STN-DBS和帕金森病药物治疗的机制和作用的神经磁研究

K. S. Sridharan
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引用次数: 0

摘要

帕金森病(PD)是一种以运动症状为主要特征的神经退行性疾病,但也有感觉症状和其他几种非运动症状。PD患者通常使用多巴胺能药物治疗数年。许多患者最终经历了药物可能无法有效控制症状以及长期多巴胺能治疗的副作用的时期。深部脑刺激(DBS)是这类患者的下一个治疗手段。DBS治疗主要包括在丘脑下核(STN)或内白球(GPi)放置刺激电极,并在锁骨下间隙植入脉冲发生器(IPG)。STN-DBS可缓解PD患者的运动症状,并显著改善PD患者的生活质量。虽然已知DBS可以改善几种症状,但DBS的作用机制仍不清楚。虽然缺乏对PD的感觉加工和治疗效果的电生理研究,但对运动任务和休息时皮质动力学的电生理研究缺乏共识。我们在三个研究中记录了PD患者的脑磁图(MEG)和肌电图(EMG): (i)休息时,(ii)正中神经刺激时,(iii)进行阶段性收缩(握紧手)时。这三项研究分别关注了静息、体感加工和运动时的皮层振荡动力学。测量在DBS治疗、未治疗(DBS冲洗)和多巴胺能药物治疗状态下进行。虽然两种治疗方法(DBS和多巴胺能药物)在所有研究中都相似地改善了运动症状,但它们在以下方面表现出不同的效果:(1)仅在DBS期间,休息时感觉运动皮质低伽马谱功率(31-45 Hz)增加(但β功率(13-30 Hz)没有变化);(2)与DBS治疗和未治疗状态相比,多巴胺能治疗状态下的体感觉加工具有更高的伽马增强(31-45 Hz, 20-60 ms);(3)与DBS期间增加的伽马功率(31-45 Hz)相比,多巴胺能治疗状态下的手部握力与运动相关的β皮质肌肉相干性(CMC, 13-30 Hz)增加。首先,我们从三项研究中推断,DBS和多巴胺能药物在改善PD症状时采用了部分不同的解剖功能途径和功能策略。其次,我们认为治疗在皮层和皮层下水平对病理振荡动力学的作用不同,并且可能通过更复杂的机制来实现,而不仅仅是在特定波段抑制病理谱功率。第三,我们迫切希望探索运动系统以外的PD治疗的作用机制。多巴胺能药物对早期体感觉加工的影响为探索治疗效果和利用电生理学研究其机制打开了大门,特别是在高阶感觉缺陷中。将这些研究结果整合到治疗机制的整体观点中可以为更好的疾病管理范例铺平道路。
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Neuromagnetic investigations of mechanisms and effects of STN-DBS and medication in Parkinson's disease
Parkinson’s disease (PD) is a neurodegenerative disorder cardinally marked by motor symptoms, but also sensory symptoms and several other non-motor symptoms. PD patients are typically treated with dopaminergic medication for several years. Many patients eventually experience bouts of periods where medication might not be able to effectively control symptoms as well as experience side-effects of long-term dopaminergic treatments. Deep brain stimulation (DBS) is an option as the next therapeutic recourse for such patients. DBS treatment essentially involves placement of stimulating electrodes in the subthalamic nucleus (STN) or the globus pallidus internum (GPi) along with an implanted pulse generator (IPG) in the sub-clavicular space. STN-DBS alleviates motor symptoms and leads to substantial improvements in quality of life for PD patients. Although DBS is known to improve several classes of symptoms, the effect mechanism of DBS is still not clear. While there is a lack of electrophysiological investigation of sensory processing and the effects of treatments in PD altogether, the electrophysiological studies of the cortical dynamics during motor tasks and at rest lack consensus. We recorded magnetoencephalography (MEG) and electromyography (EMG) from PD patients in three studies: (i) at rest, (ii) during median nerve stimulation, and (iii) while performing phasic contractions (hand gripping). The three studies focused on cortical oscillatory dynamics at rest, during somatosensory processing and during movement, respectively. The measurements were conducted in DBS-treated, untreated (DBS washout) and dopaminergic-medicated states. While both treatments (DBS and dopaminergic medication) ameliorated motor symptoms similarly in all studies, they showed differentiated effects on: (i) increased sensorimotor cortical low-gamma spectral power (31-45 Hz) (but no changes in beta power (13-30 Hz)) at rest only during DBS, (ii) somatosensory processing with higher gamma augmentation (31-45 Hz, 20-60 ms) in the dopaminergic-medicated state compared to DBS-treated and untreated states, and (iii) hand gripping with increased motor-related beta corticomuscular coherence (CMC, 13-30 Hz) during dopaminergic medication in contrast to increased gamma power (31-45 Hz) during DBS. Firstly, we infer from the three studies that DBS and dopaminergic medication employ partially different anatomo-functional pathways and functional strategies when improving PD symptoms. Secondly, we suggest that treatments act on pathological oscillatory dynamics differently at cortical and sub-cortical levels and may do so through more sophisticated mechanisms than mere suppression of the pathological spectral power in a particular band. And thirdly, we urge exploring effect mechanisms of PD treatments beyond the motor system. The effects of dopaminergic medication on early somatosensory processing has opened the door for exploring the effects of treatments and studying their mechanisms using electrophysiology, especially in higher order sensory deficits. Integration of such research findings into a holistic view on mechanisms of treatments could pave way for better disease management paradigms.
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