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非人类灵长类动物中一氧化氮受体可溶性鸟苷酸环化酶亚基α(2)/β(1)的小脑定位

Cerebellar localization of the NO-receptive soluble guanylyl cyclase subunits-alpha(2)/beta (1) in non-human primates.

作者信息

Bidmon Hans-J, Mohlberg Hartmut, Habermann Gunnar, Buse Eberhard, Zilles Karl, Behrends Sönke

机构信息

C.& O. Vogt Institute of Brain Research, Bldg. 22.03, University St. 1, 40225 Düsseldorf, Germany.

出版信息

Cell Tissue Res. 2006 Dec;326(3):707-14. doi: 10.1007/s00441-006-0246-9. Epub 2006 Jul 4.

Abstract

Nitric-oxide-sensitive guanylyl cyclase (NO-sGC) plays a pivotal role in many second messenger cascades. Neurotransmission- and neuropathology-related changes in NO-sGC have been suggested. However, the cellular localization of NO-sGC in primate brains, including humans, remains unknown. Biochemical evidence has linked the alpha(2)-subunit of NO-sGC directly to neurotransmission in rodents. Here, we have used a recently characterized subunit-specific antibody for the localization of the alpha(2)-subunit on sections from the cerebelli of the common marmoset (Callithrix jacchus; New World monkey) and macaque monkeys (Macaca mulatta, M. fascicularis; Old World monkeys). In contrast to the more ubiquitous cytoplasmic presence of subunit-beta(1), the alpha(2)-subunit is mainly confined to the somato-dendritic membrane including the spines of the Purkinje cells. Only limited colocalization with presynaptically localized synaptophysin has been seen under our staining conditions, indicating a higher abundance of subunit-alpha(2) at the postsynaptic site. This localization indicates that subunit-alpha(2) links NO-sGC to neurotransmission, whereas subunit-beta(1) may act as a cytoplasmic regulator/activator by contributing to active heterodimer formation via translocation from the cytoplasm to the cell membrane. The last-mentioned action may be a prerequisite for generating nitric-oxide-dependent, subcellular, and postsynaptically localized cGMP signals along neuronal processes.

摘要

一氧化氮敏感型鸟苷酸环化酶(NO-sGC)在许多第二信使级联反应中起关键作用。有研究表明,NO-sGC与神经传递和神经病理学相关的变化有关。然而,包括人类在内的灵长类动物大脑中NO-sGC的细胞定位仍不清楚。生化证据表明,啮齿动物中NO-sGC的α(2)亚基直接与神经传递有关。在这里,我们使用了一种最近鉴定的亚基特异性抗体,来定位普通狨猴(Callithrix jacchus;新世界猴)和猕猴(Macaca mulatta、M. fascicularis;旧世界猴)小脑切片上的α(2)亚基。与更普遍存在于细胞质中的β(1)亚基不同,α(2)亚基主要局限于包括浦肯野细胞树突棘在内的体树突膜。在我们的染色条件下,仅观察到与突触前定位的突触素的有限共定位,这表明α(2)亚基在突触后位点的丰度更高。这种定位表明,α(2)亚基将NO-sGC与神经传递联系起来,而β(1)亚基可能通过从细胞质转运到细胞膜,促进活性异二聚体的形成,从而作为细胞质调节剂/激活剂发挥作用。上述作用可能是沿神经元过程产生一氧化氮依赖性、亚细胞和突触后定位的环磷酸鸟苷信号的先决条件。

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