首页> 美国卫生研究院文献>The Journal of Neuroscience >The peptidergic organization of the cat periaqueductal gray. II. The distribution of immunoreactive substance P and vasoactive intestinal polypeptide
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The peptidergic organization of the cat periaqueductal gray. II. The distribution of immunoreactive substance P and vasoactive intestinal polypeptide

机译:猫导水管周围灰色的肽能组织。二。免疫反应性物质P和血管活性肠多肽的分布

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摘要

Despite the important contribution of the midbrain periaqueductal gray (PAG) to endogenous pain suppression systems, little is known about the neuroanatomical basis of its functional organization. In a previous study of the distribution of the endogenous opiate leucine-enkephalin (ENK) in the PAG (Moss, M. S., E. J. Glazer, and A. I. Basbaum (1983) J. Neurosci. 3: 603–616), we found that immunoreactive ENK-containing neurons and terminals are clustered in discrete populations. In this study we have extended our analysis of the neurochemical organization of the PAG by using immunocytochemistry to map the distribution of two non-opiate peptides that produce potent analgesia when administered at central gray levels: substance P (Sub P) and vasoactive intestinal polypeptide (VIP). Immunoreactive Sub P neurons and terminal fields are clustered in discrete populations throughout the PAG. The distribution pattern of these populations changes at different rostral-caudal levels of the PAG. For example, there is a ventral-to-dorsal shift in the location of Sub P-like immunoreactivity from the caudal to the rostral PAG. Few immunoreactive Sub P neurons are found in the nucleus raphe dorsalis although moderately dense terminal field staining is present. The staining pattern of immunoreactive VIP is totally different from that of Sub P. Regardless of the rostral-caudal level examined, VIP- containing neurons are found tightly clustered in the subependymal neuropil of the ventromedial PAG. Only a few immunoreactive VIP- containing neurons are found in the ventral PAG or nucleus raphe dorsalis. The striking differences between the distribution of Sub P- and VIP-like immunoreactivity in the PAG indicates that the neural circuitry underlying pain suppression by Sub P and VIP may also differ.
机译:尽管中脑导水管周围灰色(PAG)对内源性疼痛抑制系统有重要贡献,但对其功能组织的神经解剖学基础知之甚少。在以前的研究中,PAG中内源性鸦片亮氨酸-脑啡肽(ENK)的分布(Moss,MS,EJ Glazer和AI Basbaum(1983)J. Neurosci。3:603-616)中,我们发现免疫反应性ENK含神经元和末端聚集在离散种群中。在这项研究中,我们通过使用免疫细胞化学绘制了两种非鸦片肽在中央灰度水平下给药时可产生有效镇痛作用的分布图,从而扩展了PAG的神经化学组织分析:P物质(Sub P)和血管活性肠多肽( VIP)。免疫反应性Sub P神经元和终末场聚集在整个PAG中的离散种群中。这些种群的分布模式在PAG的不同尾尖水平上发生变化。例如,Sub P样免疫反应的位置从尾向PAG的腹侧到背侧转移。尽管存在中等密集的末端视野染色,但是在背核中几乎没有发现具有免疫反应性的Sub P神经元。免疫反应性VIP的染色模式与Sub P完全不同。无论所检查的鼻尾状尾巴水平如何,都发现含有VIP的神经元紧密地聚集在腹膜PAG的室管膜下神经纤维中。在腹侧PAG或背缝核中仅发现少数具有免疫反应性的含有VIP的神经元。 PAG中Sub P和VIP类免疫反应性分布之间的显着差异表明,Sub P和VIP抑制疼痛的神经回路也可能不同。

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