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食欲素受体拮抗剂诱导的睡眠不会损害犬类对情绪显著的声学刺激做出唤醒反应的能力。

Orexin receptor antagonist-induced sleep does not impair the ability to wake in response to emotionally salient acoustic stimuli in dogs.

作者信息

Tannenbaum Pamela L, Stevens Joanne, Binns Jacquelyn, Savitz Alan T, Garson Susan L, Fox Steven V, Coleman Paul, Kuduk Scott D, Gotter Anthony L, Marino Michael, Tye Spencer J, Uslaner Jason M, Winrow Christopher J, Renger John J

机构信息

Department of In Vivo Pharmacology, Merck Research Laboratories West Point, PA, USA.

Department of Neuroscience, Merck Research Laboratories West Point, PA, USA.

出版信息

Front Behav Neurosci. 2014 May 16;8:182. doi: 10.3389/fnbeh.2014.00182. eCollection 2014.

Abstract

The ability to awaken from sleep in response to important stimuli is a critical feature of normal sleep, as is maintaining sleep continuity in the presence of irrelevant background noise. Dual orexin receptor antagonists (DORAs) effectively promote sleep across species by targeting the evolutionarily conserved wake-promoting orexin signaling pathway. This study in dogs investigated whether DORA-induced sleep preserved the ability to awaken appropriately to salient acoustic stimuli but remain asleep when exposed to irrelevant stimuli. Sleep and wake in response to DORAs, vehicle, GABA-A receptor modulators (diazepam, eszopiclone and zolpidem) and antihistamine (diphenhydramine) administration were evaluated in telemetry-implanted adult dogs with continuous electrocorticogram, electromyogram (EMG), electrooculogram (EOG), and activity recordings. DORAs induced sleep, but GABA-A modulators and antihistamine induced paradoxical hyperarousal. Thus, salience gating studies were conducted during DORA-22 (0.3, 1, and 5 mg/kg; day and night) and vehicle nighttime sleep. The acoustic stimuli were either classically conditioned using food reward and positive attention (salient stimulus) or presented randomly (neutral stimulus). Once conditioned, the tones were presented at sleep times corresponding to maximal DORA-22 exposure. In response to the salient stimuli, dogs woke completely from vehicle and orexin-antagonized sleep across all sleep stages but rarely awoke to neutral stimuli. Notably, acute pharmacological antagonism of orexin receptors paired with emotionally salient anticipation produced wake, not cataplexy, in a species where genetic (chronic) loss of orexin receptor signaling leads to narcolepsy/cataplexy. DORA-induced sleep in the dog thereby retains the desired capacity to awaken to emotionally salient acoustic stimuli while preserving uninterrupted sleep in response to irrelevant stimuli.

摘要

对重要刺激做出反应从而从睡眠中醒来的能力是正常睡眠的一个关键特征,在存在无关背景噪音的情况下保持睡眠连续性也是如此。双重食欲素受体拮抗剂(DORAs)通过靶向进化上保守的促觉醒食欲素信号通路,有效地促进了跨物种的睡眠。这项在狗身上进行的研究调查了DORA诱导的睡眠是否保留了对显著声学刺激做出适当唤醒的能力,而在暴露于无关刺激时仍保持睡眠状态。在植入遥测设备的成年犬中,通过连续记录脑电图、肌电图(EMG)、眼电图(EOG)和活动情况,评估了给予DORAs、赋形剂、GABA-A受体调节剂(地西泮、艾司佐匹克隆和唑吡坦)以及抗组胺药(苯海拉明)后的睡眠和觉醒情况。DORAs诱导睡眠,但GABA-A调节剂和抗组胺药诱导反常的高度觉醒。因此,在DORA-22(0.3、1和5mg/kg;白天和晚上)和赋形剂夜间睡眠期间进行了显著性门控研究。声学刺激要么使用食物奖励和积极关注进行经典条件反射(显著刺激),要么随机呈现(中性刺激)。一旦形成条件反射,就在与最大DORA-22暴露相对应的睡眠时间呈现音调。对显著刺激的反应是,狗在所有睡眠阶段都能从赋形剂和食欲素拮抗诱导的睡眠中完全醒来,但很少对中性刺激做出反应而醒来。值得注意的是,在一个遗传(慢性)性食欲素受体信号缺失会导致发作性睡病/猝倒症的物种中,食欲素受体的急性药理学拮抗作用与情绪上显著的预期相结合会产生觉醒,而不是猝倒。因此,DORA诱导的狗睡眠保留了对情绪上显著的声学刺激做出唤醒反应的所需能力,同时在面对无关刺激时保持不间断的睡眠。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d63a/4032881/c3d93b8fa8b4/fnbeh-08-00182-g0001.jpg

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