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首页> 外文期刊>Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation >Improved Use of Small Reference Panels for Conditional and Joint Analysis with GWAS Summary Statistics
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Improved Use of Small Reference Panels for Conditional and Joint Analysis with GWAS Summary Statistics

机译:改进使用小型参考面板进行GWAS摘要统计的条件和联合分析

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摘要

Due to issues of practicality and confidentiality of genomic data sharing on a large scale, typically only meta- or mega-analyzed genome-wide association study (GWAS) summary data, not individual-level data, are publicly available. Reanalyses of such GWAS summary data for a wide range of applications have become more and more common and useful, which often require the use of an external reference panel with individual-level genotypic data to infer linkage disequilibrium (LD) among genetic variants. However, with a small sample size in only hundreds, as for the most popular 1000 Genomes Project European sample, estimation errors for LD are not negligible, leading to often dramatically increased numbers of false positives in subsequent analyses of GWAS summary data. To alleviate the problem in the context of association testing for a group of SNPs, we propose an alternative estimator of the covariance matrix with an idea similar to multiple imputation. We use numerical examples based on both simulated and real data to demonstrate the severe problem with the use of the 1000 Genomes Project reference panels, and the improved performance of our new approach.
机译:由于大规模共享基因组数据的实用性和机密性问题,通常只有公开进行了荟萃分析或巨型分析的全基因组关联研究(GWAS)摘要数据,而不是个人级别的数据。对此类GWAS摘要数据进行重新分析以用于广泛的应用已变得越来越普遍和有用,这通常需要使用具有单个水平基因型数据的外部参考面板来推断遗传变异之间的连锁不平衡(LD)。但是,对于只有数百个样本的小样本样本(对于最受欢迎的1000个欧洲基因组计划欧洲样本)而言,LD的估计误差是不可忽略的,从而导致在随后的GWAS摘要数据分析中误报的数量通常会急剧增加。为了缓解针对一组SNP的关联测试中的问题,我们提出了一种协方差矩阵的替代估计量,其思路类似于多重插补。我们使用基于模拟和真实数据的数值示例来说明使用1000个基因组计划参考面板的严重问题以及新方法的改进性能。

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