Westerman Kenneth E, Kilpeläinen Tuomas O, Sevilla-Gonzalez Magdalena, Connelly Margery A, Wood Alexis C, Tsai Michael Y, Taylor Kent D, Rich Stephen S, Rotter Jerome I, Otvos James D, Bentley Amy R, Mora Samia, Aschard Hugues, Rao D C, Gu Charles, Chasman Daniel I, Manning Alisa K
Clinical and Translational Epidemiology Unit, Massachusetts General Hospital, Boston, MA, USA.
Department of Medicine, Harvard Medical School, Boston, MA, USA.
medRxiv. 2024 Jan 24:2024.01.23.24301689. doi: 10.1101/2024.01.23.24301689.
Large-scale gene-environment interaction (GxE) discovery efforts often involve compromises in the definition of outcomes and choice of covariates for the sake of data harmonization and statistical power. Consequently, refinement of exposures, covariates, outcomes, and population subsets may be helpful to establish often-elusive replication and evaluate potential clinical utility. Here, we used additional datasets, an expanded set of statistical models, and interrogation of lipoprotein metabolism via nuclear magnetic resonance (NMR)-based lipoprotein subfractions to refine a previously discovered GxE modifying the relationship between physical activity (PA) and HDL-cholesterol (HDL-C). This GxE was originally identified by Kilpeläinen et al., with the strongest cohort-specific signal coming from the Women's Genome Health Study (WGHS). We thus explored this GxE further in the WGHS (N = 23,294), with follow-up in the UK Biobank (UKB; N = 281,380), and the Multi-Ethnic Study of Atherosclerosis (MESA; N = 4,587). Self-reported PA (MET-hrs/wk), genotypes at rs295849 (nearest gene: ), and NMR metabolomics data were available in all three cohorts. As originally reported, minor allele carriers of rs295849 in WGHS had a stronger positive association between PA and HDL-C ( = 0.002). When testing a range of NMR metabolites (primarily lipoprotein and lipid subfractions) to refine the HDL-C outcome, we found a stronger interaction effect on medium-sized HDL particle concentrations (M-HDL-P; = 1.0×10) than HDL-C. Meta-regression revealed a systematically larger interaction effect in cohorts from the original meta-analysis with a greater fraction of women ( = 0.018). In the UKB, GxE effects were stronger both in women and using M-HDL-P as the outcome. In MESA, the primary interaction for HDL-C showed nominal significance ( = 0.013), but without clear differences by sex and with a greater magnitude using large, rather than medium, HDL-P as an outcome. Towards reconciling these observations, further exploration leveraging NMR platform-specific HDL subfraction diameter annotations revealed modest agreement across all cohorts in the interaction affecting medium-to-large particles. Taken together, our work provides additional insights into a specific known gene-PA interaction while illustrating the importance of phenotype and model refinement towards understanding and replicating GxEs.
大规模基因-环境相互作用(GxE)的发现工作常常为了数据协调和统计效能而在结局定义和协变量选择上做出妥协。因此,细化暴露因素、协变量、结局和人群亚组可能有助于实现常常难以捉摸的重复验证,并评估潜在的临床实用性。在此,我们使用了额外的数据集、一组扩展的统计模型,并通过基于核磁共振(NMR)的脂蛋白亚组分对脂蛋白代谢进行分析,以细化先前发现的一种GxE,该GxE改变了体力活动(PA)与高密度脂蛋白胆固醇(HDL-C)之间的关系。这种GxE最初由基尔佩莱宁等人鉴定,最强的队列特异性信号来自女性基因组健康研究(WGHS)。因此,我们在WGHS(N = 23,294)中进一步探索了这种GxE,并在英国生物银行(UKB;N = 281,380)和多族裔动脉粥样硬化研究(MESA;N = 4,587)中进行了随访。所有三个队列都有自我报告的PA(代谢当量小时/周)、rs295849位点的基因型(最接近的基因: )以及NMR代谢组学数据。如最初报道的那样,WGHS中rs295849的次要等位基因携带者在PA与HDL-C之间有更强的正相关( = 0.002)。在测试一系列NMR代谢物(主要是脂蛋白和脂质亚组分)以细化HDL-C结局时,我们发现对中等大小HDL颗粒浓度(M-HDL-P; = 1.0×10)的相互作用效应比对HDL-C的更强。元回归显示,在原始荟萃分析中女性比例更高的队列中,相互作用效应系统性地更大( = 0.018)。在UKB中,GxE效应在女性中更强,并且以M-HDL-P作为结局时也是如此。在MESA中,HDL-C的主要相互作用显示出名义上的显著性( = 0.013),但按性别无明显差异,并且以大而非中等大小的HDL-P作为结局时效应量更大。为了协调这些观察结果,利用NMR平台特定的HDL亚组分直径注释进行的进一步探索揭示,在影响中等至大颗粒的相互作用方面,所有队列之间存在适度的一致性。综上所述,我们的工作为一种特定的已知基因-PA相互作用提供了更多见解,同时说明了表型和模型细化对于理解和重复验证GxEs的重要性。
