| Literature DB >> 31324898 |
Claudio L A Bassetti1, Antoine Adamantidis2, Denis Burdakov3,4,5, Fang Han6, Steffen Gay7, Ulf Kallweit2,8, Ramin Khatami2,9, Frits Koning10, Brigitte R Kornum11, Gert Jan Lammers12,13, Roland S Liblau14, Pierre H Luppi15,16, Geert Mayer17, Thomas Pollmächer18, Takeshi Sakurai19, Federica Sallusto20,21, Thomas E Scammell22, Mehdi Tafti23,24, Yves Dauvilliers25,26,27.
Abstract
Narcolepsy is a rare brain disorder that reflects a selective loss or dysfunction of orexin (also known as hypocretin) neurons of the lateral hypothalamus. Narcolepsy type 1 (NT1) is characterized by excessive daytime sleepiness and cataplexy, accompanied by sleep-wake symptoms, such as hallucinations, sleep paralysis and disturbed sleep. Diagnosis is based on these clinical features and supported by biomarkers: evidence of rapid eye movement sleep periods soon after sleep onset; cerebrospinal fluid orexin deficiency; and positivity for HLA-DQB1*06:02. Symptomatic treatment with stimulant and anticataplectic drugs is usually efficacious. This Review focuses on our current understanding of how genetic, environmental and immune-related factors contribute to a prominent (but not isolated) orexin signalling deficiency in patients with NT1. Data supporting the view of NT1 as a hypothalamic disorder affecting not only sleep-wake but also motor, psychiatric, emotional, cognitive, metabolic and autonomic functions are presented, along with uncertainties concerning the 'narcoleptic borderland', including narcolepsy type 2 (NT2). The limitations of current diagnostic criteria for narcolepsy are discussed, and a possible new classification system incorporating the borderland conditions is presented. Finally, advances and obstacles in the symptomatic and causal treatment of narcolepsy are reviewed.Entities:
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Year: 2019 PMID: 31324898 DOI: 10.1038/s41582-019-0226-9
Source DB: PubMed Journal: Nat Rev Neurol ISSN: 1759-4758 Impact factor: 42.937