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与非神经病理性疼痛或无痛患者相比,中枢神经性疼痛会改变皮质运动兴奋性。

Corticomotor excitability is altered in central neuropathic pain compared with non-neuropathic pain or pain-free patients.

机构信息

Pain Center, Discipline of Neurosurgery HC-FMUSP, LIM-62, University of São Paulo, Brazil; Department of Neurology, University of São Paulo, 05403-900, São Paulo, Brazil.

Pain Center, Discipline of Neurosurgery HC-FMUSP, LIM-62, University of São Paulo, Brazil.

出版信息

Neurophysiol Clin. 2023 Jun;53(3):102845. doi: 10.1016/j.neucli.2023.102845. Epub 2023 Feb 21.

Abstract

OBJECTIVES

Central neuropathic pain (CNP) is associated with altered corticomotor excitability (CE), which can potentially provide insights into its mechanisms. The objective of this study is to describe the CE changes that are specifically related to CNP.

METHODS

We evaluated CNP associated with brain injury after stroke or spinal cord injury (SCI) due to neuromyelitis optica through a battery of CE measurements and comprehensive pain, neurological, functional, and quality of life assessments. CNP was compared to two groups of patients with the same disease: i. with non-neuropathic pain and ii. without chronic pain, matched by sex and lesion location.

RESULTS

We included 163 patients (stroke=93; SCI=70: 74 had CNP, 43 had non-neuropathic pain, and 46 were pain-free). Stroke patients with CNP had lower motor evoked potential (MEP) in both affected and unaffected hemispheres compared to non- neuropathic pain and no-pain patients. Patients with CNP had lower amplitudes of MEPs (366 μV ±464 μV) than non-neuropathic (478 ±489) and no-pain (765 μV ± 880 μV) patients, p < 0.001. Short-interval intracortical inhibition (SICI) was defective (less inhibited) in patients with CNP (2.6±11.6) compared to no-pain (0.8±0.7), p = 0.021. MEPs negatively correlated with mechanical and cold-induced allodynia. Furthermore, classifying patients' results according to normative data revealed that at least 75% of patients had abnormalities in some CE parameters and confirmed MEP findings based on group analyses.

DISCUSSION

CNP is associated with decreased MEPs and SICI compared to non-neuropathic pain and no-pain patients. Corticomotor excitability changes may be helpful as neurophysiological markers of the development and persistence of pain after CNS injury, as they are likely to provide insights into global CE plasticity changes occurring after CNS lesions associated with CNP.

摘要

目的

中枢性神经病理性疼痛(CNP)与皮质运动兴奋性(CE)改变有关,这可能为其发病机制提供新的见解。本研究旨在描述与 CNP 相关的特定 CE 变化。

方法

我们通过一系列 CE 测量和全面的疼痛、神经、功能和生活质量评估,评估了由视神经脊髓炎引起的中风或脊髓损伤(SCI)后与脑损伤相关的 CNP。将 CNP 与具有相同疾病的两组患者进行比较:i. 无神经病理性疼痛,ii. 无慢性疼痛,按性别和病变部位匹配。

结果

我们纳入了 163 名患者(中风=93;SCI=70:74 例患有 CNP,43 例患有非神经病理性疼痛,46 例无疼痛)。与非神经病理性疼痛和无疼痛患者相比,患有 CNP 的中风患者在受影响和未受影响的半球中运动诱发电位(MEP)均较低。患有 CNP 的患者的 MEP 振幅较低(366μV±464μV),而非神经病理性疼痛(478±489μV)和无疼痛(765μV±880μV)患者,p<0.001。与无疼痛患者(0.8±0.7)相比,CNP 患者的短程皮质内抑制(SICI)受损(抑制减少)(2.6±11.6),p=0.021。MEP 与机械性和冷诱导性痛觉过敏呈负相关。此外,根据参考值数据对患者的结果进行分类,结果显示至少 75%的患者在某些 CE 参数上存在异常,并基于组分析证实了 MEP 发现。

讨论

与非神经病理性疼痛和无疼痛患者相比,CNP 患者的 MEP 和 SICI 降低。皮质运动兴奋性变化可能有助于作为 CNS 损伤后疼痛发展和持续的神经生理标志物,因为它们可能为 CNS 损伤后与 CNP 相关的全局 CE 可塑性变化提供见解。

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