食欲素受体拮抗作用改善Kcna1基因敲除小鼠的睡眠并减少癫痫发作
Orexin Receptor Antagonism Improves Sleep and Reduces Seizures in Kcna1-null Mice.
作者信息
Roundtree Harrison M, Simeone Timothy A, Johnson Chaz, Matthews Stephanie A, Samson Kaeli K, Simeone Kristina A
机构信息
Pharmacology Department, Creighton University School of Medicine, Omaha, NE.
出版信息
Sleep. 2016 Feb 1;39(2):357-68. doi: 10.5665/sleep.5444.
STUDY OBJECTIVE
Comorbid sleep disorders occur in approximately one-third of people with epilepsy. Seizures and sleep disorders have an interdependent relationship where the occurrence of one can exacerbate the other. Orexin, a wake-promoting neuropeptide, is associated with sleep disorder symptoms. Here, we tested the hypothesis that orexin dysregulation plays a role in the comorbid sleep disorder symptoms in the Kcna1-null mouse model of temporal lobe epilepsy.
METHODS
Rest-activity was assessed using infrared beam actigraphy. Sleep architecture and seizures were assessed using continuous video-electroencephalography-electromyography recordings in Kcna1-null mice treated with vehicle or the dual orexin receptor antagonist, almorexant (100 mg/kg, intraperitoneally). Orexin levels in the lateral hypothalamus/perifornical region (LH/P) and hypothalamic pathology were assessed with immunohistochemistry and oxygen polarography.
RESULTS
Kcna1-null mice have increased latency to rapid eye movement (REM) sleep onset, sleep fragmentation, and number of wake epochs. The numbers of REM and non-REM (NREM) sleep epochs are significantly reduced in Kcna1-null mice. Severe seizures propagate to the wake-promoting LH/P where injury is apparent (indicated by astrogliosis, blood-brain barrier permeability, and impaired mitochondrial function). The number of orexin-positive neurons is increased in the LH/P compared to wild-type LH/P. Treatment with a dual orexin receptor antagonist significantly increases the number and duration of NREM sleep epochs and reduces the latency to REM sleep onset. Further, almorexant treatment reduces the incidence of severe seizures and overall seizure burden. Interestingly, we report a significant positive correlation between latency to REM onset and seizure burden in Kcna1-null mice.
CONCLUSION
Dual orexin receptor antagonists may be an effective sleeping aid in epilepsy, and warrants further study on their somnogenic and ant-seizure effects in other epilepsy models.
研究目的
约三分之一的癫痫患者合并睡眠障碍。癫痫发作与睡眠障碍存在相互依存关系,其中一方的发生会加重另一方。食欲素是一种促进觉醒的神经肽,与睡眠障碍症状有关。在此,我们测试了以下假设:食欲素失调在颞叶癫痫的Kcna1基因敲除小鼠模型的合并睡眠障碍症状中起作用。
方法
使用红外光束活动记录仪评估静息-活动情况。在接受载体或双重食欲素受体拮抗剂阿莫瑞林(100mg/kg,腹腔注射)治疗的Kcna1基因敲除小鼠中,使用连续视频脑电图-肌电图记录来评估睡眠结构和癫痫发作情况。通过免疫组织化学和氧极谱法评估下丘脑外侧/穹窿周区域(LH/P)的食欲素水平和下丘脑病理学。
结果
Kcna1基因敲除小鼠快速眼动(REM)睡眠开始的潜伏期延长、睡眠碎片化以及觉醒期数量增加。Kcna1基因敲除小鼠的REM和非快速眼动(NREM)睡眠期数量显著减少。严重的癫痫发作扩散到促进觉醒的LH/P区域,该区域出现明显损伤(通过星形胶质细胞增生、血脑屏障通透性和线粒体功能受损来表明)。与野生型LH/P相比,LH/P中食欲素阳性神经元的数量增加。双重食欲素受体拮抗剂治疗显著增加NREM睡眠期的数量和持续时间,并缩短REM睡眠开始的潜伏期。此外,阿莫瑞林治疗降低了严重癫痫发作的发生率和总体癫痫发作负担。有趣的是,我们报告了Kcna1基因敲除小鼠中REM开始潜伏期与癫痫发作负担之间存在显著正相关。
结论
双重食欲素受体拮抗剂可能是癫痫患者有效的助眠药物,并且有必要进一步研究其在其他癫痫模型中的促眠和抗癫痫作用。
Zotero 插件