disequilibrium" (LD). LD can be used to estimate the map position of a disease mutation relative to a set of linked markers, as well as to estimate other parameters of interest, such as mutation age. Parametric methods for estimating the location of a disease mutation using marker linkage disequilibrium in a sample of normal and affected individuals require a detailed knowledge of population demography, and in particular require users to specify the postulated age of a mutation and past population growth rates. A new Bayesian method is presented for jointly estimating the position of a disease mutation and its age. The method is illustrated using haplotype data for the cystic fibrosis ΔF508 mutation in europe and the DTD mutation in Finland. It is shown that, for these datasets, the posterior probability distribution of disease mutation location is insensitive to the population growth rate when the model is averaged over possible mutation ages using a prior probability distribution for the mutation age based on the population frequency of the disease mutation. Fewer assumptions are therefore needed for parametric LD mapping.
机译:疾病和种群中染色体上的标记等位基因之间的关联可能是由诸如突变,选择和遗传漂移之类的历史力量引起的,被称为“连锁不平衡”(LD)。 LD可用于估计疾病突变相对于一组链接标记的图谱位置,以及估计其他感兴趣的参数,例如突变年龄。使用正常和受影响个体样本中的标记连锁不平衡来估计疾病突变位置的参数方法需要对人口人口统计学有详细的了解,特别是要求用户指定突变的假定年龄和过去的人口增长率。提出了一种新的贝叶斯方法,用于联合估计疾病突变的位置及其年龄。使用单倍型数据对欧洲的囊性纤维化ΔF508突变和芬兰的DTD突变进行了说明。结果表明,对于这些数据集,当使用基于疾病人群频率的突变年龄先验概率分布对模型进行可能的突变年龄平均时,疾病突变位置的后验概率分布对种群增长率不敏感。突变。因此,参数LD映射需要更少的假设。

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