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孤束核甘氨酸能和 GABA 能神经元标志物的共存:对共传递的启示。

Co-localisation of markers for glycinergic and GABAergic neurones in rat nucleus of the solitary tract: implications for co-transmission.

机构信息

Division of Cardiovascular & Neuronal Remodelling, LIGHT Institute, School of Medicine, University of Leeds, Leeds LS2 9JT, United Kingdom.

出版信息

J Chem Neuroanat. 2010 Oct;40(2):160-76. doi: 10.1016/j.jchemneu.2010.04.001. Epub 2010 Apr 29.

Abstract

Immunoreactive structures visualised with antibodies to glycine were prominent in areas of the nucleus of the solitary tract (NTS) surrounding the tractus solitarius, but scarcer in medial and ventral areas of the nucleus. This contrasted with a higher density, more homogenous distribution of structures labelled for gamma-aminobutyric acid (GABA). Immunolabelling of adjacent semi-thin sections nonetheless indicated a close correspondence between cells and puncta labelled by glycine and GABA antisera in certain NTS areas. With post-embedding electron microscopic immunolabelling, synaptic terminals with high, presumed transmitter levels of glycine were discriminated from terminals containing low, metabolic levels by quantitative analysis of gold particle labelling densities. In a random sample of terminals, 28.5% qualified on this basis as glycinergic (compared to 44.4% GABAergic); these glycinergic terminals targeted mainly dendritic structures and contained pleomorphic vesicles and symmetrical synapses. Serial section analysis revealed few terminals (5.2%) immunoreactive for glycine alone, with 82% of glycinergic terminals also containing high levels of GABA immunoreactivity. No evidence for co-localisation of glycine and glutamate was found. Light, confocal and electron microscopic labelling with antibodies to proteins specific for glycine and GABA synthesis, release and uptake confirmed that glycinergic terminals also containing GABA are found predominantly in more lateral areas of NTS, despite glycine receptors and the 'glial' glycine transporter (GLYT1) being expressed throughout all areas of the nucleus. The data suggest that synaptic terminals in certain functionally distinct areas of NTS co-release both inhibitory amino acids, which may account for the previously reported differential inhibitory effects of glycine and GABA on NTS neurones.

摘要

用针对甘氨酸的抗体显示的免疫反应结构在围绕孤束核的孤束核区域中很明显,但在核的内侧和腹侧区域则较少。这与 GABA(γ-氨基丁酸)标记结构的更高密度和更均匀分布形成对比。然而,相邻半薄切片的免疫标记表明,在某些 NTS 区域中,甘氨酸和 GABA 抗血清标记的细胞和点状结构之间存在密切对应关系。通过后嵌入电子显微镜免疫标记,通过对金颗粒标记密度的定量分析,区分了具有高(假定的甘氨酸递质水平)和低(代谢水平)的突触末端。在随机选择的末端中,有 28.5%根据此标准被鉴定为甘氨酸能(相比之下 GABA 能为 44.4%);这些甘氨酸能末端主要靶向树突结构,并包含多形小泡和对称突触。连续切片分析显示,仅有很少的末端(5.2%)仅对甘氨酸呈免疫反应,而 82%的甘氨酸能末端也含有高水平的 GABA 免疫反应性。没有发现甘氨酸和谷氨酸共定位的证据。用针对甘氨酸和 GABA 合成、释放和摄取的蛋白质的特异性抗体进行的光、共聚焦和电子显微镜标记证实,尽管甘氨酸受体和“胶质”甘氨酸转运体(GLYT1)在核的所有区域中都表达,但也存在含有 GABA 的甘氨酸能末端主要位于 NTS 的更外侧区域。这些数据表明,在 NTS 的某些功能上不同的区域中,突触末端可能会共同释放这两种抑制性氨基酸,这可能解释了先前报道的甘氨酸和 GABA 对 NTS 神经元的不同抑制作用。

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