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再探非24小时睡眠-清醒障碍——一项病例研究

Non-24-Hour Sleep-Wake Disorder Revisited - A Case Study.

作者信息

Garbazza Corrado, Bromundt Vivien, Eckert Anne, Brunner Daniel P, Meier Fides, Hackethal Sandra, Cajochen Christian

机构信息

Centre for Chronobiology, Psychiatric Hospital of the University of Basel, Basel, Switzerland; Transfaculty Research Platform Molecular and Cognitive Neurosciences, University of Basel, Basel, Switzerland.

Sleep-Wake-Epilepsy-Centre, Department of Neurology, Inselspital, Bern University Hospital , Bern , Switzerland.

出版信息

Front Neurol. 2016 Feb 29;7:17. doi: 10.3389/fneur.2016.00017. eCollection 2016.

Abstract

The human sleep-wake cycle is governed by two major factors: a homeostatic hourglass process (process S), which rises linearly during the day, and a circadian process C, which determines the timing of sleep in a ~24-h rhythm in accordance to the external light-dark (LD) cycle. While both individual processes are fairly well characterized, the exact nature of their interaction remains unclear. The circadian rhythm is generated by the suprachiasmatic nucleus ("master clock") of the anterior hypothalamus, through cell-autonomous feedback loops of DNA transcription and translation. While the phase length (tau) of the cycle is relatively stable and genetically determined, the phase of the clock is reset by external stimuli ("zeitgebers"), the most important being the LD cycle. Misalignments of the internal rhythm with the LD cycle can lead to various somatic complaints and to the development of circadian rhythm sleep disorders (CRSD). Non-24-hour sleep-wake disorders (N24HSWD) is a CRSD affecting up to 50% of totally blind patients and characterized by the inability to maintain a stable entrainment of the typically long circadian rhythm (tau > 24.5 h) to the LD cycle. The disease is rare in sighted individuals and the pathophysiology less well understood. Here, we present the case of a 40-year-old sighted male, who developed a misalignment of the internal clock with the external LD cycle following the treatment for Hodgkin's lymphoma (ABVD regimen, four cycles and AVD regimen, four cycles). A thorough clinical assessment, including actigraphy, melatonin profiles and polysomnography led to the diagnosis of non-24-hour sleep-wake disorders (N24HSWD) with a free-running rhythm of tau = 25.27 h. A therapeutic intervention with bright light therapy (30 min, 10,000 lux) in the morning and melatonin administration (0.5-0.75 mg) in the evening failed to entrain the free-running rhythm, although a longer treatment duration and more intense therapy might have been successful. The sudden onset and close timely connection led us to hypothesize that the chemotherapy might have caused a mutation of the molecular clock components leading to the observed elongation of the circadian period.

摘要

人类的睡眠 - 觉醒周期受两个主要因素支配:一个是稳态沙漏过程(过程S),它在白天呈线性上升;另一个是昼夜节律过程C,它根据外部明暗(LD)周期以约24小时的节律决定睡眠的时间。虽然这两个独立的过程都有相当明确的特征,但它们相互作用的确切性质仍不清楚。昼夜节律由下丘脑前部的视交叉上核(“主时钟”)通过DNA转录和翻译的细胞自主反馈回路产生。虽然周期的相位长度(tau)相对稳定且由基因决定,但时钟的相位会被外部刺激(“授时因子”)重置,其中最重要的是LD周期。内部节律与LD周期的失调会导致各种躯体不适,并引发昼夜节律睡眠障碍(CRSD)。非24小时睡眠 - 觉醒障碍(N24HSWD)是一种CRSD,影响高达50%的全盲患者,其特征是无法将通常较长的昼夜节律(tau > 24.5小时)稳定地与LD周期同步。这种疾病在有视力的个体中很少见,其病理生理学也了解得较少。在此,我们报告一例40岁有视力的男性病例,该患者在接受霍奇金淋巴瘤治疗(ABVD方案,四个周期和AVD方案,四个周期)后,其内部时钟与外部LD周期出现失调。通过包括活动记录仪、褪黑素谱分析和多导睡眠图在内的全面临床评估,诊断为非24小时睡眠 - 觉醒障碍(N24HSWD),其自由运行节律的tau = 25.27小时。尽管延长治疗时间和采用更强的治疗可能会成功,但早晨进行30分钟、10000勒克斯的强光治疗以及晚上给予褪黑素(0.5 - 0.75毫克)的治疗干预未能使自由运行节律同步。突然发病以及紧密的时间关联使我们推测化疗可能导致了分子时钟组件的突变,从而导致观察到的昼夜周期延长。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7965/4770037/d7112da2d8df/fneur-07-00017-g001.jpg

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