连锁不平衡
遗传力
生物
遗传建筑学
单核苷酸多态性
SNP公司
遗传学
选择(遗传算法)
回归
联动装置(软件)
遗传关联
进化生物学
数量性状位点
统计
基因
基因型
计算机科学
人工智能
数学
作者
Steven Gazal,Hilary K. Finucane,Nicholas A. Furlotte,Po‐Ru Loh,Pier Francesco Palamara,Xuanyao Liu,Armin Schoech,Brendan Bulik‐Sullivan,Benjamin M. Neale,Alexander Gusev,Alkes L. Price
出处
期刊:Nature Genetics
[Nature Portfolio]
日期:2017-09-11
卷期号:49 (10): 1421-1427
被引量:583
摘要
Recent work has hinted at the linkage disequilibrium (LD)-dependent architecture of human complex traits, where SNPs with low levels of LD (LLD) have larger per-SNP heritability. Here we analyzed summary statistics from 56 complex traits (average N = 101,401) by extending stratified LD score regression to continuous annotations. We determined that SNPs with low LLD have significantly larger per-SNP heritability and that roughly half of this effect can be explained by functional annotations negatively correlated with LLD, such as DNase I hypersensitivity sites (DHSs). The remaining signal is largely driven by our finding that more recent common variants tend to have lower LLD and to explain more heritability (P = 2.38 × 10-104); the youngest 20% of common SNPs explain 3.9 times more heritability than the oldest 20%, consistent with the action of negative selection. We also inferred jointly significant effects of other LD-related annotations and confirmed via forward simulations that they jointly predict deleterious effects.
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