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大鼠胼胝体内神经元型一氧化氮合酶神经元与神经激肽1P物质受体共定位。

Intracallosal neuronal nitric oxide synthase neurons colocalize with neurokinin 1 substance P receptor in the rat.

作者信息

Barbaresi Paolo, Mensà Emanuela, Lariccia Vincenzo, Desiato Genni, Fabri Mara, Gratteri Santo

机构信息

Department of Experimental and Clinical Medicine, Section of Neuroscience and Cell Biology, Marche Polytechnic University, I-60020, Ancona, Italy.

出版信息

J Comp Neurol. 2015 Mar 1;523(4):589-607. doi: 10.1002/cne.23695. Epub 2014 Nov 18.

Abstract

The corpus callosum (cc) contains nitric oxide (NO)-producing neurons. Because NO is a potent vasodilator, these neurons could translate neuronal signals into vascular responses that can be detected by functional brain imaging. Substance P (SP), one of the most widely expressed peptides in the CNS, also produces vasomotor responses by inducing calcium release from intracellular stores through its preferred neurokinin 1 (NK1) receptor, thus inducing NO production via activation of neuronal NO synthase (nNOS). Single- and double-labeling experiments were performed to establish whether NK1-immunopositive neurons (NK1IP -n) are found in the rat cc and the extent of NK1 colocalization with nNOS. NK1IP -n were seen to constitute a large neuronal population in the cc and had a distribution similar to that of nNOSIP neurons (nNOSIP -n). NK1IP -n were numerous in the lateral cc and gradually decreased in the more medial portions, where they were few or absent. Intracallosal NK1IP -n and their dendritic trees were intensely labeled, allowing classification into four morphological types: bipolar, round, polygonal, and pyramidal. Confocal microscopic examination demonstrated that nearly all NK1IP -n contained nNOS (96.43%) and that 84.59% of nNOSIP -n co-expressed NK1. These data suggest that the majority of intracallosal neurons can release NO as a result of the action of SP. A small proportion of nNOSIP -n does not contain NK1 and is not activated by SP; these neurons may release NO via alternative mechanisms. The possible mechanisms by which intracallosal neurons release NO are also reviewed.

摘要

胼胝体(cc)含有产生一氧化氮(NO)的神经元。由于NO是一种强效血管舒张剂,这些神经元可将神经信号转化为血管反应,而这种反应可通过功能性脑成像检测到。P物质(SP)是中枢神经系统中表达最广泛的肽类之一,它还通过其首选的神经激肽1(NK1)受体诱导细胞内钙释放,从而产生血管舒缩反应,进而通过激活神经元型一氧化氮合酶(nNOS)诱导NO生成。进行了单标记和双标记实验,以确定大鼠胼胝体中是否存在NK1免疫阳性神经元(NK1IP -n)以及NK1与nNOS共定位的程度。可见NK1IP -n在胼胝体中构成一个大的神经元群体,其分布与nNOS免疫阳性神经元(nNOSIP -n)相似。NK1IP -n在胼胝体外侧较多,在更内侧部分逐渐减少,在内侧部分数量很少或不存在。胼胝体内的NK1IP -n及其树突被强烈标记,可分为四种形态类型:双极型、圆形、多边形和锥体型。共聚焦显微镜检查表明,几乎所有NK1IP -n都含有nNOS(96.43%),并且84.59%的nNOSIP -n共表达NK1。这些数据表明,胼胝体内的大多数神经元可因SP的作用而释放NO。一小部分nNOSIP -n不含有NK1,也不受SP激活;这些神经元可能通过其他机制释放NO。本文还综述了胼胝体内神经元释放NO的可能机制。

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