使用高斯混合模型的基因型拷贝数变化:理论和算法。

IF 0.8 4区 数学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Statistical Applications in Genetics and Molecular Biology Pub Date : 2012-10-12 DOI:10.1515/1544-6115.1725
Chang-Yun Lin, Yungtai Lo, Kenny Q Ye
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引用次数: 7

摘要

拷贝数变异(CNVs)在疾病关联研究中很重要,并且通常是为GWAS研究开发的最新微阵列平台的靶标。然而,针对相同CNV区域的探针在性能上可能会有很大差异,其中一些探针除了纯粹的噪声之外几乎没有携带任何信息。本文研究了在高斯混合模型(GMM)框架下,如何最好地结合多个探针的测量值来估计个体的拷贝数。首先,我们证明了在两种规则条件下,假设除混合比例外的所有参数都已知,可以获得最优权重,从而使基于加权平均的单变量GMM与多变量GMM给出完全相同的分类。然后,我们开发了一种迭代估计参数并获得最优权重的算法,并将其用于分类。该算法在模拟数据和两组真实数据上表现良好,明显优于基于等加权平均的分类方法。
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Genotype copy number variations using Gaussian mixture models: theory and algorithms.

Copy number variations (CNVs) are important in the disease association studies and are usually targeted by most recent microarray platforms developed for GWAS studies. However, the probes targeting the same CNV regions could vary greatly in performance, with some of the probes carrying little information more than pure noise. In this paper, we investigate how to best combine measurements of multiple probes to estimate copy numbers of individuals under the framework of Gaussian mixture model (GMM). First we show that under two regularity conditions and assume all the parameters except the mixing proportions are known, optimal weights can be obtained so that the univariate GMM based on the weighted average gives the exactly the same classification as the multivariate GMM does. We then developed an algorithm that iteratively estimates the parameters and obtains the optimal weights, and uses them for classification. The algorithm performs well on simulation data and two sets of real data, which shows clear advantage over classification based on the equal weighted average.

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来源期刊
Statistical Applications in Genetics and Molecular Biology
Statistical Applications in Genetics and Molecular Biology BIOCHEMISTRY & MOLECULAR BIOLOGY-MATHEMATICAL & COMPUTATIONAL BIOLOGY
自引率
11.10%
发文量
8
期刊介绍: Statistical Applications in Genetics and Molecular Biology seeks to publish significant research on the application of statistical ideas to problems arising from computational biology. The focus of the papers should be on the relevant statistical issues but should contain a succinct description of the relevant biological problem being considered. The range of topics is wide and will include topics such as linkage mapping, association studies, gene finding and sequence alignment, protein structure prediction, design and analysis of microarray data, molecular evolution and phylogenetic trees, DNA topology, and data base search strategies. Both original research and review articles will be warmly received.
期刊最新文献
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