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中枢性过度嗜睡障碍:聚焦发作性睡病和特发性嗜睡症。

Central Disorders of Hypersomnolence: Focus on the Narcolepsies and Idiopathic Hypersomnia.

作者信息

Khan Zeeshan, Trotti Lynn Marie

机构信息

Emory Sleep Center, Emory University School of Medicine, Atlanta, GA.

Emory Sleep Center, Emory University School of Medicine, Atlanta, GA.

出版信息

Chest. 2015 Jul;148(1):262-273. doi: 10.1378/chest.14-1304.

Abstract

The central disorders of hypersomnolence are characterized by severe daytime sleepiness, which is present despite normal quality and timing of nocturnal sleep. Recent reclassification distinguishes three main subtypes: narcolepsy type 1, narcolepsy type 2, and idiopathic hypersomnia (IH), which are the focus of this review. Narcolepsy type 1 results from loss of hypothalamic hypocretin neurons, while the pathophysiology underlying narcolepsy type 2 and IH remains to be fully elucidated. Treatment of all three disorders focuses on the management of sleepiness, with additional treatment of cataplexy in those patients with narcolepsy type 1. Sleepiness can be treated with modafinil/armodafinil or sympathomimetic CNS stimulants, which have been shown to be beneficial in randomized controlled trials of narcolepsy and, quite recently, IH. In those patients with narcolepsy type 1, sodium oxybate is effective for the treatment of both sleepiness and cataplexy. Despite these treatments, there remains a subset of hypersomnolent patients with persistent sleepiness, in whom alternate therapies are needed. Emerging treatments for sleepiness include histamine H3 antagonists (eg, pitolisant) and possibly negative allosteric modulators of the gamma-aminobutyric acid-A receptor (eg, clarithromycin and flumazenil).

摘要

中枢性过度嗜睡症的特点是白天严重嗜睡,尽管夜间睡眠质量和时间正常,但仍会出现。最近的重新分类区分出三种主要亚型:1型发作性睡病、2型发作性睡病和特发性嗜睡症(IH),它们是本综述的重点。1型发作性睡病是由下丘脑分泌素神经元缺失引起的,而2型发作性睡病和特发性嗜睡症的病理生理学仍有待充分阐明。这三种疾病的治疗都侧重于嗜睡的管理,对于1型发作性睡病患者还需额外治疗猝倒症。嗜睡可以用莫达非尼/阿莫达非尼或拟交感神经中枢兴奋剂治疗,这些药物在发作性睡病以及最近在特发性嗜睡症的随机对照试验中已显示出益处。对于1型发作性睡病患者,羟丁酸钠对治疗嗜睡和猝倒症均有效。尽管有这些治疗方法,但仍有一部分过度嗜睡患者持续存在嗜睡症状,对此需要采用其他替代疗法。新兴的嗜睡治疗方法包括组胺H3拮抗剂(如匹托利生)以及可能的γ-氨基丁酸-A受体负变构调节剂(如克拉霉素和氟马西尼)。

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