Variability in perinatal sleep quality is associated with an atypical cortisol awakening response and increased mood symptoms.

IF 3.4 2区医学 Q2 ENDOCRINOLOGY & METABOLISM Psychoneuroendocrinology Pub Date : 2024-11-23 DOI:10.1016/j.psyneuen.2024.107248

Michele L Okun, Suzanne Segerstrom, Susan Jackman, Kharah Ross, Christine Dunkel Schetter, Mary Coussons-Read

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Abstract

Objective: Pregnancy is often typified with a decrease in sleep quality, which for many women, progressively worsens across gestation and into the postpartum. A mechanism linking poor sleep with certain adverse pregnancy outcomes is dysregulation of the HPA axis resulting in atypically elevated cortisol production. While total cortisol output normally increases across pregnancy, the cortisol awakening response (CAR), a response to waking up, is influenced by factors such as stress and mood. It attenuates as pregnancy progresses, with normalization in the first weeks after delivery. The goals of the present study were to (1) assess the temporal relationship between sleep quality and cortisol indices across the perinatal period; (2) evaluate whether sleep quality was associated with postpartum mood; and (3) assess whether cortisol mediated these associations.

Method: Data were collected as part of the Healthy Babies Before Birth (HB3) study. Sleep quality, depressive and anxiety symptoms, and cortisol from four time-points (8-16 weeks gestation, 30-36 weeks gestation, 6 months postpartum, and 1-year postpartum) were assessed. Participants (N = 223) who had sleep quality (PSQI) and cortisol data from at least 1 of 4 time-points were included in analyses. Three salivary cortisol indices were calculated: cortisol awakening response (CAR), diurnal slope, and area under the curve (AUC). Multi-level models were run to predict cortisol parameters based on deviations and typical maternal sleep quality at each wave as well as mood outcomes.

Results: Multilevel (time, wave, and person) modeling indicated that sleep quality was not associated with any of the cortisol indices, and none significantly varied across time. However, when PSQI scores were higher than the woman's own mean sleep quality, the CAR slope was steeper (+1 point in PSQI, γ=0.18), and when PSQI scores were lower than mean, the CAR slope was flatter (-1 point, γ=0.11). Poorer sleep quality was associated with greater depression severity (γ = 0.367) and anxiety symptoms (γ = 0.120). Cortisol did not mediate the relationship between sleep quality and depression symptoms.

Discussion: Increases in PSQI scores, but not higher mean PSQI scores, were associated with a larger CAR. There was no association between sleep quality and the diurnal slope or AUC. These data suggest that variability in sleep quality is significantly associated with the amount of cortisol secreted upon awakening.

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围产期睡眠质量的可变性与非典型皮质醇唤醒反应和情绪症状增加有关。

目的：怀孕通常以睡眠质量下降为典型，对许多妇女来说，睡眠质量在怀孕期间和产后逐渐恶化。睡眠不佳与某些不良妊娠结局之间的联系机制是下丘脑轴调节失调，导致皮质醇分泌异常升高。虽然总皮质醇分泌量在怀孕期间通常会增加，但皮质醇唤醒反应（CAR），一种对醒来的反应，受到压力和情绪等因素的影响。随着妊娠的进展，它逐渐减弱，在分娩后的最初几周恢复正常。本研究的目的是(1)评估围产儿睡眠质量与皮质醇指数之间的时间关系；(2)评估睡眠质量是否与产后情绪相关；(3)评估皮质醇是否介导了这些关联。方法：数据收集作为出生前健康婴儿（HB3）研究的一部分。从四个时间点（妊娠8-16周、妊娠30-36周、产后6个月和产后1年）评估睡眠质量、抑郁和焦虑症状以及皮质醇。4个时间点中至少1个时间点的睡眠质量（PSQI）和皮质醇数据的参与者（N = 223）被纳入分析。计算三个唾液皮质醇指数：皮质醇唤醒反应（CAR）、日斜率和曲线下面积（AUC）。运行多层次模型来预测基于偏差和每波典型母亲睡眠质量以及情绪结果的皮质醇参数。结果：多水平（时间、波和人）模型表明，睡眠质量与任何皮质醇指数都没有关联，而且没有显著的时间变化。然而，当PSQI得分高于女性自身平均睡眠质量时，CAR斜率更陡（PSQI得分+1点，γ=0.18），当PSQI得分低于平均值时，CAR斜率更平坦（-1点，γ=0.11）。睡眠质量较差与抑郁严重程度（γ = 0.367）和焦虑症状（γ = 0.120）相关。皮质醇没有调节睡眠质量和抑郁症状之间的关系。讨论：PSQI评分的增加，而不是PSQI平均评分的增加，与较大的CAR相关。睡眠质量与昼夜斜率或AUC之间没有关联。这些数据表明，睡眠质量的变化与醒来时分泌的皮质醇量显著相关。

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

Psychoneuroendocrinology 医学-精神病学

CiteScore

7.40

自引率

8.10%

发文量

268

审稿时长

66 days

期刊介绍： Psychoneuroendocrinology publishes papers dealing with the interrelated disciplines of psychology, neurobiology, endocrinology, immunology, neurology, and psychiatry, with an emphasis on multidisciplinary studies aiming at integrating these disciplines in terms of either basic research or clinical implications. One of the main goals is to understand how a variety of psychobiological factors interact in the expression of the stress response as it relates to the development and/or maintenance of neuropsychiatric illnesses.