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D(2) 受体接受旁分泌神经传递,并且始终针对甲壳类动物口面神经节系统中特定神经元的突触结构子集进行靶向定位。

D(2) receptors receive paracrine neurotransmission and are consistently targeted to a subset of synaptic structures in an identified neuron of the crustacean stomatogastric nervous system.

机构信息

Department of Biology, Georgia State University, Atlanta, Georgia 30303, USA.

出版信息

J Comp Neurol. 2010 Feb 1;518(3):255-76. doi: 10.1002/cne.22225.

Abstract

Dopamine (DA) modulates motor systems in phyla as diverse as nematodes and arthropods up through chordates. A comparison of dopaminergic systems across a broad phylogenetic range should reveal shared organizing principles. The pyloric network, located in the stomatogastric ganglion (STG), is an important model for neuromodulation of motor networks. The effects of DA on this network have been well characterized at the circuit and cellular levels in the spiny lobster, Panulirus interruptus. Here we provide the first data about the physical organization of the DA signaling system in the STG and the function of D(2) receptors in pyloric neurons. Previous studies showed that DA altered intrinsic firing properties and synaptic output in the pyloric dilator (PD) neuron, in part by reducing calcium currents and increasing outward potassium currents. We performed single cell reverse transcriptase-polymerase chain reaction (RT-PCR) experiments to show that PD neurons exclusively expressed a type 2 (D(2alphaPan)) DA receptor. This was confirmed by using confocal microscopy in conjunction with immunohistochemistry (IHC) on STG whole-mount preparations containing dye-filled PD neurons. Immunogold electron microscopy showed that surface receptors were concentrated in fine neurites/terminal swellings and vesicle-laden varicosities in the synaptic neuropil. Double-label IHC experiments with tyrosine hydroxylase antiserum suggested that the D(2alphaPan) receptors received volume neurotransmissions. Receptors were further mapped onto three-dimensional models of PD neurons built from Neurolucida tracings of confocal stacks from the IHC experiments. The data showed that D(2alphaPan) receptors were selectively targeted to approximately 40% of synaptic structures in any given PD neuron, and were nonuniformly distributed among neurites.

摘要

多巴胺(DA)调节从线虫和节肢动物到脊索动物等各个门的运动系统。对广泛的系统发育范围内的多巴胺系统进行比较,应该可以揭示出共同的组织原则。位于口胃神经节(STG)中的幽门网络是调节运动网络的神经调节剂的重要模型。已经在棘龙虾 Panulirus interruptus 中从电路和细胞水平上很好地描述了 DA 对该网络的影响。在这里,我们提供了有关 STG 中 DA 信号系统的物理组织以及 D(2)受体在幽门神经元中的功能的第一个数据。以前的研究表明,DA 通过减少钙电流和增加外向钾电流,改变了幽门扩张神经元(PD)的固有放电特性和突触输出。我们进行了单细胞逆转录聚合酶链反应(RT-PCR)实验,以证明 PD 神经元仅表达 2 型(D(2alphaPan))DA 受体。这通过在 STG 整体标本上进行共聚焦显微镜检查并用免疫组织化学(IHC)结合对包含染料填充的 PD 神经元的 PD 神经元进行了证实。免疫金电子显微镜显示,表面受体集中在突触神经丛中的细神经突/末端肿胀和充满囊泡的膨体中。用酪氨酸羟化酶抗血清进行的双重免疫标记 IHC 实验表明,D(2alphaPan)受体接受容积神经传递。然后将受体进一步映射到 PD 神经元的三维模型上,该模型是从 IHC 实验的共聚焦堆栈的 Neurolucida 轨迹构建的。数据表明,D(2alphaPan)受体选择性地靶向给定 PD 神经元中的大约 40%的突触结构,并且在神经突之间不均匀分布。

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