首页> 外文期刊>The Journal of Comparative Neurology >Localization of the Contacts Between Kenyon Cells and Aminergic Neurons in the Drosophila melanogaster Brain Using SplitGFP Reconstitution
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Localization of the Contacts Between Kenyon Cells and Aminergic Neurons in the Drosophila melanogaster Brain Using SplitGFP Reconstitution

机译:使用SplitGFP重构的果蝇黑脑中的Kenyon细胞和胺能神经元之间的接触的本地化。

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The mushroom body of the insect brain represents a neuronal circuit involved in the control of adaptive behavior, e.g., associative learning. Its function relies on the modulation of Kenyon cell activity or synaptic transmitter release by biogenic amines, e.g., octopamine, dopamine, or serotonin. Therefore, for a comprehensive understanding of the mushroom body, it is of interest not only to determine which modulatory neurons interact with Kenyon cells but also to pinpoint where exactly in the mushroom body they do so. To accomplish the latter, we made use of the GRASP technique and created transgenic Drosophila melanogaster that carry one part of a membrane-bound splitGFP in Kenyon cells, along with a cytosolic red fluorescent marker. The second part of the splitGFP is expressed in distinct neuronal populations using cell-specific Gal4 drivers. GFP is reconstituted only if these neurons interact with Kenyon cells in close proximity, which, in combination with two-photon microscopy, provides a very high spatial resolution. We characterize spatially and microstructurally distinct contact regions between Kenyon cells and dopaminergic, serotonergic, and octopaminergic/tyraminergic neurons in all subdivisions of the mushroom body. Subpopulations of dopaminergic neurons contact complementary lobe regions densely. Octopaminergic/tyraminergic neurons contact Kenyon cells sparsely and are restricted mainly to the calyx, the α'-lobes, and the γ-lobes. Contacts of Kenyon cells with serotonergic neurons are heterogeneously distributed over the entire mushroom body. In summary, the technique enables us to localize precisely a segmentation of the mushroom body by differential contacts with aminergic neurons. J. Comp. Neurol. 521:3992-4026, 2013.
机译:昆虫大脑的蘑菇体代表了参与自适应行为(例如联想学习)控制的神经元回路。其功能依赖于生物胺(例如章鱼胺,多巴胺或5-羟色胺)对Kenyon细胞活性或突触递质释放的调节。因此,为了全面了解蘑菇体,不仅要确定哪些调节神经元与Kenyon细胞相互作用,而且要查明它们在蘑菇体中的确切位置,这是令人感兴趣的。为了完成后者,我们利用GRASP技术并创建了转基因果蝇(Drosophila melanogaster),该果蝇在Kenyon细胞中带有膜结合splitGFP的一部分,并带有胞质红色荧光标记。 splitGFP的第二部分使用细胞特异性Gal4驱动程序在不同的神经元群体中表达。仅当这些神经元与Kenyon细胞紧密相互作用时,GFP才会重新构建,这与双光子显微镜相结合可提供非常高的空间分辨率。我们表征在蘑菇体的所有细分中Kenyon细胞与多巴胺能,血清素能和章胺能/酪氨酸能神经元之间在空间和微观结构上不同的接触区域。多巴胺能神经元的亚群紧密接触互补叶区域。八胺能/酪氨酸能神经元稀疏接触Kenyon细胞,并且主要局限于花萼,α'-叶和γ-叶。 Kenyon细胞与血清素能神经元的接触异质分布在整个蘑菇体内。总之,该技术使我们能够通过与胺能神经元的不同接触来精确定位蘑菇体的分割。 J.比较神经元。 521:3992-4026,2013。

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