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Dopamine-dependent long-term depression is expressed in striatal spiny neurons of both direct and indirect pathways: implications for Parkinson's disease

机译:多巴胺依赖性长期抑郁症在直接和间接途径的纹状体棘神经元中表达:对帕金森氏病的影响

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摘要

Striatal medium spiny neurons (MSNs) are divided into two subpopulations exerting distinct effects on motor behavior. Transgenic mice carrying bacterial artificial chromosome (BAC) able to confer cell type-specific expression of enhanced green fluorescent protein (eGFP) for dopamine (DA) receptors have been developed to characterize differences between these subpopulations. Analysis of these mice, in contrast with original pioneering studies, showed that striatal long-term depression (LTD) was expressed in indirect but not in the direct pathway MSNs. To address this mismatch, we applied a new approach using combined BAC technology and receptor immunohistochemistry. We demonstrate that, in physiological conditions, DA-dependent LTD is expressed in both pathways showing that the lack of synaptic plasticity found in D(1) eGFP mice is associated to behavioral deficits. Our findings suggest caution in the use of this tool and indicate that the "striatal segregation" hypothesis might not explain all synaptic dysfunctions in Parkinson's disease.
机译:纹状体多刺神经元(MSNs)分为两个亚群,对运动行为产生独特的影响。已开发出携带细菌人工染色体(BAC)的转基因小鼠,能够赋予多巴胺(DA)受体增强的绿色荧光蛋白(eGFP)细胞类型特异性表达,以表征这些亚群之间的差异。与最初的先驱研究相反,对这些小鼠的分析表明,纹状体长期抑郁症(LTD)以间接途径而非直接途径的MSNs表达。为了解决这种不匹配问题,我们采用了结合BAC技术和受体免疫组织化学的新方法。我们证明,在生理条件下,DA依赖性LTD在两种途径中均表达,表明在D(1)eGFP小鼠中缺乏突触可塑性与行为缺陷有关。我们的发现表明在使用该工具时要谨慎,并表明“纹状体分离”假说可能无法解释帕金森氏病的所有突触功能障碍。

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