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Role of NPY Y1 receptor on acquisition, consolidation and extinction on contextual fear conditioning: Dissociation between anxiety, locomotion and non-emotional memory behavior

机译:NPY Y1受体在情境恐惧条件的获得,巩固和消退中的作用:焦虑,运动和非情绪记忆行为之间的联系

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Neuropeptide Y (NPY) is the most abundant peptide in the central nervous system (CNS) and is densely localized in the brain regions involved in stress, memory, fear and anxiety. Although previous research supports a role for NPY in the mediation of rodent and human emotional behavior, there is currently a lack of information on the effects of low doses of NPY that could have a potential therapeutic advantage, minimizing side-effects such as cognition impairment or sedation. Herein, we assessed the effects of intracerebroventricular (i.c.v.) administration of low doses of NPY, and of the Y1-agonist Leu31Pro34-NPY (LP-NPY) on contextual fear conditioning (CFC), as they have no effect on unconditioned anxiety-like, locomotor activity and non-emotional memory. NPY (3. pmol) and LP-NPY (1. pmol) inhibited freezing behavior when administered in the acquisition or consolidation stages, indicating a reduction of fear. When injected in the extinction phase, only NPY inhibited freezing behavior on CFC. Pre-treatment with the Y1-antagonist BIBO3304 before NPY and LP-NPY was able to prevent the inhibition of fear responses induced by both NPY agonists. Taken together, our results demonstrate robust fear-inhibiting effects of i.c.v. injection of NPY on contextual fear conditioning in rats, a response that is mediated, at least in part, by the Y1 receptor. Moreover, these treatments were unable to change locomotor activity or to show an anxiolytic-like effect, as evaluated in an open-field and an elevated plus-maze. This specific fear reduction effect may underlie resilience systems in the CNS and has potential therapeutic relevance in PTSD.
机译:神经肽Y(NPY)是中枢神经系统(CNS)中最丰富的肽,密集分布在涉及压力,记忆,恐惧和焦虑的大脑区域。尽管先前的研究支持NPY在啮齿动物和人类情绪行为的介导中的作用,但目前尚缺乏有关低剂量NPY的影响的信息,该信息可能具有潜在的治疗优势,从而最大程度地减少了认知障碍或副作用等副作用。镇静剂。本文中,我们评估了低剂量NPY和Y1激动剂Leu31Pro34-NPY(LP-NPY)的脑室内(icv)给药对情境恐惧调节(CFC)的影响,因为它们对无条件的焦虑样症状没有影响,运动活动和非情绪记忆。当在采集或巩固阶段给药时,NPY(3. pmol)和LP-NPY(1. pmol)抑制了冰冻行为,表明恐惧减少了。在消光阶段注射时,只有NPY抑制CFC的冻结行为。在NPY和LP-NPY之前使用Y1拮抗剂BIBO3304进行的预处理能够预防两种NPY激动剂诱导的恐惧反应的抑制。综上所述,我们的结果证明了i.c.v.强大的抑制恐惧的作用。在大鼠的情境恐惧调节中注射NPY,这种反应至少部分由Y1受体介导。而且,如在旷场和高迷宫中所评估的,这些治疗不能改变运动活性或显示出抗焦虑作用。这种减少恐惧的特效可能是中枢神经系统弹性系统的基础,并且在创伤后应激障碍中具有潜在的治疗意义。

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