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全基因组方法发现了受生活方式调节的心血管健康的新型遗传和非遗传方差组分。

Whole-Genome Approach Discovers Novel Genetic and Nongenetic Variance Components Modulated by Lifestyle for Cardiovascular Health.

机构信息

Australian Centre for Precision Health University of South Australia Adelaide South Australia Australia.

South Australian Health and Medical Research Institute Adelaide South Australia Australia.

出版信息

J Am Heart Assoc. 2020 Apr 21;9(8):e015661. doi: 10.1161/JAHA.119.015661. Epub 2020 Apr 20.

Abstract

Background Both genetic and nongenetic factors can predispose individuals to cardiovascular risk. Finding ways to alter these predispositions is important for cardiovascular disease prevention. Methods and Results We used a novel whole-genome approach to estimate the genetic and nongenetic effects on-and hence their predispositions to-cardiovascular risk and determined whether they vary with respect to lifestyle factors such as physical activity, smoking, alcohol consumption, and dietary intake. We performed analyses on the ARIC (Atherosclerosis Risk in Communities) Study (N=6896-7180) and validated findings using the UKBB (UK Biobank, N=14 076-34 538). Lifestyle modulation was evident for many cardiovascular traits such as body mass index and resting heart rate. For example, alcohol consumption modulated both genetic and nongenetic effects on body mass index, whereas smoking modulated nongenetic effects on heart rate, pulse pressure, and white blood cell count. We also stratified individuals according to estimated genetic and nongenetic effects that are modulated by lifestyle factors and showed distinct phenotype-lifestyle relationships across the stratified groups. Finally, we showed that neglecting lifestyle modulations of cardiovascular traits would on average reduce single nucleotide polymorphism heritability estimates of these traits by a small yet significant amount, primarily owing to the overestimation of residual variance. Conclusions Lifestyle changes are relevant to cardiovascular disease prevention. Individual differences in the genetic and nongenetic effects that are modulated by lifestyle factors, as shown by the stratified group analyses, implies a need for personalized lifestyle interventions. In addition, single nucleotide polymorphism-based heritability of cardiovascular traits without accounting for lifestyle modulations could be underestimated.

摘要

背景 遗传和非遗传因素都可能使个体易患心血管疾病风险。寻找改变这些易感性的方法对于预防心血管疾病很重要。

方法和结果 我们使用一种新的全基因组方法来估计遗传和非遗传因素对心血管风险的影响,从而确定它们是否与生活方式因素(如体力活动、吸烟、饮酒和饮食摄入)有关。我们对 ARIC(社区动脉粥样硬化风险)研究(N=6896-7180)进行了分析,并使用 UKBB(英国生物银行,N=14 076-34 538)对结果进行了验证。生活方式的调节对许多心血管特征都有明显影响,如体重指数和静息心率。例如,饮酒对体重指数的遗传和非遗传影响都有调节作用,而吸烟对心率、脉压和白细胞计数的非遗传影响有调节作用。我们还根据遗传和非遗传因素受生活方式因素调节的程度对个体进行了分层,并在分层组中显示了不同的表型-生活方式关系。最后,我们表明,忽视对心血管特征的生活方式调节,平均会导致这些特征的单核苷酸多态性遗传度估计值降低很小但显著的量,这主要是由于剩余方差的高估。

结论 生活方式的改变与心血管疾病的预防有关。生活方式因素调节的遗传和非遗传效应的个体差异,如分层组分析所示,意味着需要个性化的生活方式干预。此外,如果不考虑生活方式的调节,基于单核苷酸多态性的心血管特征遗传度可能会被低估。

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