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首页> 外文期刊>The international journal of neuropsychopharmacology >Orexin-1 receptor signalling within the ventral tegmental area, but not the paraventricular thalamus, is critical to regulating cue-induced reinstatement of cocaine-seeking
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Orexin-1 receptor signalling within the ventral tegmental area, but not the paraventricular thalamus, is critical to regulating cue-induced reinstatement of cocaine-seeking

机译:腹侧被盖区中的Orexin-1受体信号传导,而不是脑室旁丘脑,对调节提示诱导的可卡因寻求恢复至关重要

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Orexinergic signalling is critical to drug relapse-like behaviour; however, the CNS sites(s) of action remain unknown. Two candidate brain regions are the paraventricular thalamus (PVT) and ventral tegmental area (VTA). We assessed the effect of intra-PVT or -VTA administration of the orexin-1 receptor (OrxR1) antagonist SB-334867 on discriminative cue-induced cocaine-seeking. Animals received either PVT- or VTA-directed SB-334867 (0, 3 or 6 μg; 0, 1 or 3 μg, respectively) prior to reinstatement testing elicited by presenting cocaine-paired stimuli (S+). The effect of VTA-directed injections of SB-334867 (0 or 3 μg) on locomotor activity was also assessed. Intra-VTA, but not -PVT, SB-334867 dose-dependently attenuated S+-induced reinstatement (3 μg dose, p0.01). Intra-VTA SB-334867 had no effect on locomotor activity. We conclude that OrxR1 signalling within the VTA, but not the PVT, mediates cue-induced cocaine-seeking behaviour. We hypothesize that blockade of VTA OrxR1 signalling may reduce nucleus accumbens dopamine in response to drug cue presentation.
机译:Orexinergic信号对于药物复发样行为至关重要。但是,CNS的作用部位仍然未知。两个候选的大脑区域是脑室旁丘脑(PVT)和腹侧被盖区(VTA)。我们评估了Orexin-1受体(OrxR1)拮抗剂SB-334867的PVT或-VTA给药对判别性提示诱导的可卡因寻求的影响。在接受可卡因配对刺激(S + )引发的恢复测试之前,动物接受了PVT或VTA定向的SB-334867(分别为0、3或6μg; 0、1或3μg)。 )。还评估了VTA定向注射SB-334867(0或3μg)对运动活性的影响。 VTA内,而不是-PVT,SB-334867剂量依赖性地减弱S + 诱导的恢复(3μg剂量,p <0.01)。 VTA内SB-334867对运动活性没有影响。我们得出结论,VTA内的OrxR1信号传导,而不是PVT,介导了提示诱导的可卡因寻求行为。我们假设对VTA OrxR1信号的阻断可能会减少伏伏核多巴胺对药物提示的反应。

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