丹麦 1 型嗜睡症、2 型嗜睡症和特发性嗜睡症患者的精神疾病合并症：病例对照研究。

Sleep advances : a journal of the Sleep Research Society Pub Date : 2024-10-05 eCollection Date: 2024-01-01 DOI:10.1093/sleepadvances/zpae073

Niels Christian Haubjerg Østerby, Lone Baandrup, Poul Jørgen Jennum

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引用次数: 0

摘要

研究目的研究丹麦1型嗜睡症（NT1）、2型嗜睡症（NT2）和特发性嗜睡症（IH）患者的精神病合并症差异：方法：对505名转诊到睡眠诊所进行嗜睡症诊断评估的患者进行了多导睡眠图（PSG）、多重睡眠潜伏期测试（MSLT）和腰椎穿刺。对诊断、临床特征、电生理学数据和脑脊液降视素-1（Csf-Hcrt-1）结果进行了检索。随后，在丹麦全国健康登记册中对患者进行识别，以收集睡眠障碍确诊前 10 年的精神病诊断和精神药物使用信息。研究人员将每组嗜睡症患者的精神病合并症患病率与年龄、性别和教育程度相匹配的1:4普通人群对照组进行了比较：结果：与匹配的对照组相比，NT2 和 IH 诊断与精神疾病的总合并症显著相关，但与 NT1 无关（NT1：OR = 1.5；NT2：OR = 6.1；IH：OR = 5.2）。NT1与任何精神障碍均无明显相关性。NT2与精神分裂症谱系障碍（OR = 8.5）、情绪障碍（OR = 6.7）、神经症（OR = 3.8）、人格障碍（OR = 3.1）以及行为和情感障碍（OR = 4.3）明显相关。IH与精神分裂症谱系障碍（OR = 3.3）、情绪障碍（OR = 5.9）、神经症（OR = 3.0）以及行为和情感障碍（OR = 4.0）明显相关：结论：NT2 和 IH 在确诊睡眠障碍前与精神疾病关系密切，而 NT1 则不然。这与之前的研究发现嗜睡症患者患精神疾病的比例较高的结果相吻合；不过，这也凸显了NT2和IH之间的相似性。我们相信，这种与精神疾病的联系可能在病理生理学中发挥作用。未来评估中枢源性嗜睡症与精神疾病之间关系的研究应包括嗜睡亚分类，以进一步了解这些疾病的差异。

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Psychiatric comorbidity in Danish patients with narcolepsy type 1, narcolepsy type 2, and idiopathic hypersomnia: a case-control study.

Study objectives: To examine the difference in psychiatric comorbidity of Danish patients with Narcolepsy type 1 (NT1), Narcolepsy type 2 (NT2), and idiopathic hypersomnia (IH).

Methods: Polysomnography (PSG), Multiple Sleep Latency Test (MSLT), and lumbar puncture were performed on 505 patients referred to a sleep clinic for diagnostic evaluation of hypersomnia. Diagnosis, clinical characteristics, electrophysiologic data, and cerebrospinal fluid hypocretin-1 (Csf-Hcrt-1) results were retrieved. Subsequently, the patients were identified in the Danish national health registers to collect information on psychiatric diagnoses and psychotropic medication use 10 years before the sleep disorder diagnosis. The prevalence of psychiatric comorbidities per hypersomnia group was compared to a 1:4 general population control group matched on age, gender, and educational level.

Results: A diagnosis of NT2 and IH was significantly associated with total psychiatric comorbidity compared to the matched controls but not NT1 (NT1: OR = 1.5; NT2: OR = 6.1; IH: OR = 5.2). NT1 was not significantly associated with any psychiatric disorder. NT2 was significantly associated with schizophrenia spectrum disorders (OR = 8.5), mood disorders (OR = 6.7), neurotic disorders (OR = 3.8), personality disorders (OR = 3.1), and behavioral and emotional disorders (OR = 4.3). IH was significantly associated with schizophrenia spectrum disorders (OR = 3.3), mood disorders (OR = 5.9), neurotic disorders (OR = 3.0), and behavioral and emotional disorders (OR = 4.0).

Conclusions: NT2 and IH had a close relationship to psychiatric disorders before diagnosis of their sleep disorder, while NT1 did not. This supports previous studies finding higher rates of psychiatric illness in patients with hypersomnia; however, it highlights the similarity between NT2 and IH. We believe this link to psychiatric disorders could play a role in the pathophysiology. Future studies evaluating the relation between hypersomnias of central origin and psychiatric diseases should include hypersomnia subclassifications to further the understanding of the differences in these disorders.

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Sleep advances : a journal of the Sleep Research Society

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2.10

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