Li-Tempel Ting, Larra Mauro F, Sandt Estelle, Mériaux Sophie B, Schote Andrea B, Schächinger Hartmut, Muller Claude P, Turner Jonathan D
Department of Neurobehavioral Genetics, Research Institute of Psychobiology, University of Trier, 54290 Trier, Germany.
Department of Clinical Physiology, Research Institute of Psychobiology, University of Trier, 54290 Trier, Germany.
Clin Epigenetics. 2016 Jan 28;8:12. doi: 10.1186/s13148-016-0180-y. eCollection 2016.
Gender, genetic makeup, and prior experience interact to determine physiological responses to an external perceived stressor. Here, we investigated the contribution of both genetic variants and promoter methylation of the NR3C1 (glucocorticoid receptor) gene to the cardiovascular and hypothalamus-pituitary-adrenal (HPA) axis response to the socially evaluated cold pressor test (seCPT).
Two hundred thirty-two healthy participants were recruited and underwent the experiment. They were randomly assigned to either the seCPT group (cold water) or a control group (warm water). The seCPT group had a clear stress reaction; salivary cortisol levels and peak systolic and diastolic blood pressure all increased significantly compared to the control group. GR genotype (TthIIII, NR3C1-I, 1H, E22E, R23K, BclI and 9beta) and methylation data were obtained from 218 participants. Haplotypes were built from the GR genotypes, and haplotype 2 (minor allele of BclI) carriers had a higher cortisol response to the seCPT in comparison to non-carriers (20.77 ± 13.22; 14.99 ± 8.42; p = 0.034), as well as independently of the experimental manipulation, higher baseline heart rate (72.44 ± 10.99; 68.74 ± 9.79; p = 0.022) and blood pressure (115.81 ± 10.47; 111.61 ± 10.74; p = 0.048). Average methylation levels throughout promoter 1F and 1H were low (2.76 and 1.69 %, respectively), but there was a strong correlation between individual CpGs and the distance separating them (Pearson's correlation r = 0.725, p = 3.03 × 10(-26)). Higher promoter-wide methylation levels were associated with decreased baseline blood pressure, and when incorporated into a linear mixed effect model significantly predicted lower systolic and diastolic blood pressure evolution over time in response to the experimental manipulation. The underlying genotype significantly predicted methylation levels; particularly, the homozygous BclI minor allele was associated with higher methylation in promoter 1H (p = 0.042).
This is one of the first studies linking epigenetic modifications of the GR promoter, receptor genotype and physiological measures of the stress response. At baseline, there were clear genetic and epigenetic effects on blood pressure. The seCPT induced a strong cardiovascular and HPA axis response, and both systems were affected by the functional genetic variants, although methylation also predicted blood pressure reactivity. The return to baseline was predominantly influenced by the genomic sequence. Overall, the physiological response to the seCPT is controlled by an exquisite mix of genetic and epigenetic factors.
性别、基因组成和既往经历相互作用,共同决定机体对外部感知应激源的生理反应。在此,我们研究了NR3C1(糖皮质激素受体)基因的遗传变异和启动子甲基化对社会评估冷加压试验(seCPT)的心血管及下丘脑 - 垂体 - 肾上腺(HPA)轴反应的影响。
招募了232名健康参与者并进行实验。他们被随机分为seCPT组(冷水)或对照组(温水)。seCPT组出现明显的应激反应;与对照组相比,唾液皮质醇水平、收缩压峰值和舒张压均显著升高。从218名参与者中获取了GR基因型(TthIIII、NR3C1 - I、1H、E22E、R23K、BclI和9beta)及甲基化数据。根据GR基因型构建单倍型,与非携带者相比,单倍型2(BclI的次要等位基因)携带者对seCPT的皮质醇反应更高(20.77 ± 13.22;14.99 ± 8.42;p = 0.034),并且独立于实验操作,其基线心率更高(72.44 ± 10.99;68.74 ± 9.79;p = 0.022),血压也更高(115.81 ± 10.47;111.61 ± 10.74;p = 0.048)。整个启动子1F和1H的平均甲基化水平较低(分别为2.76%和1.69%),但各个CpG之间及其间距存在强相关性(Pearson相关系数r = 0.725,p = 3.03×10(-26))。较高的启动子整体甲基化水平与较低的基线血压相关,当纳入线性混合效应模型时,显著预测了随着实验操作时间推移收缩压和舒张压的降低。潜在基因型显著预测甲基化水平;特别是,BclI次要等位基因纯合子与启动子1H中较高的甲基化相关(p = 0.042)。
这是首批将GR启动子的表观遗传修饰、受体基因型与应激反应的生理指标联系起来的研究之一。在基线时,血压存在明显的遗传和表观遗传效应。seCPT诱导了强烈的心血管和HPA轴反应,尽管甲基化也预测了血压反应性,但两个系统均受功能基因变异的影响。恢复到基线主要受基因组序列影响。总体而言,对seCPT的生理反应受遗传和表观遗传因素的精妙组合控制。
Zotero 插件
