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垂体腺苷酸环化酶激活多肽(PACAP)的结合位点:与大鼠脑切片中血管活性肠多肽(VIP)结合位点定位的比较。

Binding sites for pituitary adenylate cyclase activating polypeptide (PACAP): comparison with vasoactive intestinal polypeptide (VIP) binding site localization in rat brain sections.

作者信息

Masuo Y, Ohtaki T, Masuda Y, Tsuda M, Fujino M

机构信息

Tsukuba Research Laboratories, Takeda Chemical Industries, Ltd., Ibaraki, Japan.

出版信息

Brain Res. 1992 Mar 13;575(1):113-23. doi: 10.1016/0006-8993(92)90430-h.

Abstract

Pituitary adenylate cyclase activating polypeptide (PACAP) is structurally similar to vasoactive intestinal polypeptide (VIP). We investigated the characteristics and topographical distribution of [125I]PACAP binding sites compared with those of [125I]VIP binding sites in the rat brain. Radiolabeled PACAP and VIP showed highly specific binding to sections at the level of the dorsal hippocampus. The specific binding of [125I]PACAP was 10 times higher than that of [125I]VIP in hippocampal sections. [125I]PACAP binding was scarcely displaced by unlabeled VIP, while [125I]VIP binding was effectively displaced by unlabeled PACAP. Therefore, PACAP binding sites may reflect both PACAP specific binding sites and VIP/PACAP binding sites. However, the amount of VIP/PACAP binding sites was negligibly low. Autoradiography revealed that [125I]PACAP binding sites were dense in the piriform cortex, diagonal band, accumbens nucleus, anterior part of the striatum, hippocampal formation, habenular nucleus, lateral hypothalamic area, superior colliculus and dorsal raphe nucleus. Moderate to high labeling was observed in the medial septal nucleus, olfactory tubercle, caudal part of the striatum, most parts of the thalamus, supraoptic and periventricular hypothalamic nuclei, central gray, substantia nigra pars compacta, locus coeruleus, pontine reticular nucleus and cerebellum. Distribution pattern was remarkably different from that of [125I]VIP binding sites in the hippocampal formation, lateral hypothalamic area, substantia nigra pars compacta, pontine reticular nucleus and cerebellum. The present results suggest that PACAP may have a physiological role in the regulation of the central nervous system.

摘要

垂体腺苷酸环化酶激活多肽(PACAP)在结构上与血管活性肠肽(VIP)相似。我们研究了大鼠脑中[125I]PACAP结合位点与[125I]VIP结合位点相比的特征和拓扑分布。放射性标记的PACAP和VIP对背侧海马水平的切片显示出高度特异性结合。在海马切片中,[125I]PACAP的特异性结合比[125I]VIP高10倍。未标记的VIP几乎不能取代[125I]PACAP的结合,而未标记的PACAP能有效取代[125I]VIP的结合。因此,PACAP结合位点可能既反映了PACAP特异性结合位点,也反映了VIP/PACAP结合位点。然而,VIP/PACAP结合位点的数量极低,可忽略不计。放射自显影显示,[125I]PACAP结合位点在梨状皮质、斜角带、伏隔核、纹状体前部、海马结构、缰核、下丘脑外侧区、上丘和中缝背核中密集。在内侧隔核、嗅结节、纹状体尾部、丘脑大部分区域、视上核和室旁下丘脑核、中央灰质、黑质致密部、蓝斑、脑桥网状核和小脑中观察到中度至高度标记。在海马结构、下丘脑外侧区、黑质致密部、脑桥网状核和小脑中,其分布模式与[125I]VIP结合位点明显不同。目前的结果表明,PACAP可能在中枢神经系统的调节中具有生理作用。

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