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The Discovery of Suvorexant, the First Orexin Receptor Drug for Insomnia
Annual Review of Pharmacology and Toxicology ( IF 12.5 ) Pub Date : 2017-01-06 00:00:00 , DOI: 10.1146/annurev-pharmtox-010716-104837
Paul J. Coleman 1 , Anthony L. Gotter 2 , W. Joseph Herring 3 , Christopher J. Winrow 2 , John J. Renger 2
Affiliation  

Historically, pharmacological therapies have used mechanisms such as γ-aminobutyric acid A (GABAA) receptor potentiation to drive sleep through broad suppression of central nervous system activity. With the discovery of orexin signaling loss as the etiology underlying narcolepsy, a disorder associated with hypersomnolence, orexin antagonism emerged as an alternative approach to attenuate orexin-induced wakefulness more selectively. Dual orexin receptor antagonists (DORAs) block the activity of orexin 1 and 2 receptors to both reduce the threshold to transition into sleep and attenuate orexin-mediated arousal. Among DORAs evaluated clinically, suvorexant has pharmacokinetic properties engineered for a plasma half-life appropriate for rapid sleep onset and maintenance at low to moderate doses. Unlike GABAA receptor modulators, DORAs promote both non-rapid eye movement (NREM) and REM sleep, do not disrupt sleep stage–specific quantitative electroencephalogram spectral profiles, and allow somnolence indistinct from normal sleep. The preservation of cognitive performance and the ability to arouse to salient stimuli after DORA administration suggest further advantages over historical therapies.

中文翻译:


Suvorexant,首个失眠的Orexin受体药物的发现

从历史上看,药物治疗使用诸如γ-氨基丁酸A(GABA A)受体增强的机制来通过广泛抑制中枢神经系统活动来驱动睡眠。随着食欲素信号丧失作为发作性睡病的病因基础的发现,与嗜睡症相关的疾病,食欲素拮抗作用应运而生,成为一种选择性地减弱食欲素诱导的觉醒的替代方法。双重orexin受体拮抗剂(DORA)阻断orexin 1和2受体的活性,以降低过渡到睡眠的阈值并减弱orexin介导的唤醒。在经过临床评估的DORA中,suvorexant具有针对血浆半衰期设计的药代动力学特性,适合于快速睡眠发作并维持中低剂量。与GABA不同DORA是一种受体调节剂,可促进非快速眼动(NREM)和REM睡眠,不破坏特定于睡眠阶段的定量脑电图频谱图,并且使人的嗜睡感与正常睡眠不明显。在DORA给药后,认知功能的保持和引起显着刺激的能力表明,与历史疗法相比,它具有更多的优势。

更新日期:2017-01-06
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