中年后期缓解期早发性与晚发性抑郁症患者睡眠期间心率变异性特征不同。
Different heart rate variability profile during sleep in mid-later life adults with remitted early-onset versus late-onset depression.
机构信息
School of Psychology, Faculty of Science, University of Sydney, Sydney, NSW, Australia; Healthy Brain Ageing Program, Brain and Mind Centre, University of Sydney, Camperdown, NSW 2050, Australia; Charles Perkins Centre, University of Sydney, Camperdown, NSW 2050, Australia; CogSleep, Australian National Health and Medical Research Council Centre of Research Excellence, Australia.
School of Psychology, Faculty of Science, University of Sydney, Sydney, NSW, Australia; Healthy Brain Ageing Program, Brain and Mind Centre, University of Sydney, Camperdown, NSW 2050, Australia.
出版信息
J Affect Disord. 2024 Aug 1;358:175-182. doi: 10.1016/j.jad.2024.04.054. Epub 2024 May 1.
BACKGROUND
In mid-later life adults, early-onset and late-onset (i.e., onset ≥50 years) depression appear to be underpinned by different pathophysiology yet have not been examined in relation to autonomic function. Sleep provides an opportunity to examine the autonomic nervous system as the physiology changes across the night. Hence, we aimed to explore if autonomic profile is altered in mid-later life adults with remitted early-onset, late-onset and no history of lifetime depression.
METHODS
Participants aged 50-90 years (n = 188) from a specialised clinic underwent a comprehensive clinical assessment and completed an overnight polysomnography study. General Linear Models were used to examine the heart rate variability differences among the three groups for four distinct sleep stages and the wake after sleep onset. All analyses controlled for potential confounders - age, sex, current depressive symptoms and antidepressant usage.
RESULTS
For the wake after sleep onset, mid-later life adults with remitted early-onset depression had reduced standard deviation of Normal to Normal intervals (SDNN; p = .014, d = -0.64) and Shannon Entropy (p = .004, d = -0.46,) than those with no history of lifetime depression. Further, the late-onset group showed a reduction in high-frequency heart rate variability (HF during non-rapid eye movement sleep stage 2 (N2; p = .005, d = -0.53) and non-rapid eye movement sleep stage 3 (N3; p = .009, d = -0.55) when compared to those with no lifetime history.
LIMITATIONS
Causality between heart rate variability and depression cannot be derived in this cross-sectional study. Longitudinal studies are needed to examine the effects remitted depressive episodes on autonomic function.
CONCLUSION
The findings suggest differential autonomic profile for remitted early-onset and late-onset mid-later life adults during sleep stages and wake periods. The differences could potentially serve as peripheral biomarkers in conjunction with more disease-specific markers of depression to improve diagnosis and prognosis.
背景
在中老年人群中,早发性和晚发性(即发病年龄≥50 岁)抑郁症似乎有不同的病理生理学基础,但尚未针对自主功能进行研究。睡眠为研究自主神经系统提供了机会,因为生理机能会在整个夜晚发生变化。因此,我们旨在探索在缓解期的早发性、晚发性和无终生抑郁史的中老年人群中,自主功能谱是否发生改变。
方法
来自专门诊所的年龄在 50-90 岁的参与者(n=188)接受了全面的临床评估,并完成了一整夜的多导睡眠图研究。使用一般线性模型来检查三组在四个不同的睡眠阶段和睡眠后觉醒期间的心率变异性差异。所有分析均控制了潜在的混杂因素——年龄、性别、当前抑郁症状和抗抑郁药的使用。
结果
对于睡眠后觉醒,缓解期的早发性抑郁中老年人群的正常到正常间期标准差(SDNN;p=.014,d=-0.64)和香农熵(p=.004,d=-0.46)均低于无终生抑郁史者。此外,晚发性组在非快速眼动睡眠阶段 2(N2;p=.005,d=-0.53)和非快速眼动睡眠阶段 3(N3;p=.009,d=-0.55)期间的高频心率变异性(HF)降低与无终生史者相比。
局限性
在这项横断面研究中,不能从因果关系上得出心率变异性和抑郁症之间的关系。需要进行纵向研究来检查缓解期抑郁发作对自主功能的影响。
结论
这些发现表明,在睡眠阶段和觉醒期间,缓解期的早发性和晚发性中老年人群的自主功能谱存在差异。这些差异可能作为外周生物标志物,与更具特异性的抑郁疾病标志物相结合,以改善诊断和预后。
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