Disturbance of sleep maintenance, but not sleep duration, activates nuclear factor-κB and signal transducer and activator of transcription family proteins in older adults: sex differences.

IF 5.3 2区医学 Q1 CLINICAL NEUROLOGY

Sleep Pub Date : 2023-10-11 DOI:10.1093/sleep/zsad130

Dominique Piber, Richard Olmstead, Joshua H Cho, Michael R Irwin

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引用次数: 0

Abstract

Study objectives: Disturbances of sleep maintenance and sleep duration are common in older adults and associated with an increased risk for age-related mortality and morbidity. Converging evidence implicates inflammation as an underlying mechanism, especially in females. However, it is unknown what specific aspects of sleep disturbance impact inflammatory mechanisms in older adults.

Methods: Using data from community-dwelling older adults who participated in the Sleep Health and Aging Research (SHARE) field study (n = 262, mean age 71.9 ± 8.0 years), we conducted a secondary analysis to examine whether disturbance of sleep maintenance (i.e. greater amount of wake time after sleep onset [WASO]) and sleep duration (i.e. shorter total sleep time [TST]) assessed by sleep diary and actigraphy are associated with greater activation of nuclear factor (NF)-κB and signal transducer and activator of transcription (STAT) family proteins STAT1, STAT3, and STAT5 in peripheral blood monocytic cells. In addition, moderation effects of sex were explored.

Results: Data were available for sleep diary (n = 82), actigraphy (n = 74), and inflammatory signaling and transcriptional measures (n = 132). As assessed by sleep diary, greater amount of WASO (β = 0.39, p < 0.01), but not TST, was associated with higher levels of NF-κB. Whereas diary-assessed sleep measures were not associated with STAT family proteins, a moderation analysis revealed that greater diary-assessed WASO was associated with higher levels of STAT1 (p < 0.05), STAT3 (p < 0.05), and STAT5 (p < 0.01) in females, but not in males. Actigraphy-assessed sleep measures were not associated either with NF-κB or STAT activation.

Conclusions: In older adults, self-reported disturbance of sleep maintenance assessed by sleep diary was uniquely associated with higher levels of NF-κB, along with higher levels of STAT family proteins in females, but not in males. Our data suggest that improvingself-reported sleep maintenance might mitigate age-related increases in inflammatory signaling and transcriptional pathways, possibly more strongly in females, with the potential to reduce mortality risk in older adults.

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睡眠维持障碍，而不是睡眠持续时间，激活老年人的核因子-κB和信号转导子和转录激活子家族蛋白：性别差异。

研究目的：睡眠维持和睡眠持续时间的紊乱在老年人中很常见，并与年龄相关的死亡率和发病率的增加有关。集中的证据表明炎症是一种潜在的机制，尤其是在女性中。然而，尚不清楚睡眠障碍的哪些具体方面会影响老年人的炎症机制。方法：采用参与睡眠健康与老龄化研究（SHARE）现场研究的社区老年人（n=262，平均年龄71.9±8.0岁）的数据，我们进行了二次分析，以检查通过睡眠日记和活动描记术评估的睡眠维持障碍（即睡眠开始后较长的唤醒时间[WASO]）和睡眠持续时间（即较短的总睡眠时间[TST]）是否与核因子（NF）-κB和信号转导子和转录激活子（STAT）家族蛋白STAT1、STAT3、，以及外周血单核细胞中的STAT5。此外，还探讨了性别的调节效应。结果：睡眠日记（n=82）、活动描记术（n=74）以及炎症信号和转录测量（n=132）的数据可用。根据睡眠日记评估，更多的WASO（β=0.39，p<0.01），而不是TST，与更高水平的NF-κB相关。尽管日记评估的睡眠测量与STAT家族蛋白无关，但一项适度分析显示，日记评估的WASO越大，女性的STAT1（p<0.05）、STAT3（p<0.05）和STAT5（p<0.01）水平越高，而男性则不然。行为学评估的睡眠指标与NF-κB或STAT的激活无关。结论：在老年人中，通过睡眠日记评估的自我报告的睡眠维持障碍与女性较高水平的NF-κB以及较高水平的STAT家族蛋白独特相关，但在男性中没有。我们的数据表明，即兴报告的睡眠维持可能会缓解与年龄相关的炎症信号和转录途径的增加，在女性中可能更为强烈，并有可能降低老年人的死亡率。

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

Sleep 医学-临床神经学

CiteScore

10.10

自引率

10.70%

发文量

1134

审稿时长

3 months

期刊介绍： SLEEP® publishes findings from studies conducted at any level of analysis, including: Genes Molecules Cells Physiology Neural systems and circuits Behavior and cognition Self-report SLEEP® publishes articles that use a wide variety of scientific approaches and address a broad range of topics. These may include, but are not limited to: Basic and neuroscience studies of sleep and circadian mechanisms In vitro and animal models of sleep, circadian rhythms, and human disorders Pre-clinical human investigations, including the measurement and manipulation of sleep and circadian rhythms Studies in clinical or population samples. These may address factors influencing sleep and circadian rhythms (e.g., development and aging, and social and environmental influences) and relationships between sleep, circadian rhythms, health, and disease Clinical trials, epidemiology studies, implementation, and dissemination research.