非典型N3睡眠:路易体病精神状态改变的生物标志物?

D Levendowski, T Neylan, J Lee-Iannotti, D Tsuang, C Walsh, C Berka, G Mazeika, B Boeve, E St. Louis
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摘要

非典型N3睡眠(AN3= δ波伴有限θ波和σ波)与ICU谵妄和脓毒症有关,平均占日本ICU患者睡眠时间的25%。我们感兴趣的是探索AN3是否可能是一系列神经退行性疾病(包括那些被诊断为痴呆的患者)的门诊患者脑功能障碍的标志。方法经伦理审查和知情同意后,选择路易体病(DLB/PDD: n=20,男性=90%,年龄=70 + 6.2)、阿尔茨海默病痴呆(AD: n=29,男性=79%,年龄=75 + 6.7)、帕金森病(PD: n=16,男性=69%,年龄=67 + 8.7)、轻度认知障碍(MCI: n=41,男性=63%,年龄=70 + 8.5)、单发REM睡眠行为障碍(iRBD: n=19,男性=74%,年龄=64 + 9.6)和对照组(CG: n=61,男性=47%,年龄=65 + 8.3)患者进行研究,并计算自动检测AN3。组间比较采用Mann-Whitney U检验和卡方检验。结果DLB/PDD患者AN3睡眠时间的平均百分比(8 + 12.3)明显高于PD(4 + 10.8)、AD(2 + 3.7)、MCI(2 + 2.3)、iRBD(1 + 1.6)和CG(1 + 2.4)(均为p<0.02)。与MCI=10%、iRBD=5%和CG=5%相比,DLB/PDD=35%的患者AN3异常(占睡眠时间的5%)的记录比例显著高于MCI=10%、iRBD=5%和CG=5%(均为p<0.05),但AD=17%和PD=13%的记录比例不高。结论AN3异常是否可能是区分路易体谱系疾病患者和其他病理的生物标志物,以及/或可能有助于监测中枢神经系统作用药物的副作用,还需要进一步的研究
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P025 Atypical N3 Sleep: A Biomarker for Altered Mental Status in Lewy Body Disease?
Abstract Introduction Atypical N3 sleep (AN3=delta waves with limited theta and sigma) has been associated with ICU delirium and sepsis and averaged 25% of sleep time in Japanese ICU patients. We were interested in exploring whether AN3 might be a marker of cerebral dysfunction in ambulatory patients across a range of neurodegenerative disorders, including those with a dementia diagnosis. Methods After ethics review and with informed consent, patients with Lewy body disease (DLB/PDD: n=20,male=90%,age=70 + 6.2), Alzheimers disease dementia (AD: n=29,male=79%,age=75 + 6.7), Parkinson disease (PD: n=16,male=69%,age=67 + 8.7), mild cognitive impairment (MCI: n=41,male=63%,age=70 + 8.5), isolated REM sleep behavior disorder (iRBD: n=19,male=74%,age=64 + 9.6) and a control group (CG: n=61,male=47%,age=65 + 8.3) were studied with the Sleep Profiler and auto-detected AN3 computed. Between-group comparisons were assessed with Mann-Whitney U and Chi-square tests. Results The mean percentages of sleep time with AN3 were significantly greater in DLB/PDD (8 + 12.3) vs. PD (4 + 10.8), AD (2 + 3.7), MCI (2 + 2.3), iRBD (1 + 1.6), and CG (1 + 2.4)(all p&lt;0.02). The proportions of records with abnormal AN3 (&gt;5% of sleep time) were significantly greater in those with DLB/PDD=35% vs. MCI=10%, iRBD=5% and CG=5% (all p&lt;0.05), but not AD=17% and PD=13%. Conclusions Further investigations are needed to determine if abnormal AN3 may be a biomarker that distinguishes patients with Lewy body spectrum diseases from alternative pathologies and/or could be helpful in monitoring the side effects of CNS-acting medications
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