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大鼠岛叶皮质中δ-阿片受体和甲硫氨酸脑啡肽免疫反应性的超微结构定位

Ultrastructural localization of delta-opioid receptor and Met5-enkephalin immunoreactivity in rat insular cortex.

作者信息

Svingos A L, Cheng P Y, Clarke C L, Pickel V M

机构信息

Department of Neurology and Neuroscience, Cornell University Medical College, New York, NY 10021, USA.

出版信息

Brain Res. 1995 Nov 27;700(1-2):25-39. doi: 10.1016/0006-8993(95)00977-x.

Abstract

The insular cortex has been implicated in the reinforcing properties of opiates as well as in the integration of responses to sensory-motor stimulation. Moreover, the delta-opioid receptor (DOR) and the endogenous opioid ligand, Met5-enkephalin (ENK) are known to be prominently distributed in insular limbic cortex. To examine the anatomical sites for opioid activation of DOR in rat insular cortex, we used immunoperoxidase for detection of an antiserum raised against a peptide sequence unique to the DOR alone, and in combination with immunogold-silver labeling for ENK. Light microscopy showed intense DOR-like immunoreactivity (DOR-LI) in pyramidal cells and interneurons in deep laminae, and in varicose processes in both superficial and deep layers of the insular cortex. Ultrastructural analysis of layers V and VI in insular cortex showed that the most prominent immunoperoxidase labeling for DOR was in dendrites. This labeling was associated with asymmetric excitatory-type junctions postsynaptic to unlabeled terminals. Dendritic DOR-LI was also distributed along selective portions of non-synaptic plasma membranes and subsurface organelles. In dually labeled sections, dendrites containing DOR-LI sometimes received synaptic input from ENK-labeled terminals or more infrequently colocalized with ENK. Other axon terminals were exclusively immunolabeled for DOR or more rarely contained both DOR and ENK immunoreactivity. Within labeled axon terminals, distinct segments of the plasma membrane and membranes of immediately adjacent synaptic vesicles showed the largest accumulation of the peroxidase reaction product for DOR. These results indicate that in rat insular cortex DOR is primarily heteroreceptive, but also serves an autoreceptive function on certain ENK-containing neurons. Our results also provide the first ultrastructural evidence that in rat insular cortex endogenous opioids interact through the DOR (1) to modulate the postsynaptic responses to other excitatory afferents and (2) to presynaptically regulate the release of other neurotransmitters. The modulatory actions on both ENK-containing and non-ENK-containing neurons may contribute significantly to the reinforcing properties of exogenous opiates acting on the DOR in limbic cortex.

摘要

岛叶皮质与阿片类药物的强化特性以及对感觉运动刺激的反应整合有关。此外,已知δ阿片受体(DOR)和内源性阿片配体甲硫氨酸脑啡肽(ENK)在岛叶边缘皮质中分布显著。为了研究大鼠岛叶皮质中DOR的阿片类激活的解剖部位,我们使用免疫过氧化物酶检测针对仅DOR特有的肽序列产生的抗血清,并结合ENK的免疫金银染色。光学显微镜显示,在深层的锥体细胞和中间神经元以及岛叶皮质浅层和深层的曲张突起中存在强烈的DOR样免疫反应性(DOR-LI)。岛叶皮质V层和VI层的超微结构分析表明,DOR最显著的免疫过氧化物酶标记位于树突中。这种标记与未标记终末的不对称兴奋性突触后连接有关。树突状DOR-LI也分布在非突触质膜和亚表面细胞器的选择性部分。在双重标记的切片中,含有DOR-LI的树突有时接受来自ENK标记终末的突触输入,或更罕见地与ENK共定位。其他轴突终末仅对DOR进行免疫标记,或更罕见地同时含有DOR和ENK免疫反应性。在标记的轴突终末内,质膜的不同节段和紧邻的突触小泡膜显示出DOR过氧化物酶反应产物的最大积累。这些结果表明,在大鼠岛叶皮质中,DOR主要是异源性感受的,但在某些含ENK的神经元上也具有自身感受功能。我们的结果还提供了第一个超微结构证据,即在大鼠岛叶皮质中,内源性阿片类物质通过DOR相互作用:(1)调节对其他兴奋性传入的突触后反应;(2)在突触前调节其他神经递质的释放。对含ENK和不含ENK的神经元的调节作用可能对外源性阿片类物质作用于边缘皮质中的DOR的强化特性有显著贡献。

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