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Brain connectivity changes when comparing effects of subthalamic deep brain stimulation with levodopa treatment in Parkinsons disease

机译:比较丘脑深部脑刺激与左旋多巴治疗帕金森病的效果

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摘要

Levodopa and, later, deep brain stimulation (DBS) have become the mainstays of therapy for motor symptoms associated with Parkinson's disease (PD). Although these therapeutic options lead to similar clinical outcomes, the neural mechanisms underlying their efficacy are different. Therefore, investigating the differential effects of DBS and levodopa on functional brain architecture and associated motor improvement is of paramount interest. Namely, we expected changes in functional brain connectivity patterns when comparing levodopa treatment with DBS.Clinical assessment and functional magnetic resonance imaging (fMRI) was performed before and after implanting electrodes for DBS in the subthalamic nucleus (STN) in 13 PD patients suffering from severe levodopa-induced motor fluctuations and peak-of-dose dyskinesia. All measurements were acquired in a within subject-design with and without levodopa treatment, and with and without DBS. Brain connectivity changes were computed using eigenvector centrality (EC) that offers a data-driven and parameter-free approach—similarly to Google's PageRank algorithm—revealing brain regions that have an increased connectivity to other regions that are highly connected, too. Both levodopa and DBS led to comparable improvement of motor symptoms as measured with the Unified Parkinson's Disease Rating Scale motor score (UPDRS-III). However, this similar therapeutic effect was underpinned by different connectivity modulations within the motor system. In particular, EC revealed a major increase of interconnectedness in the left and right motor cortex when comparing DBS to levodopa. This was accompanied by an increase of connectivity of these motor hubs with the thalamus and cerebellum.We observed, for the first time, significant functional connectivity changes when comparing the effects of STN DBS and oral levodopa administration, revealing different treatment-specific mechanisms linked to clinical benefit in PD. Specifically, in contrast to levodopa treatment, STN DBS was associated with increased connectivity within the cortico-thalamo-cerebellar network. Moreover, given the favorable effects of STN DBS on motor complications, the changes in the patients' clinical profile might also contribute to connectivity changes associated with STN-DBS. Understanding the observed connectivity changes may be essential for enhancing the effectiveness of DBS treatment, and for better defining the pathophysiology of the disrupted motor network in PD.
机译:左旋多巴以及后来的深部脑刺激(DBS)已成为治疗与帕金森氏病(PD)相关的运动症状的主要手段。尽管这些治疗选择导致相似的临床结果,但其功效所依据的神经机制却不同。因此,研究DBS和左旋多巴对功能性大脑结构和相关运动改善的不同作用至关重要。也就是说,我们预计左旋多巴治疗与DBS相比,功能性大脑连接模式会发生变化。在13例重症PD患者中,在丘脑下核(STN)植入DBS电极之前和之后进行了临床评估和功能磁共振成像(fMRI)左旋多巴引起的运动波动和剂量峰值运动障碍。所有测量均在受试者体内进行,有或没有左旋多巴治疗,有或没有DBS。大脑连接性变化是使用特征向量中心性(EC)来计算的,它提供了一种数据驱动且无参数的方法(类似于Google的PageRank算法),揭示了与其他高度连接的区域也具有更高连接性的大脑区域。用统一帕金森氏病评分量表运动评分(UPDRS-III)衡量,左旋多巴和DBS均可导致运动症状的相应改善。但是,这种相似的治疗效果是由电机系统内不同的连接调制所支撑的。尤其是,与DBS与左旋多巴相比,EC揭示了左右运动皮层的相互连接性显着增加。这伴随着这些运动枢纽与丘脑和小脑的连接性增加。我们首次观察到,在比较STN DBS和口服左旋多巴的效果时,功能连接性发生了显着变化,揭示了不同的治疗特异性机制PD的临床获益。具体而言,与左旋多巴治疗相反,STN DBS与皮质-丘脑-小脑网络内的连通性增加相关。此外,鉴于STN DBS对运动并发症的有利影响,患者临床资料的变化也可能导致与STN-DBS相关的连接性变化。了解观察到的连通性变化对于增强DBS治疗的有效性以及更好地确定PD中运动神经网络的病理生理可能至关重要。

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