首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >The role of the globus pallidus D2 subfamily of dopamine receptors in pallidal immediate early gene expression.
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The role of the globus pallidus D2 subfamily of dopamine receptors in pallidal immediate early gene expression.

机译:多巴胺受体的苍白球D2亚科在苍白立即早期基因表达中的作用。

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摘要

The globus pallidus plays an important role in basal ganglia circuitry, representing the first relay nucleus of the 'indirect pathway' of striatal efferents. In contrast to the well-characterized actions of dopamine on striatal neurons, the functional role of the dopamine innervation of globus pallidus is less well understood. Previous research showed that systemic administration of either a dopamine D2 receptor antagonist or combined dopamine D1 and D2 receptor agonists induces Fos, the protein product of the immediate early gene c-fos, in neurons of globus pallidus [Ruskin and Marshall (1997) Neuroscience 81, 79-92]. To determine whether the ability of the D2 receptor antagonist, sulpiride, to induce Fos in rat pallidal neurons is mediated by D2-like receptors in striatum or globus pallidus, intrastriatal or intrapallidal sulpiride infusions were conducted. The diffusion of intrastriatal sulpiride was estimated by measuring this antagonist's competition for N-ethoxycarbonyl-2-ethoxy-1,2-dihydroquinoline (EEDQ)-induced D2 receptor inactivation. The phenotype of the striatal neurons expressing Fos after intrastriatal infusion was assessed by combining Fos immunocytochemistry with D2 receptor mRNA in situ hybridization. Intrastriatal infusions of (-)-sulpiride (10-200 ng) dose-dependently increased the number of striatal cells expressing Fos; and the Fos-immunoreactive striatal cells were D2 receptor mRNA-expressing, the same population in which systemic D2 receptor antagonists induce Fos. Intrastriatal infusions of high (5 microg), but not low (10-200 ng), (-)-sulpiride doses also induced Fos in globus pallidus cells but the sulpiride appeared to spread to the globus pallidus. Direct intrapallidal infusions of (-)-sulpiride (50-100 ng) dose-dependently induced Fos in globus pallidus with minimal influence on striatum or other basal ganglia structures. Using sensitive in situ hybridization conditions, prominent labeling of D2 receptor mRNA was evident in globus pallidus. D2 receptor mRNA was densest in a lateral 200 microm wide band that follows the curvature of the pallidal/striatal boundary. Cellular analysis revealed silver clusters associated with D2 receptor mRNA labeling over globus pallidus neurons that were immunoreactive for neuron-specific nuclear protein. These results strongly suggest that the dopaminergic innervation of globus pallidus, acting through D2-like receptors internal to this structure, can control gene expression in pallidal neurons.
机译:苍白球在基底神经节回路中起重要作用,代表纹状体传出的“间接途径”的第一个中继核。与多巴胺对纹状体神经元的良好作用相反,对苍白球的多巴胺神经支配的功能作用了解得较少。先前的研究表明,多巴胺D2受体拮抗剂或多巴胺D1和D2受体联合激动剂的全身给药会在苍白球的神经元中诱导Fos(即早期早期基因c-fos的蛋白质产物)[Ruskin and Marshall(1997)Neuroscience 81 ,79-92]。为了确定D2受体拮抗剂舒必利在大鼠苍白球神经元中诱导Fos的能力是否由纹状体或苍白球中的D2样受体介导,进行了纹状体内或苍白球内的舒必利输注。通过测量该拮抗剂对N-乙氧基羰基-2-乙氧基-1,2-二氢喹啉(EEDQ)诱导的D2受体失活的竞争,估计纹状体内舒必利的扩散。通过结合Fos免疫细胞化学和D2受体mRNA原位杂交,评估纹状体内注入后表达Fos的纹状体神经元的表型。纹状体内注入(-)-舒必利(10-200 ng)剂量依赖性地增加了表达Fos的纹状体细胞的数量。 Fos免疫反应性纹状细胞表达D2受体mRNA,与系统性D2受体拮抗剂诱导Fos的种群相同。纹状体内高剂量(5微克)但不低剂量(10-200 ng)(-)-舒必利的输注也会在苍白球细胞中诱导Fos,但舒必利似乎扩散到苍白球。直接苍白球内输注(-)-舒必利(50-100 ng)剂量依赖性地诱导苍白球中的Fos,对纹状体或其他基底神经节结构的影响最小。使用敏感的原位杂交条件,苍白球中D2受体mRNA的显着标记是明显的。 D2受体mRNA在沿苍白/纹状体边界弯曲的侧面200微米宽带中最密集。细胞分析显示,与在苍白球神经元上标记D2受体mRNA相关的银簇,对神经元特异性核蛋白具有免疫反应性。这些结果强烈表明,苍白球的多巴胺能神经支配通过该结构内部的D2样受体起作用,可以控制苍白神经元中的基因表达。

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