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果蝇衰老大脑中的多巴胺能系统。

The dopaminergic system in the aging brain of Drosophila.

作者信息

White Katherine E, Humphrey Dickon M, Hirth Frank

机构信息

Department of Neuroscience, Institute of Psychiatry, Medical Research Council Centre for Neurodegeneration Research, King's College London London, UK.

出版信息

Front Neurosci. 2010 Dec 8;4:205. doi: 10.3389/fnins.2010.00205. eCollection 2010.

Abstract

Drosophila models of Parkinson's disease are characterized by two principal phenotypes: the specific loss of dopaminergic (DA) neurons in the aging brain and defects in motor behavior. However, an age-related analysis of these baseline parameters in wildtype Drosophila is lacking. Here we analyzed the DA system and motor behavior in aging Drosophila. DA neurons in the adult brain can be grouped into bilateral symmetric clusters, each comprising a stereotypical number of cells. Analysis of TH > mCD8::GFP and cell type-specific MARCM clones revealed that DA neurons show cluster-specific, stereotypical projection patterns with terminal arborization in target regions that represent distinct functional areas of the adult brain. Target areas include the mushroom bodies, involved in memory formation and motivation, and the central complex, involved in the control of motor behavior, indicating that similar to the mammalian brain, DA neurons in the fly brain are involved in the regulation of specific behaviors. Behavioral analysis revealed that Drosophila show an age-related decline in startle-induced locomotion and negative geotaxis. Motion tracking however, revealed that walking activity, and exploration behavior, but not centrophobism increase at late stages of life. Analysis of TH > Dcr2, mCD8::GFP revealed a specific effect of Dcr2 expression on walking activity but not on exploratory or centrophobic behavior, indicating that the siRNA pathway may modulate distinct DA behaviors in Drosophila. Moreover, DA neurons were maintained between early- and late life, as quantified by TH > mCD8::GFP and anti-TH labeling, indicating that adult onset, age-related degeneration of DA neurons does not occur in the aging brain of Drosophila. Taken together, our data establish baseline parameters in Drosophila for the study of Parkinson's disease as well as other disorders affecting DA neurons and movement control.

摘要

帕金森病的果蝇模型具有两种主要表型

衰老大脑中多巴胺能(DA)神经元的特异性缺失以及运动行为缺陷。然而,缺乏对野生型果蝇这些基线参数的年龄相关分析。在此,我们分析了衰老果蝇中的DA系统和运动行为。成年大脑中的DA神经元可分为双侧对称簇,每个簇包含固定数量的细胞。对TH > mCD8::GFP和细胞类型特异性MARCM克隆的分析表明,DA神经元呈现簇特异性、固定的投射模式,其终末分支位于代表成年大脑不同功能区域的靶区域。靶区域包括参与记忆形成和动机的蘑菇体以及参与运动行为控制的中央复合体,这表明与哺乳动物大脑类似,果蝇大脑中的DA神经元参与特定行为的调节。行为分析表明,果蝇在惊吓诱导的运动和负趋地性方面表现出与年龄相关的下降。然而,运动跟踪显示,在生命后期,行走活动和探索行为增加,但避中心性不增加。对TH > Dcr2、mCD8::GFP的分析表明,Dcr2表达对行走活动有特异性影响,但对探索或避中心性行为无影响,这表明siRNA途径可能调节果蝇中不同的DA行为。此外,通过TH > mCD8::GFP和抗TH标记定量分析表明,DA神经元在生命早期和晚期之间得以维持,这表明果蝇衰老大脑中不会发生成年期开始的、与年龄相关的DA神经元退化。综上所述,我们的数据为研究帕金森病以及其他影响DA神经元和运动控制的疾病建立了果蝇的基线参数。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/01f5/3002484/530c2e9a920f/fnins-04-00205-g001.jpg

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