用于检测与定量表型相关的罕见变异的基因-环境相互作用的柯西组合方法。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2023-07-22 DOI:10.1038/s41437-023-00640-7
Xiaoqin Jin, Gang Shi
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引用次数: 0

摘要

基因-环境相互作用(GEIs)的表征可以为复杂疾病的生物学机制提供详细的见解。尽管最近人们对罕见变异的GEI感兴趣,但已发表的GEI测试对基因或区域中极少数罕见变异的因果关系缺乏动力。通过扩展聚合Cauchy关联检验(ACAT),我们提出了三种GEI检验来解决这个问题:具有固定主效应的Cauchy组合GEI检验(CCGEI-F)、具有随机主效应的Couchy组合GE检验(CCGE I-R)和综合Cauchy组合GE检验(CC GEI-O)。ACAT用于组合单变量GEI分析的p值,以获得CCGEI-F和CCGEI-R,并将多个GEI测试的p值组合在CCGEI-O中。通过数值模拟,对于少量的因果变量,CCGEI-F、CCGEI-R和CCGEI-O提供的功率比现有的GEI测试INT-FIX和INT-RAN高出约5%;然而,它们的功率略高于现有的GEI测试TOW-GE。对于大量的因果变异,尽管CCGEI-F和CCGEI-R表现出与竞争测试相当或略低的功率值,但结果仍然令人满意。在评估的所有模拟条件中,CCGEI-O提供的功率明显高于竞争的GEI测试。我们使用英国生物银行的全外显子组测序数据,进一步将GEI测试应用于收缩压或舒张压的全基因组分析,以检测基因-体重指数(BMI)的相互作用。提示显著性水平为1.0 × 通过我们的GEI测试,10-4、KCNC4、GAR1、FAM120AOS和NT5C3B显示出与BMI的相互作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Cauchy combination methods for the detection of gene–environment interactions for rare variants related to quantitative phenotypes
The characterization of gene–environment interactions (GEIs) can provide detailed insights into the biological mechanisms underlying complex diseases. Despite recent interest in GEIs for rare variants, published GEI tests are underpowered for an extremely small proportion of causal rare variants in a gene or a region. By extending the aggregated Cauchy association test (ACAT), we propose three GEI tests to address this issue: a Cauchy combination GEI test with fixed main effects (CCGEI-F), a Cauchy combination GEI test with random main effects (CCGEI-R), and an omnibus Cauchy combination GEI test (CCGEI-O). ACAT was applied to combine p values of single-variant GEI analyses to obtain CCGEI-F and CCGEI-R and p values of multiple GEI tests were combined in CCGEI-O. Through numerical simulations, for small numbers of causal variants, CCGEI-F, CCGEI-R and CCGEI-O provided approximately 5% higher power than the existing GEI tests INT-FIX and INT-RAN; however, they had slightly higher power than the existing GEI test TOW-GE. For large numbers of causal variants, although CCGEI-F and CCGEI-R exhibited comparable or slightly lower power values than the competing tests, the results were still satisfactory. Among all simulation conditions evaluated, CCGEI-O provided significantly higher power than that of competing GEI tests. We further applied our GEI tests in genome-wide analyses of systolic blood pressure or diastolic blood pressure to detect gene–body mass index (BMI) interactions, using whole-exome sequencing data from UK Biobank. At a suggestive significance level of 1.0 × 10−4, KCNC4, GAR1, FAM120AOS and NT5C3B showed interactions with BMI by our GEI tests.
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