Fine-mapping across diverse ancestries drives the discovery of putative causal variants underlying human complex traits and diseases

IF 31.7 1区 生物学 Q1 GENETICS & HEREDITY
Kai Yuan, Ryan J. Longchamps, Antonio F. Pardiñas, Mingrui Yu, Tzu-Ting Chen, Shu-Chin Lin, Yu Chen, Max Lam, Ruize Liu, Yan Xia, Zhenglin Guo, Wenzhao Shi, Chengguo Shen, The Schizophrenia Workgroup of Psychiatric Genomics Consortium, Mark J. Daly, Benjamin M. Neale, Yen-Chen A. Feng, Yen-Feng Lin, Chia-Yen Chen, Michael C. O’Donovan, Tian Ge, Hailiang Huang
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Abstract

Genome-wide association studies (GWAS) of human complex traits or diseases often implicate genetic loci that span hundreds or thousands of genetic variants, many of which have similar statistical significance. While statistical fine-mapping in individuals of European ancestry has made important discoveries, cross-population fine-mapping has the potential to improve power and resolution by capitalizing on the genomic diversity across ancestries. Here we present SuSiEx, an accurate and computationally efficient method for cross-population fine-mapping. SuSiEx integrates data from an arbitrary number of ancestries, explicitly models population-specific allele frequencies and linkage disequilibrium patterns, accounts for multiple causal variants in a genomic region and can be applied to GWAS summary statistics. We comprehensively assessed the performance of SuSiEx using simulations. We further showed that SuSiEx improves the fine-mapping of a range of quantitative traits available in both the UK Biobank and Taiwan Biobank, and improves the fine-mapping of schizophrenia-associated loci by integrating GWAS across East Asian and European ancestries. The cross-population Sum of Single Effects (SuSiEx) model is a robust and computationally efficient method for conducting multi-ancestry fine-mapping of genome-wide association signals, producing smaller credible sets and capturing population-specific causal variants.

Abstract Image

Abstract Image

对不同祖先的精细图谱绘制推动了人类复杂性状和疾病的潜在因果变异的发现。
对人类复杂性状或疾病进行的全基因组关联研究(GWAS)往往涉及到数百或数千个基因变异的遗传位点,其中许多变异具有相似的统计意义。虽然欧洲血统个体的统计精细图谱已经取得了重要发现,但跨人群精细图谱有可能通过利用不同血统的基因组多样性来提高研究效率和分辨率。在这里,我们介绍一种精确且计算效率高的跨人群精细图谱绘制方法--SuSiEx。SuSiEx 整合了来自任意数量祖先的数据,明确地模拟了特定人群的等位基因频率和连锁不平衡模式,考虑了基因组区域中的多个因果变异,并可应用于 GWAS 的汇总统计。我们通过模拟全面评估了 SuSiEx 的性能。我们进一步表明,SuSiEx 改善了英国生物库和台湾生物库中一系列数量性状的精细图谱,并通过整合东亚和欧洲血统的 GWAS 改善了精神分裂症相关位点的精细图谱。
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来源期刊
Nature genetics
Nature genetics 生物-遗传学
CiteScore
43.00
自引率
2.60%
发文量
241
审稿时长
3 months
期刊介绍: Nature Genetics publishes the very highest quality research in genetics. It encompasses genetic and functional genomic studies on human and plant traits and on other model organisms. Current emphasis is on the genetic basis for common and complex diseases and on the functional mechanism, architecture and evolution of gene networks, studied by experimental perturbation. Integrative genetic topics comprise, but are not limited to: -Genes in the pathology of human disease -Molecular analysis of simple and complex genetic traits -Cancer genetics -Agricultural genomics -Developmental genetics -Regulatory variation in gene expression -Strategies and technologies for extracting function from genomic data -Pharmacological genomics -Genome evolution
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