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发育中和成年大鼠脊髓中的神经肽受体:降钙素基因相关肽、神经激肽、μ-阿片样物质、甘丙肽、生长抑素、神经降压素和血管活性肠肽受体的体外定量放射自显影研究

Neuropeptide receptors in developing and adult rat spinal cord: an in vitro quantitative autoradiography study of calcitonin gene-related peptide, neurokinins, mu-opioid, galanin, somatostatin, neurotensin and vasoactive intestinal polypeptide receptors.

作者信息

Kar S, Quirion R

机构信息

Douglas Hospital Research Center, Department of Psychiatry, McGill University, Montreal, Canada.

出版信息

J Comp Neurol. 1995 Apr 3;354(2):253-81. doi: 10.1002/cne.903540208.

Abstract

A number of neuroactive peptides including calcitonin gene-related peptide (CGRP), substance P, neurokinin B, opioids, somatostatin (SRIF), galanin, neurotensin and vasoactive intestinal polypeptide (VIP) have been localized in adult rat spinal cord and are considered to participate either directly and/or indirectly in the processing of sensory, motor and autonomic functions. Most of these peptides appear early during development, leading to the suggestion that peptides, in addition to their neurotransmitter/neuromodulator roles, may possibly be involved in the normal growth and maturation of the spinal cord. To provide an anatomical substrate for a better understanding of the possible roles of peptides in the ontogenic development of the cord, we investigated the topographical profile as well as variation in densities of [125I]hCGRP alpha, [125I]substance P/neurokinin-1 (NK-1), [125I]eledoisin/neurokinin-3 (NK-3), [125I]FK 33-824 ([D-Ala2, Me-Phe4, Met(O)ol5]enkephalin)/mu-opioid, [125I]galanin, [125I]T0D8-SRIF14 (an analog of somatostatin); [125I]neurotensin and [125I]VIP binding sites in postnatal and adult rat spinal cord using in vitro quantitative receptor autoradiography. Receptor binding sites recognized by each radioligand are found to be distributed widely during early stages of postnatal development and then to undergo selective modification to attain their adult profile of distribution during the third week of postnatal development. The apparent density of various receptor sites, however, are differently regulated depending on the lamina and the stage of development studied. For example, the density of mu-opioid binding sites, following a peak at postnatal day 4 (P4), declines gradually in almost all regions of the spinal cord with the increasing age of the animal. [125I]substance P/NK-1 binding sites, on the other hand, show very little variation until P14 and then subsequently decrease as the development proceeds. In the adult rat, most of these peptide receptor binding sites are localized in relatively high amounts in the superficial laminae of the dorsal horn. To varying extents, moderate to low density of various peptide receptor binding sites are also found to be present in the ventral horn, intermediolateral cell column and around the central canal. Taken together, these results suggest that each receptor-ligand system is regulated differently during development and may each uniquely be involved in cellular growth, differentiation and in maturation of the normal neural circuits of the spinal cord. Furthermore, the selective localization of various receptor binding sites in adult rat spinal cord over a wide variety of functionally distinct regions reinforces the neurotransmitter/modulator roles of these peptides in sensory, motor and autonomic functions associated with the spinal cord.

摘要

包括降钙素基因相关肽(CGRP)、P物质、神经激肽B、阿片类物质、生长抑素(SRIF)、甘丙肽、神经降压素和血管活性肠肽(VIP)在内的多种神经活性肽已在成年大鼠脊髓中定位,并被认为直接和/或间接参与感觉、运动和自主功能的处理。这些肽中的大多数在发育早期出现,这表明肽除了其神经递质/神经调质作用外,可能还参与脊髓的正常生长和成熟。为了提供一个解剖学基础,以便更好地理解肽在脊髓个体发育中的可能作用,我们使用体外定量受体放射自显影技术,研究了出生后和成年大鼠脊髓中[125I]人α-CGRP、[125I]P物质/神经激肽-1(NK-1)、[125I]伊列毒素/神经激肽-3(NK-3)、[125I]FK 33-824([D-Ala2,Me-Phe4,Met(O)ol5]脑啡肽)/μ-阿片受体、[125I]甘丙肽、[125I]T0D8-SRIF14(生长抑素类似物)、[125I]神经降压素和[125I]VIP结合位点的拓扑分布以及密度变化。发现每个放射性配体识别的受体结合位点在出生后发育的早期阶段广泛分布,然后在出生后发育的第三周经历选择性修饰,以达到其成年分布模式。然而,各种受体位点的表观密度根据所研究的板层和发育阶段而受到不同的调节。例如,μ-阿片受体结合位点的密度在出生后第4天(P4)达到峰值后,随着动物年龄的增加,在脊髓的几乎所有区域逐渐下降。另一方面,[125I]P物质/NK-1结合位点在P14之前变化很小,然后随着发育的进行而逐渐减少。在成年大鼠中,这些肽受体结合位点中的大多数在背角的浅层层中含量相对较高。在不同程度上,还发现腹角、中间外侧细胞柱和中央管周围存在中度至低密度的各种肽受体结合位点。综上所述,这些结果表明,每个受体-配体系统在发育过程中受到不同的调节,并且可能各自独特地参与脊髓正常神经回路的细胞生长、分化和成熟。此外,各种受体结合位点在成年大鼠脊髓中广泛的功能不同区域的选择性定位,强化了这些肽在与脊髓相关的感觉、运动和自主功能中的神经递质/调质作用。

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