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抑制控制训练对短睡眠时表现型失眠症的益处:一项试点随机试验。

The benefit of inhibitory control training for insomnia with short sleep duration phenotype: a pilot randomized trial.

作者信息

Zhang Haobo, Lv Zhangwei, Chen Hanfei, Tang Zijie, Lei Xu

机构信息

Sleep and NeuroImaging Center, Faculty of Psychology, Southwest University, Chongqing, 400715, China.

Key Laboratory of Cognition and Personality (Southwest University), Ministry of Education, Chongqing, 400715, China.

出版信息

BMC Med. 2024 Dec 18;22(1):591. doi: 10.1186/s12916-024-03813-1.

Abstract

BACKGROUND

Two phenotypes of insomnia disorder (ID) have been identified based on objective total sleep duration (TST): one with short sleep duration (ISSD) and another with normal sleep duration (INSD). Recent proposals suggested that insomnia with objective short-sleep duration (TST < 7 h) is associated with impaired inhibitory function, leading to a dysregulation of cortical inhibition, which may underlie its prevalence. This study investigated the status of impaired response inhibition in these two phenotypes and examined the potential different effect of response inhibition training on these two phenotypes.

METHODS

Twenty-two healthy controls (HC) and eighty-one patients with ID were recruited, with IDs further categorized into ISSD and INSD (with TST ≥ 7 h). Clinical behavior measures, including the Pittsburgh Sleep Quality Index (PSQI), Insomnia Severity Index (ISI), Pre-sleep Arousal Scale (PSAS), objective sleep characteristics assessed by all-night sleep electroencephalography, and the accuracy of NoGo trials in the Go/NoGo task were compared among the three groups. Subsequently, within each ID phenotype, participants were divided into training and blank control sub-groups. The two training sub-groups completed Adaptive Go/NoGo training task (Through adaptive difficulty adjustment, the task trains participants' inhibitory control) 15 times over 3 weeks, and all IDs were assessed using sleep-related subjective and objective measures and Go/NoGo task before and after the intervention.

RESULTS

ISSD patients exhibited significantly longer sleep latency (p = 0.003) compared to HC, while wakefulness duration (p = 0.004) and light sleep duration (p < 0.001) were shorter than INSD. No significant differences in objective sleep characteristics were observed between INSD and HC. Following adaptive training, the ISSD training sub-group showed decreased scores in PSQI (p = 0.039) and ISI (p = 0.053) compared to their blank control sub-group. In the INSD groups, both training and blank control sub-groups demonstrated reductions in PSQI (p < 0.001), ISI (p < 0.001), and the cognitive arousal sub-dimension of the PSAS scores (p = 0.003) in the post-session test.

CONCLUSIONS

Impaired response inhibition is a characteristic of ISSD, potentially indicating dysfunctional cortical inhibition, whereas INSD pathogenesis may be related to cognitive-emotional arousal. Response inhibition training effectively alleviates sleep problems in ISSD. These findings provide new insights for developing precise intervention strategies in ID.

TRIAL REGISTRATION

The study was prospectively registered on May 30, 2024, in Chinese Clinical Trials registry (ChiCTR2400085063).

摘要

背景

基于客观总睡眠时间(TST)已确定失眠障碍(ID)的两种表型:一种是短睡眠时间(ISSD),另一种是正常睡眠时间(INSD)。最近的研究表明,客观短睡眠时间(TST < 7小时)的失眠与抑制功能受损有关,导致皮质抑制失调,这可能是其患病率的基础。本研究调查了这两种表型中反应抑制受损的状况,并检验了反应抑制训练对这两种表型可能产生的不同影响。

方法

招募了22名健康对照者(HC)和81名ID患者,ID患者进一步分为ISSD和INSD(TST≥7小时)。比较了三组的临床行为指标,包括匹兹堡睡眠质量指数(PSQI)、失眠严重程度指数(ISI)、睡前觉醒量表(PSAS)、通过整夜睡眠脑电图评估的客观睡眠特征以及Go/NoGo任务中NoGo试验的准确性。随后,在每个ID表型中,将参与者分为训练组和空白对照组。两个训练组在3周内完成15次自适应Go/NoGo训练任务(通过自适应难度调整,该任务训练参与者的抑制控制),所有ID患者在干预前后均使用与睡眠相关的主观和客观指标以及Go/NoGo任务进行评估。

结果

与HC相比,ISSD患者的睡眠潜伏期明显更长(p = 0.003),而清醒时间(p = 0.004)和浅睡眠持续时间(p < 0.001)比INSD患者短。INSD和HC之间在客观睡眠特征方面未观察到显著差异。经过自适应训练后,与空白对照组相比,ISSD训练组的PSQI(p = 0.039)和ISI(p = 0.053)得分降低。在INSD组中,训练组和空白对照组在训练后测试中的PSQI(p < 0.001)、ISI(p < 0.001)以及PSAS得分的认知觉醒子维度(p = 0.003)均有所降低。

结论

反应抑制受损是ISSD的一个特征,可能表明皮质抑制功能失调,而INSD的发病机制可能与认知 - 情绪唤醒有关。反应抑制训练有效缓解了ISSD患者的睡眠问题。这些发现为制定ID的精准干预策略提供了新的见解。

试验注册

该研究于2024年5月30日在中国临床试验注册中心(ChiCTR2400085063)进行前瞻性注册。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7078/11657586/1b3c9e85da2d/12916_2024_3813_Fig1_HTML.jpg

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