Toll样受体4(TLR4)甲基化与酒精摄入之间的相互作用对酒精输注主观反应的影响
Interactions between TLR4 methylation and alcohol consumption on subjective responses to an alcohol infusion.
作者信息
Karoly Hollis C, Ellingson Jarrod M, Hutchison Kent E
机构信息
Department of Psychology and Neuroscience, University of Colorado Boulder, UCB 344, Boulder, CO, USA.
出版信息
Alcohol Alcohol. 2018 Nov 1;53(6):650-658. doi: 10.1093/alcalc/agy046.
AIMS
Converging evidence has implicated perturbed inflammatory signaling in alcohol use disorders (AUDs), and both animal and human studies suggest that alcohol-induced inflammatory signaling is mediated by Toll-Like Receptor 4 (TLR4). We previously demonstrated that TLR4 is hypermethylated in subjects with AUD compared to control individuals. Examining the relationship between TLR4 methylation and subjective alcohol responses could shed light on the role of TLR4 in promoting AUDs, thereby highlighting its potential as a treatment target.
SHORT SUMMARY
Significant interactions were demonstrated between Toll-like Receptor 4 (TLR4) methylation and human alcohol consumption patterns, such that greater methylation was associated with decreased positive and negative self-reported arousal during an alcohol infusion among light-to-moderate drinkers, but increased self-reported positive arousal and physiological arousal (i.e. systolic blood pressure) among heavy drinkers.
METHODS
Latent growth models were used to examine the relationship between TLR4 methylation and subjective responses and physiological measures of arousal during an alcohol infusion across 222 drinkers.
RESULTS
We observed significant interactions of TLR4 methylation and alcohol use (drinks per week) on intercepts for self-report and physiological arousal measures. Specifically, light-to-moderate drinkers had positive associations between methylation and stimulation and tension (r's = 0.21-0.24), and heavy drinkers had negative associations (r's = -0.15 to -0.21). There were also significant interaction effects on changes in tension (β = 0.31, P < 0.01), systolic blood pressure (β = 0.74, P < 0.01) and marginal effects on stimulation (β = 0.15, P = 0.07) during the infusion, such that methylation was associated with decreased arousal among light-to-moderate drinkers (r's = -0.12 to -0.25) but stable or increased arousal among heavy drinkers (r's = 0.05-0.19).
CONCLUSIONS
Findings suggest that the relationship between TLR4 methylation and subjective and physiological arousal during acute alcohol intoxication depends upon on self-reported alcohol use. These data demonstrate the influence of TLR4 on subjective responses to alcohol, thereby supporting the need for further research on its potential as a pharmacological treatment target.
目的
越来越多的证据表明炎症信号紊乱与酒精使用障碍(AUDs)有关,动物和人体研究均表明酒精诱导的炎症信号由Toll样受体4(TLR4)介导。我们之前证明,与对照个体相比,AUD患者的TLR4存在高甲基化。研究TLR4甲基化与主观酒精反应之间的关系,有助于揭示TLR4在促进AUDs中的作用,从而突出其作为治疗靶点的潜力。
简短总结
研究表明Toll样受体4(TLR4)甲基化与人类饮酒模式之间存在显著相互作用,即甲基化程度越高,轻度至中度饮酒者在酒精输注期间自我报告的正向和负向唤醒水平越低,但重度饮酒者自我报告的正向唤醒水平和生理唤醒水平(即收缩压)越高。
方法
使用潜在增长模型研究222名饮酒者TLR4甲基化与酒精输注期间主观反应和唤醒生理指标之间的关系。
结果
我们观察到TLR4甲基化与酒精使用量(每周饮酒量)在自我报告和生理唤醒指标截距上存在显著相互作用。具体而言,轻度至中度饮酒者的甲基化与刺激和紧张感呈正相关(r值 = 0.21 - 0.24),而重度饮酒者呈负相关(r值 = -0.15至-0.21)。在输注期间,紧张感变化(β = 0.31,P < 0.01)、收缩压(β = 0.74,P < 0.01)以及刺激的边际效应(β = 0.15,P = 0.07)也存在显著交互作用,即甲基化与轻度至中度饮酒者的唤醒水平降低相关(r值 = -0.12至-0.25),但与重度饮酒者的唤醒水平稳定或升高相关(r值 = 0.05 - 0.19)。
结论
研究结果表明,急性酒精中毒期间TLR4甲基化与主观和生理唤醒之间的关系取决于自我报告的饮酒情况。这些数据证明了TLR4对酒精主观反应的影响,从而支持对其作为药物治疗靶点的潜力进行进一步研究的必要性。
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