Efficiency of trans-ethnic genome-wide meta-analysis and fine-mapping

被引:0
|
作者
Rick Twee-Hee Ong
Xu Wang
Xuanyao Liu
Yik-Ying Teo
机构
[1] Saw Swee Hock School of Public Health,Department of Statistics and Applied Probability
[2] National University of Singapore,undefined
[3] NUS Graduate School for Integrative Science and Engineering,undefined
[4] National University of Singapore,undefined
[5] Life Sciences Institute,undefined
[6] National University of Singapore,undefined
[7] Faculty of Science,undefined
[8] National University of Singapore,undefined
[9] Genome Institute of Singapore,undefined
[10] Agency for Science,undefined
[11] Technology and Research,undefined
来源
European Journal of Human Genetics | 2012年 / 20卷
关键词
linkage disequilibrium; genome-wide association study; meta-analysis; fine-mapping;
D O I
暂无
中图分类号
学科分类号
摘要
Genome-wide association studies have seen unprecedented success in identifying genetic loci that correlate with disease susceptibility and severity. Early phases of these studies have predominantly been performed in the Caucasian populations. The next phase in medical genetics is to extend the exploration across genetically diverse populations to leverage on larger sample sizes for locating smaller effects that may be present in most human populations. However, discoveries from these studies do not actually reveal the underlying functional changes to the human genome, but only point to broad regions stipulated by the extent of linkage disequilibrium (LD). Fine-mapping the functional variants can, however, be hampered by extensive LD, which can yield multiple perfect surrogates that are not distinguishable from the underlying causal variants, although several studies have illustrated the value of relying on multiple genetically diverse populations to narrow the candidate regions where the functional variants can be found in. Here, we explore the efficiency of trans-ethnic meta-analysis in discovering genetic association and in fine-mapping the causal variants by asking: are there any population diversity metrics that will be useful for: (i) identifying the populations or genomic regions where meta-analysis are likely to be more successful for discovering associations?; (ii) identifying the populations or loci to perform deep targeted sequencing for the purpose of fine-mapping causal variants? Our results indicate that simple metrics like the FST or the population specificity of haplotypes are useful in trans-ethnic meta-analyses, while the degree of haplotype sharing and LD variation are informative of the efficiency in trans-ethnic fine-mapping.
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页码:1300 / 1307
页数:7
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