炎症在儿童期短睡眠持续时间与青年期精神病中的作用。
Role of Inflammation in Short Sleep Duration Across Childhood and Psychosis in Young Adulthood.
机构信息
Institute for Mental Health, School of Psychology, University of Birmingham, Birmingham, United Kingdom.
Specialist Mood Disorders Clinic, Zinnia Centre, Birmingham, United Kingdom.
出版信息
JAMA Psychiatry. 2024 Aug 1;81(8):825-833. doi: 10.1001/jamapsychiatry.2024.0796.
IMPORTANCE
Short sleep duration over a prolonged period in childhood could have a detrimental impact on long-term mental health, including the development of psychosis. Further, potential underlying mechanisms of these associations remain unknown.
OBJECTIVE
To examine the association between persistent shorter nighttime sleep duration throughout childhood with psychotic experiences (PEs) and/or psychotic disorder (PD) at age 24 years and whether inflammatory markers (C-reactive protein [CRP] and interleukin 6 [IL-6]) potentially mediate any association.
DESIGN, SETTING, AND PARTICIPANTS: This cohort study used data from the Avon Longitudinal Study of Parents and Children. Data analysis was conducted from January 30 to August 1, 2023.
EXPOSURES
Nighttime sleep duration was collected at 6, 18, and 30 months and at 3.5, 4 to 5, 5 to 6, and 6 to 7 years.
MAIN OUTCOMES AND MEASURES
PEs and PD were assessed at age 24 years from the Psychosislike Symptoms Interview. CRP level at ages 9 and 15 years and IL-6 level at 9 years were used as mediators. Latent class growth analyses (LCGAs) were applied to detect trajectories of nighttime sleep duration, and logistic regressions were applied for the longitudinal associations between trajectories of nighttime sleep duration and psychotic outcomes at 24 years. Path analyses were applied to test CRP and IL-6 as potential mediators.
RESULTS
Data were available on 12 394 children (6254 female [50.5%]) for the LCGA and on 3962 young adults (2429 female [61.3%]) for the logistic regression and path analyses. The LCGA identified a group of individuals with persistent shorter nighttime sleep duration across childhood. These individuals were more likely to develop PD (odds ratio [OR], 2.50; 95% CI, 1.51-4.15; P < .001) and PEs (OR, 3.64; 95% CI, 2.23-5.95; P < .001) at age 24 years. Increased levels of IL-6 at 9 years, but not CRP at 9 or 15 years, partially mediated the associations between persistent shorter sleep duration and PD (bias-corrected estimate = 0.003; 95% CI, 0.002-0.005; P = .007) and PEs (bias-corrected estimate = 0.002; 95% CI, 0-0.003; P = .03) in young adulthood.
CONCLUSIONS AND RELEVANCE
Findings of this cohort study highlight the necessity of addressing short sleep duration in children, as persistence of this sleep problem was associated with subsequent psychosis. This study also provides preliminary evidence for future targeted interventions in children addressing both sleep and inflammatory responses.
重要性
儿童时期长期睡眠时间短可能对长期心理健康产生不利影响,包括精神病的发展。此外,这些关联的潜在潜在机制仍然未知。
目的
研究整个儿童期夜间睡眠时间持续较短与 24 岁时精神病体验(PEs)和/或精神病(PD)之间的关联,以及炎症标志物(C 反应蛋白[CRP]和白细胞介素 6 [IL-6])是否可能介导任何关联。
设计、地点和参与者:这项队列研究使用了来自雅芳纵向父母与子女研究的数据。数据分析于 2023 年 1 月 30 日至 8 月 1 日进行。
暴露
在 6、18 和 30 个月以及 3.5、4 至 5、5 至 6 和 6 至 7 岁时收集夜间睡眠时间。
主要结果和措施
在 24 岁时,使用精神病样症状访谈评估 PEs 和 PD。9 岁和 15 岁时的 CRP 水平和 9 岁时的 IL-6 水平被用作中介。应用潜在类别增长分析(LCGA)来检测夜间睡眠时间的轨迹,应用逻辑回归来检测夜间睡眠时间轨迹与 24 岁时精神病结局之间的纵向关联。应用路径分析来测试 CRP 和 IL-6 作为潜在的中介。
结果
12394 名儿童(6254 名女性[50.5%])可用于 LCGA,3962 名年轻人(2429 名女性[61.3%])可用于逻辑回归和路径分析。LCGA 确定了一组在整个儿童期持续睡眠时间较短的个体。这些人更有可能在 24 岁时患上 PD(优势比[OR],2.50;95%CI,1.51-4.15;P<.001)和 PEs(OR,3.64;95%CI,2.23-5.95;P<.001)。9 岁时 IL-6 水平升高,但 9 岁或 15 岁时 CRP 水平没有升高,部分介导了持续较短睡眠时间与 PD(偏置校正估计值=0.003;95%CI,0.002-0.005;P=0.007)和 PEs(偏置校正估计值=0.002;95%CI,0-0.003;P=0.03)之间的关联。
结论和相关性
这项队列研究的结果强调了在儿童中解决睡眠时间短的必要性,因为这种睡眠问题的持续存在与随后的精神病有关。这项研究还为未来针对儿童的睡眠和炎症反应的靶向干预提供了初步证据。
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