Neuronal plasticity and cerebellar circuitry
神经元可塑性和小脑回路
基本信息
- 批准号:7477499
- 负责人:
- 金额:$ 30.18万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2007
- 资助国家:美国
- 起止时间:2007-08-01 至 2012-07-31
- 项目状态:已结题
- 来源:
- 关键词:CellsCerebellar DiseasesCerebellumClassComplexContralateralDendritesDepthFiberGolgi ApparatusGreen Fluorescent ProteinsInferiorInjection of therapeutic agentInterneuronsIpsilateralKetamineLabelLabyrinthLeftMeasuresMedial Dorsal NucleusMediatingMessenger RNAMethodsMicroRNAsMolecularMusNeuronal PlasticityOligonucleotidesOlives - dietaryOutputPathway interactionsPatientsPatternPhasePhysiologicalPhysiologyProteinsPurkinje CellsRNA InterferenceRelative (related person)ResearchResearch PersonnelRoleSideSignal TransductionSpeedStimulusSystemTechniquesTestingTimeViral VectorXylazineadeno-associated viral vectorbasecell typegamma-Aminobutyric Acidgranule cellin vivoknock-downlabyrinthectomymetabotropic glutamate receptor 2mossy fiberneurobiotinprogramspromoterreceptorresearch studysynthetic enzymetheoriesuvulavector
项目摘要
DESCRIPTION (provided by applicant): In vivo analysis of cerebellar circuitry has focused almost exclusively on Purkinje cells, identified by their iconic patterns of complex and simple spikes (CSs and SSs). However, views of cerebellar function based exclusively on the physiology of Purkinje cells ignore the role of interneurons and distort the attributes of cerebellar afferent systems. It is universally assumed that SSs are modulated by the activity of the mossy fiber-granule cell-parallel fiber projection to Purkinje cell dendrites. In fact, during natural vestibular stimulation, vestibular primary afferent mossy fiber afferents discharge out of phase with the SSs recorded from nodular Purkinje cells. Consequently, it is unlikely that the cerebellar output signal merely reflects a gain-controlled version of the mossy fiber input signal. We proposed that SS modulation reflects the action of climbing fibers on cerebellar interneurons. We will test specific versions of this hypothesis by recording from identified interneurons. We have three objectives. First, we will record extracellularly from interneurons in the uvula-nodulus of anesthetized mice during natural vestibular stimulation. Interneurons will be labeled juxtacellularly with neurobiotin. The depth and phase of modulation of interneuronal discharge relative to that of Purkinje cell CSs and SSs will indicate which interneurons could modulate SSs. Second, we will study how the modulated activity of interneurons and Purkinje cells is altered by a unilateral labyrinthectomy (UL). Following a UL, the ipsilateral uvula-nodulus is accessible to vestibular information mediated only by climbing fibers whose modulation depends on the contralateral, intact labyrinth. Third, we will also make microlesions in the p-nucleus and dorsomedial cell column (dmcc) in the contralateral inferior olive. This will leave one side of the cerebellum accessible to vestibular information mediated only by vestibular mossy fibers. We will compare the effects of reduced vestibular signaling on interneurons and Purkinje cells. Fourth, we will microinject miRNAs in viral vectors with a cell specific promoter to selectively reduce expression of GABA-A alpha 1 receptors in nodular Purkinje cells. Fifth, we will also use miRNAs to selectively reduce synthesis of GABA in Golgi cells. We will analyze the effects of "knocking down" GABAergic signaling in these two cell types. We will characterize the stimulus-modulated functions of identified interneurons for the first time. We will interfere with cerebellar circuitry at a cellular level and test the role of interneurons in the modulation of SSs. The proposed research will speed application of molecular techniques to the treatment of patients with cerebellar disorders.
描述(申请人提供):对小脑回路的活体分析几乎完全集中在浦肯野细胞上,通过它们复杂和简单的棘波的标志性模式(css和sss)来识别。然而,完全基于浦肯野细胞生理学的小脑功能观点忽视了中间神经元的作用,扭曲了小脑传入系统的属性。人们普遍认为SSS是由苔藓纤维-颗粒细胞-平行纤维投射到浦肯野细胞树突的活动调节的。事实上,在自然的前庭刺激中,前庭初级传入苔藓纤维传入放电与从结节浦肯野细胞记录到的SSS不同步。因此,小脑输出信号不太可能仅仅反映苔藓纤维输入信号的增益控制版本。我们认为SS的调制反映了攀爬纤维对小脑中间神经元的作用。我们将通过记录已识别的中间神经元来测试这一假说的特定版本。我们有三个目标。首先,我们将记录自然前庭刺激时麻醉小鼠悬雍垂结节中的中间神经元的细胞外记录。中间神经元将与神经生物素并列标记。神经元间放电相对于浦肯野细胞、SS和SSS的调制深度和时相将指示哪些中间神经元可以调制SSS。其次,我们将研究单侧迷路切除术(UL)如何改变中间神经元和浦肯野细胞的调节活动。UL手术后,同侧悬垂结节仅通过攀升纤维获得前庭信息,而攀升纤维的调节依赖于对侧完整的迷路。第三,我们还将在对侧下橄榄的p核和背内侧细胞柱(DMCC)进行微损伤。这将使小脑的一侧仅通过前庭苔藓纤维传递前庭信息。我们将比较前庭信号减少对中间神经元和浦肯野细胞的影响。第四,我们将在带有细胞特异性启动子的病毒载体中微量注射miRNAs,以选择性地减少结节浦肯野细胞中GABA-Aα1受体的表达。第五,我们还将使用miRNAs选择性地减少高尔基体细胞中GABA的合成。我们将分析“击倒”GABA能信号在这两种细胞类型中的作用。我们将首次表征已识别的中间神经元的刺激调制功能。我们将在细胞水平上干扰小脑回路,并测试中间神经元在SSS调制中的作用。这项拟议的研究将加快分子技术在小脑疾病患者治疗中的应用。
项目成果
期刊论文数量(0)
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{{ truncateString('NEAL H BARMACK', 18)}}的其他基金
Vestibulo-cerebellar contribution to spatial adaptation
前庭小脑对空间适应的贡献
- 批准号:
6876527 - 财政年份:2004
- 资助金额:
$ 30.18万 - 项目类别:
Vestibulo-cerebellar contribution to spatial adaptation
前庭小脑对空间适应的贡献
- 批准号:
7934470 - 财政年份:2004
- 资助金额:
$ 30.18万 - 项目类别:
Vestibulo-cerebellar contribution to spatial adaptation
前庭小脑对空间适应的贡献
- 批准号:
7782264 - 财政年份:2004
- 资助金额:
$ 30.18万 - 项目类别:
Vestibulo-cerebellar contribution to spatial adaptation
前庭小脑对空间适应的贡献
- 批准号:
8118509 - 财政年份:2004
- 资助金额:
$ 30.18万 - 项目类别:
Vestibulo-cerebellar contribution to spatial adaptation
前庭小脑对空间适应的贡献
- 批准号:
7014554 - 财政年份:2004
- 资助金额:
$ 30.18万 - 项目类别:
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