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Consistent sleep onset and maintenance of body weight after weight loss: An analysis of data from the NoHoW trial

机译:减重后,一致的睡眠发作和体重维持:从Nohow试验中的数据分析

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Background Several studies have suggested that reduced sleep duration and quality are associated with an increased risk of obesity and related metabolic disorders, but the role of sleep in long-term weight loss maintenance (WLM) has not been thoroughly explored using prospective data. Methods and findings The present study is an ancillary study based on data collected on participants from the Navigating to a Healthy Weight (NoHoW) trial, for which the aim was to test the efficacy of an evidence-based digital toolkit, targeting self-regulation, motivation, and emotion regulation, on WLM among 1,627 British, Danish, and Portuguese adults. Before enrolment, participants had achieved a weight loss of ≥5% and had a BMI of ≥25 kg/m2 prior to losing weight. Participants were enrolled between March 2017 and March 2018 and followed during the subsequent 12-month period for change in weight (primary trial outcome), body composition, metabolic markers, diet, physical activity, sleep, and psychological mediators/moderators of WLM (secondary trial outcomes). For the present study, a total of 967 NoHoW participants were included, of which 69.6% were women, the mean age was 45.8 years (SD 11.5), the mean baseline BMI was 29.5 kg/m2 (SD 5.1), and the mean weight loss prior to baseline assessments was 11.4 kg (SD 6.4). Objectively measured sleep was collected using the Fitbit Charge 2 (FC2), from which sleep duration, sleep duration variability, sleep onset, and sleep onset variability were assessed across 14 days close to baseline examinations. The primary outcomes were 12-month changes in body weight (BW) and body fat percentage (BF%). The secondary outcomes were 12-month changes in obesity-related metabolic markers (blood pressure, low- and high-density lipoproteins [LDL and HDL], triglycerides [TGs], and glycated haemoglobin [HbA1c]). Analysis of covariance and multivariate linear regressions were conducted with sleep-related variables as explanatory and subsequent changes in BW, BF%, and metabolic markers as response variables. We found no evidence that sleep duration, sleep duration variability, or sleep onset were associated with 12-month weight regain or change in BF%. A higher between-day variability in sleep onset, assessed using the standard deviation across all nights recorded, was associated with weight regain (0.55 kg per hour [95% CI 0.10 to 0.99]; P = 0.016) and an increase in BF% (0.41% per hour [95% CI 0.04 to 0.78]; P = 0.031). Analyses of the secondary outcomes showed that a higher between-day variability in sleep duration was associated with an increase in HbA1c (0.02% per hour [95% CI 0.00 to 0.05]; P = 0.045). Participants with a sleep onset between 19:00 and 22:00 had the greatest reduction in diastolic blood pressure (DBP) (P = 0.02) but also the most pronounced increase in TGs (P = 0.03). The main limitation of this study is the observational design. Hence, the observed associations do not necessarily reflect causal effects. Conclusion Our results suggest that maintaining a consistent sleep onset is associated with improved WLM and body composition. Sleep onset and variability in sleep duration may be associated with subsequent change in different obesity-related metabolic markers, but due to multiple-testing, the secondary exploratory outcomes should be interpreted cautiously. Trial registration The trial was registered with the ISRCTN registry (ISRCTN88405328).
机译:背景技术若干研究表明,减少睡眠持续时间和质量与肥胖症和相关代谢障碍的风险增加有关,但睡眠在长期减肥维护(WLM)中的作用尚未使用预期数据彻底探索。方法和结果目前的研究是基于参与者从导航到健康重量(NOHOW)试验的数据的数据的辅助研究,目的是测试基于证据的数字工具包的疗效,目标是自我监管的效果,动机和情感监管,在英国人,丹麦语和葡萄牙人的1,627名中,WLM。在注册之前,参与者在减轻重量之前达到了≥5%的体重减轻≥5%,并且在减肥之前具有≥25kg/ m2的BMI。参与者于2017年3月至2018年3月之间注册,并在随后的12个月期间进行重量变化(初级审判结果),身体成分,代谢标志物,饮食,身体活动,睡眠和心理介质/主持人的WLM(二级试验结果)。对于目前的研究,共有967名诺什参与者包括,其中69.6%是女性,平均年龄为45.8岁(SD 11.5),平均基线BMI为29.5 kg / m2(SD 5.1),平均重量基线评估前的损失为11.4公斤(SD 6.4)。使用Fitbit Charge 2(FC2)收集客观测量的睡眠,从中休眠持续时间,睡眠持续时间可变性,睡眠发作和睡眠发作可变性,接近基线检查的14天。主要结果是体重(BW)和体脂百分比(BF%)的12个月变化。二次结果是肥胖相关的代谢标记(血压,低密度和高密度脂蛋白[LDL和HDL],甘油三酯[TGS]和糖化血红蛋白[HBA1C])的12个月改变。通过与睡眠相关的变量进行协方差和多变量线性回归的分析,作为BW,BF%和代谢标记的解释性和随后的变化作为响应变量。我们发现没有证据表明睡眠持续时间,睡眠持续时间可变性或睡眠发作与12个月的重量重新获得或改变BF%相关。在记录的所有夜晚评估的睡眠发作中的白天变异性较高,与重量恢复有关(0.55kg /小时0.5%[95%CI 0.10至0.99]; p = 0.016),Bf%增加(每小时0.41%[95%CI 0.04至0.78]; P = 0.031)。二次结果的分析表明,睡眠持续时间之间的较高变异性与HBA1C的增加有关(0.02%/小时[95%CI 0.00至0.05]; P = 0.045)。睡眠发放的参与者在19:00至22:00之间的舒张压(DBP)的最大减少(P = 0.02),但也是TGS最明显的增加(P = 0.03)。本研究的主要限制是观察设计。因此,观察到的关联不一定反映因果效应。结论我们的研究结果表明,维持一致的睡眠发作与改善的WLM和身体组成相关。睡眠起来和睡眠持续时间的可变性可能与随后的不同肥胖相关的代谢标记的随后变化相关,但由于多次测试,次要探索结果应谨慎地解释。试用注册试验在ISRCTN注册表(ISRCTN88405328)中注册。

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