Cannabinoid CB1 receptors are early downregulated followed by a further upregulation in the basal ganglia of mice with deletion of specific park genes.

Moisés García-Arencibia, Concepción García, Alexander Kurz, José A Rodríguez-Navarro, Suzana Gispert-Sáchez, Maria A Mena, Georg Auburger, Justo García de Yébenes, Javier Fernández-Ruiz
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引用次数: 38

Abstract

This study was designed to examine the type of changes experienced by the CB1 receptor, a key element of the cannabinoid signaling system, in the basal ganglia of different mouse mutants generated by deletion of specific genes associated with the development of Parkinson's disease in humans [PARK1 (alpha-synuclein), PARK2 (parkin) or PARK6 (PINK1)]. We observed that CB1 receptor-mRNA levels were significantly reduced in the caudate-putamen in the three models under examination when animals were analyzed at early phases (< or = 12 months of age). This decrease was, in general, associated with a reduction in CB1 receptor binding in the substantia nigra and the globus pallidus, particularly in the case of alpha-synuclein-deficient mice. By contrast, both parameters, mRNA levels and binding for the CB1 receptor, showed an elevation in the same areas when animals were analyzed at older ages, mainly in the case of the CB1 receptor binding in the substantia nigra. In summary, our data revealed the existence of a biphasic response for CB1 receptors, with losses at early phases, when dopaminergic dysfunction is possibly the major event that takes place, followed by upregulatory responses at advanced phases characterized by the occurrence of evident nigrostriatal pathology including neuronal death in some cases.

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在特定park基因缺失的小鼠基底神经节中,大麻素CB1受体早期下调,随后进一步上调。
本研究旨在检测与人类帕金森病发展相关的特定基因[PARK1 (α -synuclein), PARK2 (parkin)或PARK6 (PINK1)]缺失所产生的不同小鼠突变体基底神经节中CB1受体(大麻素信号系统的关键元件)的变化类型。我们观察到,当动物在早期阶段(<或= 12月龄)进行分析时,所检查的三种模型的尾壳核中CB1受体mrna水平显著降低。总的来说,这种减少与黑质和苍白球中CB1受体结合的减少有关,特别是在α -突触核蛋白缺陷的小鼠中。相比之下,当动物在老年时进行分析时,这两个参数,CB1受体的mRNA水平和结合,在同一区域都显示出升高,主要是在黑质CB1受体结合的情况下。综上所述,我们的数据揭示了CB1受体的双相反应的存在,在早期阶段损失,当多巴胺能功能障碍可能是发生的主要事件时,随后在晚期阶段出现上调反应,其特征是发生明显的黑质纹状体病理,在某些情况下包括神经元死亡。
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