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首页> 外文期刊>Frontiers in Neural Circuits >Modulation of Specific Sensory Cortical Areas by Segregated Basal Forebrain Cholinergic Neurons Demonstrated by Neuronal Tracing and Optogenetic Stimulation in Mice
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Modulation of Specific Sensory Cortical Areas by Segregated Basal Forebrain Cholinergic Neurons Demonstrated by Neuronal Tracing and Optogenetic Stimulation in Mice

机译:分离的基底前脑胆碱能神经元在小鼠的神经元示踪和光遗传学刺激下对特定感觉皮层区域的调节。

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Neocortical cholinergic activity plays a fundamental role in sensory processing and cognitive functions. Previous results have suggested a refined anatomical and functional topographical organization of basal forebrain (BF) projections that may control cortical sensory processing in a specific manner. We have used retrograde anatomical procedures to demonstrate the existence of specific neuronal groups in the BF involved in the control of specific sensory cortices. Fluoro-Gold (FlGo) and Fast Blue (FB) fluorescent retrograde tracers were deposited into the primary somatosensory (S1) and primary auditory (A1) cortices in mice. Our results revealed that the BF is a heterogeneous area in which neurons projecting to different cortical areas are segregated into different neuronal groups. Most of the neurons located in the horizontal limb of the diagonal band of Broca (HDB) projected to the S1 cortex, indicating that this area is specialized in the sensory processing of tactile stimuli. However, the nucleus basalis magnocellularis (B) nucleus shows a similar number of cells projecting to the S1 as to the A1 cortices. In addition, we analyzed the cholinergic effects on the S1 and A1 cortical sensory responses by optogenetic stimulation of the BF neurons in urethane-anesthetized transgenic mice. We used transgenic mice expressing the light-activated cation channel, channelrhodopsin-2, tagged with a fluorescent protein (ChR2-YFP) under the control of the choline-acetyl transferase promoter (ChAT). Cortical evoked potentials were induced by whisker deflections or by auditory clicks. According to the anatomical results, optogenetic HDB stimulation induced more extensive facilitation of tactile evoked potentials in S1 than auditory evoked potentials in A1, while optogenetic stimulation of the B nucleus facilitated either tactile or auditory evoked potentials equally. Consequently, our results suggest that cholinergic projections to the cortex are organized into segregated pools of neurons that may modulate specific cortical areas.
机译:新皮层胆碱能活性在感觉加工和认知功能中起基本作用。先前的结果表明,基底前脑(BF)投影的解剖学和功能拓扑结构精细,可以以特定方式控制皮质的感觉处理。我们已经使用逆行解剖程序来证明高炉中特定神经元群的存在与特定感觉皮质的控制有关。荧光金(FlGo)和坚牢蓝(FB)荧光逆行示踪剂沉积在小鼠的主要体感(S1)和主要听觉(A1)皮层中。我们的研究结果表明,BF是一个异质区域,其中投射到不同皮层区域的神经元被分为不同的神经元组。位于Broca(HDB)对角带水平臂上的大多数神经元都投射到S1皮质,表明该区域专门用于触觉刺激的感觉处理。但是,基底大细胞核(B)核显示出与A1皮质相似的细胞数量。此外,我们分析了尿烷麻醉的转基因小鼠中BF神经元的光遗传刺激对S1和A1皮质感觉反应的胆碱能作用。我们使用表达在胆碱乙酰基转移酶启动子(ChAT)的控制下标记有荧光蛋白(ChR2-YFP)的光激活阳离子通道channelrhodopsin-2的转基因小鼠。晶须偏转或听觉咔嗒声诱发了皮质诱发电位。根据解剖结果,光遗传学HDB刺激比A1的听觉诱发电位更能促进S1的触觉诱发电位,而B核的光遗传刺激同样能促进触觉或听觉诱发电位。因此,我们的研究结果表明,胆碱能投射到皮层组织成分离的神经元池,这些池可能会调节特定的皮质区域。

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