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首页> 外文期刊>Behavioural Brain Research: An International Journal >Differential behavioral reinforcement effects of dopamine receptor agonists in the rat with bilateral lesion of the posterior ventral tegmental area
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Differential behavioral reinforcement effects of dopamine receptor agonists in the rat with bilateral lesion of the posterior ventral tegmental area

机译:多巴胺受体激动剂对大鼠后腹侧被盖区双侧病变的差异行为增强作用

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Dopamine dysregulation syndrome in Parkinson's disease has been attributed to dopamine replacement therapies and/or a lesion of the dopaminergic system. The dopaminergic neuronal loss targets the substantia nigra and the ventral tegmental area (VTA). We hypothesize that dopamine replacement therapy is responsible for the potential reinforcement effect in Parkinson's disease by acting on the neuronal reward circuitry. Therefore this study was designed to explore the potential motivational effect of dopamine replacement therapy in bilateral VTA-lesioned animals. The posterior (p)VTA, which project to the nucleus accumbens (NAc) constitutes the major dopamine neuronal circuitry implicated in addictive disorders. Using the conditioned place preference (CPP) behavioral paradigm, we investigated the motivational effects of dopamine receptor agonists, and cocaine in rat with a 6-OHDA bilateral lesion of the pVTA. Amongst the dopamine receptor agonists used in this study only the D2R and D3R agonists (bromocriptine, PD128907 and pramipexole), induced a significant CPP in pVTA-lesioned animals. Dopamine receptor agonists did not induce behavioral sensitization in sham animals. Moreover, confocal D2R immunostaining analysis showed a significant increase in the number of D2R per cell body in the NAc shell of pVTA lesioned rats compared to sham. This result correlated, for the first time, the dopamine receptor agonists effect with DR2 overexpression in the NAc shell of pVTA-lesioned rats. In addition, cocaine, which is known to increase dopamine release, induced behavioral sensitization in sham group but not in dopamine deprived group. Thus, the later result highlighted the importance of pVTA-NAc dopaminergic pathway in positive reinforcements. Altogether these data suggested that the implication of the dopamine replacement therapy in the appearance of dopamine dysregulation syndrome in Parkinson's disease is probably due to both neuronal degeneration in the posterior VTA and dopamine receptor sensitization in the dopamine depleted NAc.
机译:帕金森氏病中的多巴胺失调综合症已归因于多巴胺替代疗法和/或多巴胺能系统病变。多巴胺能神经元损失的目标是黑质和腹侧被盖区(VTA)。我们假设多巴胺替代疗法通过作用于神经元奖赏回路来负责帕金森氏病的潜在增强作用。因此,本研究旨在探讨多巴胺替代疗法对双侧VTA病变动物的潜在激励作用。投射到伏隔核(NAc)的后(p)VTA构成了与成瘾性疾病有关的主要多巴胺神经元回路。使用条件性位置偏爱(CPP)行为范例,我们研究了多巴胺受体激动剂和可卡因在pVTA的6-OHDA双侧病变中对大鼠的刺激作用。在这项研究中使用的多巴胺受体激动剂中,只有D2R和D3R激动剂(溴隐亭,PD128907和普拉克索)在受pVTA损伤的动物中诱导了显着的CPP。多巴胺受体激动剂不会在假动物中引起行为敏化。此外,共聚焦D2R免疫染色分析显示,与假手术相比,pVTA损伤大鼠的NAc壳中每个细胞体中的D2R数量显着增加。该结果首次使多巴胺受体激动剂与pVTA损伤大鼠的NAc外壳中DR2过表达有关。此外,已知可卡因会增加多巴胺的释放,在假手术组中引起行为敏化,而在多巴胺缺乏组则不会。因此,后面的结果强调了pVTA-NAc多巴胺能途径在正强化中的重要性。总而言之,这些数据表明,在帕金森氏病中出现多巴胺替代疗法对多巴胺失调综合症的影响可能是由于后VTA中的神经元变性和多巴胺消耗的NAc中的多巴胺受体敏化。

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