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产生副甲状腺素的皮质中间神经元在近端接受抑制性输入,在远端树突接受皮质兴奋性输入。

Parvalbumin-producing cortical interneurons receive inhibitory inputs on proximal portions and cortical excitatory inputs on distal dendrites.

机构信息

Department of Morphological Brain Science, Graduate School of Medicine, Kyoto University, Kyoto 606-8501, Japan.

出版信息

Eur J Neurosci. 2012 Mar;35(6):838-54. doi: 10.1111/j.1460-9568.2012.08027.x.

Abstract

To examine inputs to parvalbumin (PV)-producing interneurons, we generated transgenic mice expressing somatodendritic membrane-targeted green fluorescent protein specifically in the interneurons, and completely visualized their dendrites and somata. Using immunolabeling for vesicular glutamate transporter (VGluT)1, VGluT2, and vesicular GABA transporter, we found that VGluT1-positive terminals made contacts 4- and 3.1-fold more frequently with PV-producing interneurons than VGluT2-positive and GABAergic terminals, respectively, in the primary somatosensory cortex. Even in layer 4, where VGluT2-positive terminals were most densely distributed, VGluT1-positive inputs to PV-producing interneurons were 2.4-fold more frequent than VGluT2-positive inputs. Furthermore, although GABAergic inputs to PV-producing interneurons were as numerous as VGluT2-positive inputs in most cortical layers, GABAergic inputs clearly preferred the proximal dendrites and somata of the interneurons, indicating that the sites of GABAergic inputs were more optimized than those of VGluT2-positive inputs. Simulation analysis with a PV-producing interneuron model compatible with the present morphological data revealed a plausible reason for this observation, by showing that GABAergic and glutamatergic postsynaptic potentials evoked by inputs to distal dendrites were attenuated to 60 and 87%, respectively, of those evoked by somatic inputs. As VGluT1-positive and VGluT2-positive axon terminals were presumed to be cortical and thalamic glutamatergic inputs, respectively, cortical excitatory inputs to PV-producing interneurons outnumbered the thalamic excitatory and intrinsic inhibitory inputs more than two-fold in any cortical layer. Although thalamic inputs are known to evoke about two-fold larger unitary excitatory postsynaptic potentials than cortical ones, the present results suggest that cortical inputs control PV-producing interneurons at least as strongly as thalamic inputs.

摘要

为了研究 PV 阳性中间神经元的传入信号,我们构建了一种转基因小鼠,在中间神经元中特异性表达 somatodendritic 膜靶向绿色荧光蛋白,从而可以完整地观察其树突和胞体。利用囊泡谷氨酸转运体(VGluT)1、VGluT2 和囊泡 GABA 转运体的免疫标记,我们发现初级体感皮层中,VGluT1 阳性终末与 PV 阳性中间神经元形成的突触分别比 VGluT2 阳性终末和 GABA 能终末多 4 倍和 3.1 倍。即使在 VGluT2 阳性终末最密集的第 4 层,VGluT1 阳性传入到 PV 阳性中间神经元的频率也比 VGluT2 阳性传入高出 2.4 倍。此外,尽管 GABA 能传入到 PV 阳性中间神经元的数量与 VGluT2 阳性传入相当,但在大多数皮层层中,GABA 能传入明显偏向于中间神经元的近侧树突和胞体,表明 GABA 能传入的部位比 VGluT2 阳性传入更优化。利用与本研究形态学数据相兼容的 PV 阳性中间神经元模型进行的仿真分析表明,这种现象的一个可能原因是,输入到远侧树突的 GABA 能和谷氨酸能突触后电位分别被削弱到体细胞输入所诱发的 60%和 87%。由于 VGluT1 阳性和 VGluT2 阳性轴突末梢分别被认为是皮质和丘脑谷氨酸能传入,所以在任何皮层层中,皮质兴奋性传入到 PV 阳性中间神经元的数量都比丘脑兴奋性传入和内在抑制性传入多两倍以上。尽管已知丘脑传入可以诱发比皮质传入大两倍左右的单位兴奋性突触后电位,但本研究结果表明,皮质传入至少与丘脑传入一样强烈地控制 PV 阳性中间神经元。

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