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首页> 外文期刊>Behavioural Brain Research: An International Journal >Selective orexin 2 receptor antagonism blocks cue-induced reinstatement, but not nicotine self-administration or nicotine-induced reinstatement
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Selective orexin 2 receptor antagonism blocks cue-induced reinstatement, but not nicotine self-administration or nicotine-induced reinstatement

机译:选择性orexin 2受体拮抗作用可阻止提示诱导的恢复,但不能阻断尼古丁的自我给药或尼古丁的诱导的恢复

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摘要

The orexinergic system has been implicated in a number of behaviors, including reward and incentive motivation. Orexin 1 receptor antagonism has been reported to reduce drug self-administration, conditioned place preference, and reinstatement in rodents, but the role of the orexin 2 receptor is unclear. Here we evaluated the impact of the novel and selective orexin 2 receptor antagonist, 2-SORA18, on motivation for nicotine as measured by responding on a progressive ratio schedule, as well as cue-induced reinstatement of a response previously associated with nicotine reward, and nicotine-induced reinstatement. 2-SORA 18 demonstrated selective effects on these behaviors. Specifically, doses up to 60 mg/kg 2-SORA 18 were without significant effect on nicotine self-administration or nicotine-induced reinstatement, but doses as low as 15 mg/kg 2-SORA 18 completely blocked cue-induced reinstatement. These findings indicate that orexin 2 receptor antagonism might have utility for attenuating relapse, particularly for patients sensitive to environmental stimuli associated with drug taking.
机译:食欲能系统涉及许多行为,包括奖励和激励动机。据报道,Orexin 2受体拮抗作用可减少啮齿类动物的药物自我给药,条件位置偏爱和恢复,但尚不清楚Orexin 2受体的作用。在这里,我们评估了新型和选择性的orexin 2受体拮抗剂2-SORA18对尼古丁动机的影响,方法是按渐进的比例表进行响应,并通过提示诱导恢复先前与尼古丁奖励有关的响应,并尼古丁引起的恢复。 2-SORA 18对这些行为表现出选择性作用。具体而言,剂量高达60 mg / kg的2-SORA 18对尼古丁的自我给药或烟碱诱导的恢复没有显着影响,但是低至15 mg / kg的2-SORA 18的剂量完全阻止了提示诱导的恢复。这些发现表明,orexin 2受体拮抗作用可能具有减轻复发的作用,特别是对于对与吸毒有关的环境刺激敏感的患者。

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