首页> 美国卫生研究院文献>Frontiers in Neurology >Do Studies on Cortical Plasticity Provide a Rationale for Using Non-Invasive Brain Stimulation as a Treatment for Parkinson’s Disease Patients?
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Do Studies on Cortical Plasticity Provide a Rationale for Using Non-Invasive Brain Stimulation as a Treatment for Parkinson’s Disease Patients?

机译:皮质可塑性研究是否为使用非侵入性脑刺激治疗帕金森氏病患者提供了理论依据?

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摘要

Animal models of Parkinson’s disease (PD) have shown that key mechanisms of cortical plasticity such as long-term potentiation (LTP) and long-term depression (LTD) can be impaired by the PD pathology. In humans protocols of non-invasive brain stimulation, such as paired associative stimulation (PAS) and theta-burst stimulation (TBS), can be used to investigate cortical plasticity of the primary motor cortex. Through the amplitude of the motor evoked potential these transcranial magnetic stimulation methods allow to measure both LTP-like and LTD-like mechanisms of cortical plasticity. So far these protocols have reported some controversial findings when tested in PD patients. While various studies described evidence for reduced LTP- and LTD-like plasticity, others showed different results, demonstrating increased LTP-like and normal LTD-like plasticity. Recent evidence provided support to the hypothesis that these different patterns of cortical plasticity likely depend on the stage of the disease and on the concomitant administration of l-DOPA. However, it is still unclear how and if these altered mechanisms of cortical plasticity can be taken as a reliable model to build appropriate protocols aimed at treating PD symptoms by applying repetitive sessions of repetitive TMS (rTMS) or transcranial direct current stimulation (tDCS). The current article will provide an up-to-date overview of these issues together with some reflections on future studies in the field.
机译:帕金森氏病(PD)的动物模型显示,PD病理学可能会破坏诸如长期增强(LTP)和长期抑郁(LTD)等皮质可塑性的关键机制。在人类的非侵入性脑刺激方案中,例如配对联想刺激(PAS)和θ-爆发刺激(TBS),可用于研究初级运动皮层的皮质可塑性。通过运动诱发电位的幅度,这些经颅磁刺激方法可以测量皮质可塑性的LTP类和LTD类机制。到目前为止,这些协议在PD患者中进行测试时已经报告了一些有争议的发现。虽然各种研究描述了降低LTP样和LTD型可塑性的证据,但其他研究则显示了不同的结果,表明LTP样和LTD LTD样可塑性增加。最近的证据为以下假设提供了支持:这些不同的皮质可塑性模式可能取决于疾病的阶段以及同时使用1-DOPA。然而,仍然不清楚如何以及是否可以将这些改变的皮质可塑性机制作为可靠的模型,以通过应用重复性TMS(rTMS)或经颅直流电刺激(tDCS)来建立旨在治疗PD症状的适当方案。本文将提供这些问题的最新概述,以及对该领域未来研究的一些反思。

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