Respiratory Arousal Threshold in Patients with Epilepsy and Obstructive Sleep Apnea.

IF 3.4 2区医学 Q2 CLINICAL NEUROLOGY

Nature and Science of Sleep Pub Date : 2025-08-08 eCollection Date: 2025-01-01 DOI:10.2147/NSS.S535940

Ting-Wei Liao, Chun-Wei Chang, Mei-Yun Cheng, Tony Wu, Ning-Hung Chen, Shih-Wei Lin, Li-Pang Chuang

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Abstract

Background: Patients with epilepsy (PWE) have a higher likelihood of developing obstructive sleep apnea (OSA). However, limited literature investigates the phenotypes of OSA in this population. This study aimed to evaluate the respiratory arousal threshold (rAT) in PWE with concurrent OSA.

Methods: Patients were recruited from the Sleep and Epilepsy Center at Chang Gung Memorial Hospital between January 2010 and June 2022. We included adult patients who underwent overnight in-laboratory polysomnography after the onset of epilepsy. Additionally, age-, sex-, and apnea-hypopnea index (AHI)-matched patients with OSA only were included as controls. Low rAT was defined using predictive models based on polysomnography criteria.

Results: We enrolled 48 PWE, of whom 36 (75%) had concurrent OSA (PWE+OSA), and 108 patients with OSA only. PWE+OSA were older upon PSG examination and had a later epilepsy onset compared to PWE only. PWE had more concomitant antiseizure medications and hypnotics compared to patients with OSA only. Among those with OSA, 19 (52.8%) with PWE+OSA and 68 (63.0%) with OSA only were predicted to have a low rAT. Continuous positive airway pressure compliance was significantly lower in the low rAT subgroup compared to the high rAT subgroup (p = 0.021) within the OSA-only group, whereas no significant difference was observed between rAT subgroups in the PWE+OSA group.

Conclusion: Our study provides insights into the presence of a low rAT in PWE+OSA, with no significant difference in its ratio compared to OSA controls. However, since rAT was estimated using a predictive model rather than direct measurement, this limitation may affect the interpretation of our findings. Further studies using gold-standard methods are needed to clarify the underlying mechanisms contributing to the higher OSA prevalence in PWE.

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癫痫和阻塞性睡眠呼吸暂停患者的呼吸唤醒阈值。

背景：癫痫患者（PWE）发展为阻塞性睡眠呼吸暂停（OSA）的可能性较高。然而，有限的文献调查OSA在这一人群中的表型。本研究旨在评估PWE并发OSA患者的呼吸唤醒阈值（rAT）。方法：2010年1月至2022年6月从长庚纪念医院睡眠与癫痫中心招募患者。我们纳入了癫痫发作后接受夜间实验室多导睡眠描记术的成年患者。此外，年龄、性别和呼吸暂停低通气指数（AHI）匹配的OSA患者被纳入对照组。使用基于多导睡眠图标准的预测模型定义低rAT。结果：我们纳入48例PWE患者，其中36例（75%）合并OSA (PWE+OSA)， 108例仅合并OSA。PWE+OSA组在PSG检查时年龄较大，癫痫发作时间较PWE组晚。与仅有OSA的患者相比，PWE患者有更多的抗癫痫药物和催眠药物。在OSA患者中，PWE+OSA 19例（52.8%），OSA仅68例（63.0%）预测rAT较低。OSA组低鼠亚组持续气道正压依从性明显低于高鼠亚组（p = 0.021），而PWE+OSA组大鼠亚组间无显著差异。结论：我们的研究揭示了PWE+OSA中存在低鼠，其比例与OSA对照组相比无显著差异。然而，由于rAT是使用预测模型而不是直接测量来估计的，因此这一局限性可能会影响我们研究结果的解释。需要使用金标准方法进行进一步的研究，以阐明导致PWE患者OSA患病率较高的潜在机制。

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来源期刊

Nature and Science of Sleep Neuroscience-Behavioral Neuroscience

CiteScore

5.70

自引率

5.90%

发文量

245

审稿时长

16 weeks

期刊介绍： Nature and Science of Sleep is an international, peer-reviewed, open access journal covering all aspects of sleep science and sleep medicine, including the neurophysiology and functions of sleep, the genetics of sleep, sleep and society, biological rhythms, dreaming, sleep disorders and therapy, and strategies to optimize healthy sleep. Specific topics covered in the journal include: The functions of sleep in humans and other animals Physiological and neurophysiological changes with sleep The genetics of sleep and sleep differences The neurotransmitters, receptors and pathways involved in controlling both sleep and wakefulness Behavioral and pharmacological interventions aimed at improving sleep, and improving wakefulness Sleep changes with development and with age Sleep and reproduction (e.g., changes across the menstrual cycle, with pregnancy and menopause) The science and nature of dreams Sleep disorders Impact of sleep and sleep disorders on health, daytime function and quality of life Sleep problems secondary to clinical disorders Interaction of society with sleep (e.g., consequences of shift work, occupational health, public health) The microbiome and sleep Chronotherapy Impact of circadian rhythms on sleep, physiology, cognition and health Mechanisms controlling circadian rhythms, centrally and peripherally Impact of circadian rhythm disruptions (including night shift work, jet lag and social jet lag) on sleep, physiology, cognition and health Behavioral and pharmacological interventions aimed at reducing adverse effects of circadian-related sleep disruption Assessment of technologies and biomarkers for measuring sleep and/or circadian rhythms Epigenetic markers of sleep or circadian disruption.