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A Biologically Informed Method for Detecting Associations with Rare Variants

机译:一种检测稀有变异的关联的生物学方法

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With the recent flood of genome sequence data, there has been increasing interest in rare variants and methods to detect their association to disease. Many of these methods are collapsing strategies which bin rare variants based on allele frequency and functional predictions; but at this point, most have been limited to candidate gene studies with a small number of candidate genes. We propose a novel method to collapse rare variants based on incorporating biological information from the public domain. This paper introduces the functionality of BioBin, a biologically informed method to collapse rare variants and detect associations with a particular phenotype. We tested BioBin using low coverage data from the 1000 Genomes Project and discovered appropriate binning characteristics based on what one might expect given the size of the gene. We also tested BioBin using the pilot targeted exome data from 1000 Genomes Project. We used biologically-informed binning and differences in minor allele frequencies as a means to distinguish between two ancestral populations. Although BioBin is still in developmental stages, it will be a useful tool in analyzing sequence data and uncovering novel associations with complex disease.
机译:随着最近的基因组序列数据泛滥,人们越来越关注稀有变体和检测其与疾病相关性的方法。这些方法中有许多是折叠策略,它们基于等位基因频率和功能预测将稀有变异体进行分类。但是在这一点上,大多数研究仅限于具有少量候选基因的候选基因研究。我们提出了一种新方法,该方法基于合并来自公共领域的生物信息来折叠稀有变体。本文介绍了BioBin的功能,这是一种生物学上可知的方法,可以折叠稀有变体并检测与特定表型的关联。我们使用来自1000个基因组计划的低覆盖率数据对BioBin进行了测试,并根据给定基因大小的预期发现了适当的分箱特征。我们还使用来自1000个基因组计划的目标靶向外显子组数据测试了BioBin。我们使用生物学信息分类和较小等位基因频率的差异作为区分两个祖先种群的手段。尽管BioBin仍处于开发阶段,但它将是分析序列数据和发现与复杂疾病的新型关联的有用工具。

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