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Levodopa-induced abnormal involuntary movements correlate with altered permeability of the blood-brain-barrier in the basal ganglia

机译:左旋多巴诱导的异常不自主运动与基底神经节中血脑屏障的渗透性改变相关

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摘要

Chronic levodopa treatment leads to the appearance of dyskinesia in the majority of Parkinson's disease patients. Neurovascular dysregulation in putaminal and pallidal regions is thought to be an underlying feature of this complication of treatment. We used microPET to study unilaterally lesioned 6-hydroxydopamine rats that developed levodopa-induced abnormal involuntary movements (AIMs) after three weeks of drug treatment. Animals were scanned with [15O]-labeled water and [18F]-fluorodeoxyglucose, to map regional cerebral blood flow and glucose metabolism, and with [11C]-isoaminobutyric acid (AIB), to assess blood-brain-barrier (BBB) permeability, following separate injections of levodopa or saline. Multitracer scan data were acquired in each animal before initiating levodopa treatment, and again following the period of daily drug administration. Significant dissociation of vasomotor and metabolic levodopa responses was seen in the striatum/globus pallidus (GP) of the lesioned hemisphere. These changes were accompanied by nearby increases in [11C]-AIB uptake in the ipsilateral GP, which correlated with AIMs scores. Histopathological analysis revealed high levels of microvascular nestin immunoreactivity in the same region. The findings demonstrate that regional flow-metabolism dissociation and increased BBB permeability are simultaneously induced by levodopa within areas of active microvascular remodeling, and that such changes correlate with the severity of dyskinesia.
机译:慢性左旋多巴治疗导致大多数帕金森氏病患者出现运动障碍。认为睑板区和苍白质区的神经血管失调是这种治疗并发症的潜在特征。我们使用microPET研究了单侧病变的6-羟基多巴胺大鼠,该大鼠在药物治疗三周后出现了左旋多巴诱导的异常不自主运动(AIM)。用[15O]标记的水和[18F]-氟脱氧葡萄糖对动物进行扫描,以绘制局部脑血流和葡萄糖代谢图,并使用[11C]-异氨基丁酸(AIB)进行扫描,以评估血脑屏障(BBB)的通透性,分别注射左旋多巴或生理盐水后。在开始左旋多巴治疗之前以及在每天给药后再次在每只动物中获取多示踪剂扫描数据。在病变半球的纹状体/苍白球(GP)中观察到血管舒缩和代谢性左旋多巴反应显着分离。这些变化伴随着同侧GP的[11C] -AIB摄取附近增加,这与AIMs评分相关。组织病理学分析显示在同一区域中高水平的微血管巢蛋白免疫反应性。这些发现表明左旋多巴在活跃的微血管重塑区域内同时诱导了局部血流代谢解离和血脑屏障通透性增加,并且这种变化与运动障碍的严重程度有关。

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