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μ阿片受体存在于大鼠海马结构中γ-氨基丁酸能神经元的树突体和轴突部分。

Mu opioid receptors are in somatodendritic and axonal compartments of GABAergic neurons in rat hippocampal formation.

作者信息

Drake C T, Milner T A

机构信息

Department of Neurology, Division of Neurobiology, Weill Medical College of Cornell University, 411 East 69th Street, New York, NY, USA.

出版信息

Brain Res. 1999 Dec 4;849(1-2):203-15. doi: 10.1016/s0006-8993(99)01910-1.

Abstract

Activation of mu opioid receptors (MORs) has a net excitatory effect in the hippocampal formation through inhibition of gamma-amino butyric acid (GABA)-containing interneurons. To determine the precise subcellular targets of MOR agonists, immunoreactivity against MOR1 and GABA was examined in single sections of the hippocampal formation prepared for dual-labeling electron microscopy. In both the CA1 region of hippocampus and the dentate gyrus, MOR-like immunoreactivity (-li) was present in neuronal somata, dendrites, axons, and axon terminals, as well as a very few glial processes. Axon terminals with MOR-li formed symmetric synapses with principal cell dendrites and somata. Many MOR-labeled profiles of all types also contained GABA-li, and the vast majority possessed the ultrastructural characteristics of interneurons. Additionally, in the dentate gyrus a very small proportion of granule cell dendrites contained MOR-li. MOR-li, identified using immunogold-silver particles, was often affiliated with the extrasynaptic regions of neuronal plasma membranes, consistent with responsiveness to diffusing endogenous neuropeptide ligands. Semiquantitative analysis of the distribution of MOR-li revealed significantly more "presynaptic" (axons and terminals) than "postsynaptic" (somata and dendrites) labeled profiles in most laminae. We conclude that in addition to previously described somatodendritic MOR-li, a substantial amount of MOR-li in hippocampal formation is presynaptic. Furthermore, MORs are almost exclusively in GABAergic interneurons.

摘要

μ阿片受体(MORs)的激活通过抑制含γ-氨基丁酸(GABA)的中间神经元,在海马结构中产生净兴奋效应。为了确定MOR激动剂的确切亚细胞靶点,在为双标记电子显微镜准备的海马结构单切片中检测了针对MOR1和GABA的免疫反应性。在海马的CA1区和齿状回中,MOR样免疫反应性(-li)存在于神经元的胞体、树突、轴突和轴突终末,以及极少数胶质细胞突起中。具有MOR-li的轴突终末与主细胞树突和胞体形成对称突触。所有类型的许多MOR标记的结构也含有GABA-li,并且绝大多数具有中间神经元的超微结构特征。此外,在齿状回中,一小部分颗粒细胞树突含有MOR-li。使用免疫金银颗粒鉴定的MOR-li通常与神经元质膜的突触外区域相关,这与对扩散的内源性神经肽配体的反应性一致。对MOR-li分布的半定量分析显示,在大多数层中,“突触前”(轴突和终末)标记的结构比“突触后”(胞体和树突)标记的结构明显更多。我们得出结论,除了先前描述的体树突MOR-li外,海马结构中大量的MOR-li是突触前的。此外,MORs几乎只存在于GABA能中间神经元中。

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