Effects of low-dose acetylsalicylic acid on the inflammatory response to experimental sleep restriction in healthy humans

IF 8.8 2区 医学 Q1 IMMUNOLOGY
Larissa C. Engert , Carola Ledderose , Careen Biniamin , Paola Birriel , Olivia Buraks , Bryan Chatterton , Rammy Dang , Surya Daniel , Annika Eske , Taylor Reed , Ava Tang , Suzanne M. Bertisch , Janet M. Mullington , Wolfgang G. Junger , Monika Haack
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引用次数: 0

Abstract

Background

Sleep deficiencies, such as manifested in short sleep duration or insomnia symptoms, are known to increase the risk for multiple disease conditions involving immunopathology. Inflammation is hypothesized to be a mechanism through which deficient sleep acts as a risk factor for these conditions. Thus, one potential way to mitigate negative health consequences associated with deficient sleep is to target inflammation. Few interventional sleep studies investigated whether improving sleep affects inflammatory processes, but results suggest that complementary approaches may be necessary to target inflammation associated with sleep deficiencies. We investigated whether targeting inflammation through low-dose acetylsalicylic acid (ASA, i.e., aspirin) is able to blunt the inflammatory response to experimental sleep restriction.

Methods

46 healthy participants (19F/27M, age range 19–63 years) were studied in a double-blind randomized placebo-controlled crossover trial with three protocols each consisting of a 14-day at-home monitoring phase followed by an 11-day (10-night) in-laboratory stay (sleep restriction/ASA, sleep restriction/placebo, control sleep/placebo). In the sleep restriction/ASA condition, participants took low-dose ASA (81 mg/day) daily in the evening (22:00) during the at-home phase and the subsequent in-laboratory stay. In the sleep restriction/placebo and control sleep/placebo conditions, participants took placebo daily. Each in-laboratory stay started with 2 nights with a sleep opportunity of 8 h/night (23:00–07:00) for adaptation and baseline measurements. Under the two sleep restriction conditions, participants were exposed to 5 nights of sleep restricted to a sleep opportunity of 4 h/night (03:00–07:00) followed by 3 nights of recovery sleep with a sleep opportunity of 8 h/night. Under the control sleep condition, participants had a sleep opportunity of 8 h/night throughout the in-laboratory stay. During each in-laboratory stay, participants had 3 days of intensive monitoring (at baseline, 5th day of sleep restriction/control sleep, and 2nd day of recovery sleep). Variables, including pro-inflammatory immune cell function, C-reactive protein (CRP), and actigraphy-estimated measures of sleep, were analyzed using generalized linear mixed models.

Results

Low-dose ASA administration reduced the interleukin (IL)-6 expression in LPS-stimulated monocytes (p<0.05 for condition*day) and reduced serum CRP levels (p<0.01 for condition) after 5 nights of sleep restriction compared to placebo administration in the sleep restriction condition. Low-dose ASA also reduced the amount of cyclooxygenase (COX)-1/COX-2 double positive cells among LPS-stimulated monocytes after 2 nights of recovery sleep following 5 nights of sleep restriction compared to placebo (p<0.05 for condition). Low-dose ASA further decreased wake after sleep onset (WASO) and increased sleep efficiency (SE) during the first 2 nights of recovery sleep (p<0.001 for condition and condition*day). Baseline comparisons revealed no differences between conditions for all of the investigated variables (p>0.05 for condition).

Conclusion

This study shows that inflammatory responses to sleep restriction can be reduced by preemptive administration of low-dose ASA. This finding may open new therapeutic approaches to prevent or control inflammation and its consequences in those experiencing sleep deficiencies.

Trial Registration

ClinicalTrials.gov NCT03377543.

小剂量乙酰水杨酸对健康人实验性睡眠限制的炎症反应的影响。
背景:众所周知,睡眠不足(如睡眠时间短或失眠症状)会增加罹患多种涉及免疫病理的疾病的风险。据推测,炎症是睡眠不足作为这些疾病风险因素的一种机制。因此,缓解与睡眠不足相关的负面健康后果的一个潜在方法就是针对炎症。很少有干预性睡眠研究调查改善睡眠是否会影响炎症过程,但研究结果表明,针对与睡眠不足有关的炎症可能需要补充性方法。我们研究了通过低剂量乙酰水杨酸(ASA,即阿司匹林)来消除炎症是否能够减轻睡眠不足对健康的影响、方法:46 名健康参与者(19 名女性/27 名男性,年龄 19-63 岁)在一项双盲随机安慰剂对照交叉试验中接受了研究,该试验有三个方案,每个方案包括 14 天的居家监测阶段,然后是 11 天(10 夜)的实验室住院治疗(睡眠限制/ASA、睡眠限制/安慰剂、对照睡眠/安慰剂)。在睡眠限制/ASA 条件下,参与者在在家监测阶段和随后的实验室住院期间,每天傍晚(22:00)服用低剂量 ASA(81 毫克/天)。在限制睡眠/安慰剂和控制睡眠/安慰剂条件下,参与者每天服用安慰剂。每次在实验室停留时,都会有 2 个晚上的睡眠时间为 8 小时/晚(23:00-07:00),以便进行适应和基线测量。在两种睡眠限制条件下,参试者要接受 5 个晚上的睡眠限制,睡眠时间为 4 小时/晚(03:00-07:00),然后是 3 个晚上的恢复性睡眠,睡眠时间为 8 小时/晚。在对照睡眠条件下,参与者在整个实验室停留期间的睡眠时间为 8 小时/晚。每次在实验室停留期间,参与者都要接受 3 天的强化监测(基线、睡眠限制/控制睡眠的第 5 天和恢复睡眠的第 2 天)。使用广义线性混合模型分析了包括促炎免疫细胞功能、C反应蛋白(CRP)和动图估算的睡眠测量值在内的变量:结果:服用小剂量 ASA 可减少 LPS 刺激的单核细胞中白细胞介素(IL)-6 的表达(各条件下的 P 均为 0.05):本研究表明,预先服用低剂量的ASA可减少睡眠限制引起的炎症反应。这一发现可能为预防或控制睡眠不足患者的炎症及其后果提供了新的治疗方法:试验注册:ClinicalTrials.gov NCT03377543。
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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来源期刊
CiteScore
29.60
自引率
2.00%
发文量
290
审稿时长
28 days
期刊介绍: Established in 1987, Brain, Behavior, and Immunity proudly serves as the official journal of the Psychoneuroimmunology Research Society (PNIRS). This pioneering journal is dedicated to publishing peer-reviewed basic, experimental, and clinical studies that explore the intricate interactions among behavioral, neural, endocrine, and immune systems in both humans and animals. As an international and interdisciplinary platform, Brain, Behavior, and Immunity focuses on original research spanning neuroscience, immunology, integrative physiology, behavioral biology, psychiatry, psychology, and clinical medicine. The journal is inclusive of research conducted at various levels, including molecular, cellular, social, and whole organism perspectives. With a commitment to efficiency, the journal facilitates online submission and review, ensuring timely publication of experimental results. Manuscripts typically undergo peer review and are returned to authors within 30 days of submission. It's worth noting that Brain, Behavior, and Immunity, published eight times a year, does not impose submission fees or page charges, fostering an open and accessible platform for scientific discourse.
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