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首页> 外文期刊>Cell and Tissue Research >Two ancient neuropeptides, PACAP and AVP, modulate motivated behavior at synapses in the extrahypothalamic brain: a study in contrast
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Two ancient neuropeptides, PACAP and AVP, modulate motivated behavior at synapses in the extrahypothalamic brain: a study in contrast

机译:两种古代神经肽,PACAP和AVP,调节突出致命脑中突触的动机行为:相比之下的研究

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We examine evolutionary aspects of two primordial neuropeptides, arginine vasopressin (AVP) and pituitary adenylate cyclase-activating polypeptide (PACAP); the distribution of AVP and PACAP and their receptors in mammals; AVP and PACAP release patterns relevant to their roles in neuroendocrine control in brain and periphery; and finally the intricate interlocking of homeostatic and allostatic regulation created by extrahypothalamic AVP and PACAP projections to brain circuit nodes important in controlling appetitive, avoidance and aggressive motor responses. A cardinal feature of peptide neurotransmission important in regulatory control of organismic responses and emphasized in this review, is that neuropeptides are released from large dense-core vesicles docked not only within axonal varicosities and dendrites but also at presynaptic nerve terminal sites, along with small clear synaptic vesicles, at active zones. Peptide transmitter nerve terminals, from hypothalamic and other projections, are distributed widely to multiple brain areas important in integrative control of behavior. They converge with heterologous inputs that release other transmitters, including other peptides, in the same areas. The concept of a quasi-hormonal effect of peptide neurotransmission through coordinated release at multiple synapses throughout the brain echoes earlier conceptualizations of action-at-a-distance by diffusion following peptide release at non-synaptic sites. Yet, it recognizes that peptide delivery occurs with neuroanatomical precision, from discrete peptide-containing brain nuclei, via highly distributed projections to multiple extrahypothalamic nodes, registering multiple homeostatic, hedonistic, aversive and reproductive drives that modulate real-time motor decisions. There is paradigmatic value in the discussion of these two particular ancient neuropeptides, for peptide-centric translational neuroendocrinology and peptide GPCR-based neurotherapeutics.
机译:我们研究了两种原始神经肽,精氨酸加压素(AVP)和垂体腺苷酸环酶活化多肽(PACAP)的进化方面; AVP和PACAP及其在哺乳动物中的受体的分布; AVP和PACAP释放模式与脑和周边的神经内分泌控制中的作用相关;最后,通过额外的AVP和PACAP突起产生的稳态和近似调节的复杂互锁,在控制满意,避免和侵蚀电动机响应的脑电路节点中重要。在本综述中对生物反应的监管控制中肽神经递血的主要特征是,在本综述中,神经肽从大型密集核囊泡中释放而不仅在腋窝神经末端位点,以及小清晰突触囊泡,处于有源区。从下丘脑和其他突起的肽变送器神经终端被广泛分布到在对行为的综合控制中重要的多个脑区域。它们与异源输入汇聚,该输入释放在同一区域中的其他发射器,包括其他肽。在整个大脑中通过多个突起的协调释放的肽神经递血对肽释放的概念回应了在非突触位点肽释放后的扩散的概念概念化。然而,它识别出通过高度分布的脑核,通过高度分布式突出的突起,从多个含卵母细胞节点的高度分布式突起,注册了调节了实时电机决策的多个稳态,HEDONIC,厌恶和生殖驱动器的肽递送。对这两种特定的古代神经肽的讨论存在范例价值,用于以肽为中心的平移神经内部病理学和肽GPCR基神经治疗剂。

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