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大鼠黑质和腹侧被盖区中神经激肽-1受体的亚细胞分布及可塑性

Subcellular distribution and plasticity of neurokinin-1 receptors in the rat substantia nigra and ventral tegmental area.

作者信息

Lessard A, Pickel V M

机构信息

Department of Neurology and Neuroscience, Weill Medical College of Cornell University, 411 East 69th Street, KB 410, New York, NY 10021, USA.

出版信息

Neuroscience. 2005;135(4):1309-23. doi: 10.1016/j.neuroscience.2005.07.025. Epub 2005 Sep 13.

Abstract

Neurokinin-1 receptors show activity-dependent changes in their surface distributions that are critical in spinal pain mechanisms, and also may play an important role in the motor and affective behaviors influenced by dopaminergic projections from the substantia nigra and ventral tegmental area. To determine the relevant sites for neurokinin-1 receptor activation in these midbrain regions, we examined the electron microscopic immunolabeling of neurokinin-1 receptors and the dopamine-synthesizing enzyme, tyrosine hydroxylase in normal rats. We also examined whether neurokinin-1 receptor distributions in one or both regions are affected by (1) startle-evoking intense auditory stimulation or (2) acute administration of apomorphine, a dopamine D1/D2 agonist that enhances startle while paradoxically reducing the prepulse inhibition produced by low intensity conditioning stimuli in rat models of schizophrenia. In each region, neurokinin-1 immunogold was located on the plasma membrane and endomembranes of somatodendritic profiles with or without tyrosine hydroxylase. As compared with controls, animals receiving intense auditory stimulation either alone or together with smaller low intensity prepulses showed a significant increase in neurokinin-1-plasmalemmal labeling in non-dopaminergic dendrites of both regions, and a reduction in this labeling in dopaminergic dendrites of the ventral tegmental area. Both effects were diminished following apomorphine administration. In absence of the intense auditory stimulation, however, apomorphine increased neurokinin-1-immunogold particles on the plasma membrane of the non-dopaminergic dendrites exclusively in the substantia nigra. Our results are the first to show that neurokinin-1 receptors have plasmalemmal distributions in dopaminergic and non-dopaminergic neurons that can be differentially modified by startle-evoking auditory stimulation. They suggest that while apomorphine can independently affect neurokinin-1 receptor trafficking in substantia nigra motor circuits, its effects on neurokinin-1 receptor distributions in the ventral tegmental area are exclusively dependent on sensory activation.

摘要

神经激肽-1受体在其表面分布上呈现出活性依赖性变化,这在脊髓疼痛机制中至关重要,并且可能在受黑质和腹侧被盖区多巴胺能投射影响的运动和情感行为中也发挥重要作用。为了确定这些中脑区域中神经激肽-1受体激活的相关位点,我们检测了正常大鼠中神经激肽-1受体和多巴胺合成酶酪氨酸羟化酶的电子显微镜免疫标记。我们还研究了一个或两个区域中的神经激肽-1受体分布是否受到以下因素影响:(1)引发惊吓的强烈听觉刺激,或(2)急性给予阿扑吗啡,一种多巴胺D1/D2激动剂,在精神分裂症大鼠模型中,它增强惊吓反应,同时反常地降低低强度条件刺激产生的前脉冲抑制。在每个区域中,神经激肽-1免疫金位于有或没有酪氨酸羟化酶的树突状轮廓的质膜和内膜上。与对照组相比,单独接受强烈听觉刺激或同时接受较小强度低强度预脉冲刺激的动物,两个区域的非多巴胺能树突中神经激肽-1质膜标记显著增加,而腹侧被盖区多巴胺能树突中的这种标记减少。给予阿扑吗啡后,这两种效应均减弱。然而,在没有强烈听觉刺激的情况下,阿扑吗啡仅增加黑质中非多巴胺能树突质膜上的神经激肽-1免疫金颗粒。我们的结果首次表明,神经激肽-1受体在多巴胺能和非多巴胺能神经元中具有质膜分布,可被引发惊吓的听觉刺激差异性修饰。结果表明,虽然阿扑吗啡可独立影响黑质运动回路中神经激肽-1受体的转运,但其对腹侧被盖区神经激肽-1受体分布的影响完全依赖于感觉激活。

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