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肌强直性营养不良 1 型患者睡眠-觉醒连续性中断:超越传统睡眠分期。

Disruption of sleep-wake continuum in myotonic dystrophy type 1: Beyond conventional sleep staging.

机构信息

Department of Clinical and Experimental Medicine, Neurology Unit, University of Pisa, Pisa, Italy.

Department of Clinical and Experimental Medicine, Neurology Unit, University of Pisa, Pisa, Italy.

出版信息

Neuromuscul Disord. 2018 May;28(5):414-421. doi: 10.1016/j.nmd.2018.02.004. Epub 2018 Feb 12.

Abstract

Sleep disruption and excessive daytime sleepiness are well recognised symptoms in myotonic dystrophy type 1 (DM1), where a central dysfunction of sleep-wake regulation may play a pivotal role. Few studies evaluated sleep macrostructure in DM1, but none investigated more refined sleep variables. Eight DM1 patients (6 male, aged 20-50 years) and 10 healthy controls (7 male, aged 22-67 years) underwent nocturnal polysomnography and multiple sleep latency test. Sleep stages and events were scored according to standard criteria; sleep microstructure was analyzed through cyclic alternating pattern. Relative and absolute delta powers were computed for whole non REM and each non REM period. DM1 patients showed increased REM sleep and decreased N2. N3, although not significantly, was increased. Three patients, but no controls, had sleep-onset REM period in nocturnal sleep. DM1 patients showed slower delta power dissipation across the night, and increased sleep instability (CAP rate). Multiple sleep latency tests showed shorter sleep latencies, five patients presenting at least one sleep-onset REM period and, when including also night sleep, two sleep-onset REM periods. Our data confirm a narcoleptic-like phenotype in DM1 with a prominent REM sleep dysregulation, that may account for daytime sleepiness, together with increased sleep instability and impaired delta power dissipation that seem peculiar of the disease.

摘要

睡眠中断和日间过度嗜睡是肌强直性营养不良 1 型(DM1)的典型症状,其中睡眠-觉醒调节的中枢功能障碍可能起着关键作用。少数研究评估了 DM1 的睡眠宏观结构,但没有研究更精细的睡眠变量。8 名 DM1 患者(6 名男性,年龄 20-50 岁)和 10 名健康对照者(7 名男性,年龄 22-67 岁)接受了夜间多导睡眠图和多次睡眠潜伏期试验。睡眠阶段和事件根据标准标准进行评分;通过循环交替模式分析睡眠微结构。计算了整个非快速眼动和每个非快速眼动期的相对和绝对 delta 功率。DM1 患者的 REM 睡眠增加,N2 减少。N3 虽然没有显著增加,但有所增加。有 3 名患者,但没有对照者,在夜间睡眠中出现睡眠开始时 REM 期。DM1 患者表现出夜间 delta 功率消散较慢,睡眠不稳定性增加(CAP 率)。多次睡眠潜伏期试验显示睡眠潜伏期缩短,5 名患者至少出现一次睡眠开始时 REM 期,包括夜间睡眠时,2 名患者出现两次睡眠开始时 REM 期。我们的数据证实了 DM1 中存在类似于发作性睡病的表型,其特征是 REM 睡眠失调,这可能导致日间嗜睡,同时伴有睡眠不稳定性增加和 delta 功率消散受损,这似乎是该疾病的特有表现。

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