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评估小脑神经刺激对患有运动障碍的儿童和青年运动障碍型脑性瘫痪患者的综合单病例试验方案。

Protocol for combined N-of-1 trials to assess cerebellar neurostimulation for movement disorders in children and young adults with dyskinetic cerebral palsy.

作者信息

San Luciano Marta, Oehrn Carina R, Wang Sarah S, Tolmie John S, Wiltshire Allisun, Graff Rebecca E, Zhu Jennifer, Starr Philip A

机构信息

University of California, San Francisco, Weill Institute for Neurosciences.

University of California, San Francisco.

出版信息

Res Sq. 2024 Apr 1:rs.3.rs-4077387. doi: 10.21203/rs.3.rs-4077387/v1.

Abstract

BACKGROUND

Movement and tone disorders in children and young adults with cerebral palsy are a great source of disability. Deep brain stimulation (DBS) of basal ganglia targets has a major role in the treatment of isolated dystonias, but its efficacy in dyskinetic cerebral palsy (DCP) is lower, due to structural basal ganglia and thalamic damage and lack of improvement of comorbid choreoathetosis and spasticity. The cerebellum is an attractive target for DBS in DCP since it is frequently spared from hypoxic ischemic damage, it has a significant role in dystonia network models, and small studies have shown promise of dentate stimulation in improving CP-related movement and tone disorders.

METHODS

Ten children and young adults with DCP and disabling movement disorders with or without spasticity will undergo bilateral DBS in the dorsal dentate nucleus, with the most distal contact ending in the superior cerebellar peduncle. We will implant Medtronic Percept, a bidirectional neurostimulator that can sense and store brain activity and deliver DBS therapy. The efficacy of cerebellar DBS in improving quality of life and motor outcomes will be tested by a series of N-of-1 clinical trials. Each N-of-1 trial will consist of three blocks, each consisting of one month of effective stimulation and one month of sham stimulation in a random order with weekly motor and quality of life scales as primary and secondary outcomes. In addition, we will characterize abnormal patterns of cerebellar oscillatory activity measured by local field potentials from the intracranial electrodes related to clinical assessments and wearable monitors. Pre- and 12-month postoperative volumetric structural and functional MRI and diffusion tensor imaging will be used to identify candidate imaging markers of baseline disease severity and response to DBS.

DISCUSSION

Our goal is to test a cerebellar neuromodulation therapy that produces meaningful changes in function and well-being for people with CP, obtain a mechanistic understanding of the underlying brain network disorder, and identify physiological and imaging-based predictors of outcomes useful in planning further studies.

TRIAL REGISTRATION

ClinicalTrials.gov NCT06122675, first registered November 7, 2023.

摘要

背景

脑性瘫痪儿童和青年的运动及肌张力障碍是致残的重要原因。基底神经节靶点的深部脑刺激(DBS)在孤立性肌张力障碍的治疗中起主要作用,但其在运动障碍型脑性瘫痪(DCP)中的疗效较低,这是由于基底神经节和丘脑存在结构性损伤,且合并的舞蹈手足徐动症和痉挛未得到改善。小脑是DCP中DBS的一个有吸引力的靶点,因为它经常免受缺氧缺血性损伤,在肌张力障碍网络模型中起重要作用,并且小型研究已显示齿状核刺激在改善与CP相关的运动和肌张力障碍方面具有前景。

方法

10名患有DCP且伴有或不伴有痉挛的致残性运动障碍的儿童和青年将接受双侧齿状核背侧DBS,最远端触点终止于小脑上脚。我们将植入美敦力Percept,这是一种双向神经刺激器,可感知和存储脑活动并提供DBS治疗。小脑DBS改善生活质量和运动结果的疗效将通过一系列单病例临床试验进行测试。每个单病例试验将包括三个阶段,每个阶段由一个月的有效刺激和一个月的假刺激组成,顺序随机,以每周的运动和生活质量量表作为主要和次要结果。此外,我们将通过与临床评估和可穿戴监测器相关的颅内电极局部场电位来表征小脑振荡活动的异常模式。术前和术后12个月的容积性结构和功能MRI以及扩散张量成像将用于识别基线疾病严重程度和对DBS反应的候选成像标志物。

讨论

我们的目标是测试一种小脑神经调节疗法,该疗法能为CP患者的功能和健康带来有意义的改变,获得对潜在脑网络障碍的机制性理解,并确定可用于规划进一步研究的基于生理和成像的结果预测指标。

试验注册

ClinicalTrials.gov NCT06122675,首次注册于2023年11月7日。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6dc7/11030503/7aefc0a4a7ff/nihpp-rs4077387v1-f0001.jpg

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