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与氟西汀治疗抑郁症和强迫症相关的非快速眼动睡眠期显著眼动及快速眼动睡眠行为障碍。

Prominent eye movements during NREM sleep and REM sleep behavior disorder associated with fluoxetine treatment of depression and obsessive-compulsive disorder.

作者信息

Schenck C H, Mahowald M W, Kim S W, O'Connor K A, Hurwitz T D

机构信息

Minnesota Regional Sleep Disorders Center, Minneapolis 55415.

出版信息

Sleep. 1992 Jun;15(3):226-35. doi: 10.1093/sleep/15.3.226.

Abstract

The clinical polysomnographic (PSG) reports of 2,650 consecutive adults studied during 41 months were reviewed retrospectively to identify all patients treated with fluoxetine or tricyclic antidepressants. The PSG reports of four other adult groups were also reviewed: periodic limb movement (PLM) disorder (n = 28); sleep terror/sleepwalking (ST/SW) (n = 54); rapid eye movement (REM) sleep behavior disorder (RBD) (n = 70); patients with clinically unremarkable sleep during two consecutive PSG studies (n = 30). Standard PSG recording and scoring methods were employed. A total of 1.5% (n = 41) and 2.0% (n = 52) of patients were receiving fluoxetine or tricyclics (amitriptyline or nortriptyline, n = 31; imipramine or desipramine, n = 16; protriptyline or trimipramine, n = 5). A selective association between fluoxetine and extensive, prominent eye movements in nonrapid eye movement (NREM) sleep was detected, utilizing Fisher's exact one-tailed statistic (p less than 0.00001 for each comparison). The detection rates were fluoxetine, 48.8% (20/41); tricyclics, 5.8% (3/52); RBD, 4.3% (3/70); objectively normal sleepers, 3.3% (1/30); PLM, ST/SW, 0% (0/82). These groups had similar mean ages (31.5-45.4 years) and gender distributions (50.0-60.7% male), apart from RBD. The effect of fluoxetine, a potent and specific serotonin reuptake inhibitor, on NREM eye movements is postulated to derive from potentiation of serotonergic neurons that inhibit brainstem "omnipause neurons", which, in turn, inhibit saccadic eye movements, thus resulting in disinhibited release of saccades. In addition, a 31-year-old man with obsessive-compulsive disorder developed RBD soon after starting fluoxetine therapy, which persisted at PSG study 19 months after fluoxetine discontinuation.

摘要

回顾性分析了41个月期间连续研究的2650名成年人的临床多导睡眠图(PSG)报告,以确定所有接受氟西汀或三环类抗抑郁药治疗的患者。还回顾了其他四个成年人群体的PSG报告:周期性肢体运动(PLM)障碍(n = 28);睡惊症/梦游症(ST/SW)(n = 54);快速眼动(REM)睡眠行为障碍(RBD)(n = 70);在连续两次PSG研究中睡眠临床无异常的患者(n = 30)。采用标准的PSG记录和评分方法。共有1.5%(n = 41)和2.0%(n = 52)的患者正在接受氟西汀或三环类药物治疗(阿米替林或去甲替林,n = 31;丙咪嗪或地昔帕明,n = 16;普罗替林或曲米帕明,n = 5)。利用Fisher精确单尾统计量检测到氟西汀与非快速眼动(NREM)睡眠中广泛、明显的眼球运动之间存在选择性关联(每次比较p<0.00001)。检测率分别为:氟西汀组48.8%(20/41);三环类药物组5.8%(3/52);RBD组4.3%(3/70);客观睡眠正常者3.3%(1/30);PLM、ST/SW组0%(0/82)。除RBD外,这些组的平均年龄(31.5 - 45.4岁)和性别分布(男性占50.0 - 60.7%)相似。推测强效特异性5-羟色胺再摄取抑制剂氟西汀对NREM眼球运动的影响源于增强了抑制脑干“暂停神经元”的5-羟色胺能神经元,而脑干“暂停神经元”反过来又抑制眼球跳动,从而导致眼球跳动释放不受抑制。此外,一名31岁患有强迫症的男性在开始氟西汀治疗后不久出现RBD,在停用氟西汀19个月后的PSG研究中仍持续存在。

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