法布里病和多发性神经病的冷诱发电位

D. Kersebaum, M. Sendel, J. Lassen, S. Fabig, J. Forstenpointner, M. Reimer, Sima Canaan-Kühl, Jens Gaedeke, S. Rehm, J. Gierthmühlen, Ralf Baron, P. Hüllemann
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引用次数: 0

摘要

法布里病(Fabry disease,FD)通过小纤维损伤导致冷诱发痛和冷觉受损,这也发生在其他原因引起的多发性神经病(PNP)中。冷诱发电位(CEPs)可评估薄髓鞘纤维和脊髓丘脑束的完整性。在这项研究中,我们旨在通过研究 CEP 与疼痛、自律神经措施、感觉缺失和神经病理性体征之间的关联来评估 CEP 的临床价值。使用定量感觉测试(QST)进行了感觉表型分析。此外,还采用了疼痛DETECT问卷(PDQ)、法布里扫描(FabryScan)和自律神经系统测量方法。87.5%的FD患者和85.7%的PNP患者的CEP符合统计分析条件。在所有患者中,CEP 数据与冷检测损失、PDQ 项目、疼痛和自律神经测量结果有显著相关性。FD患者的CEP潜伏期异常与心频变异性项目异常相关(r = -0.684;调整后p = 0.04)。在 PNP 患者中,CEP 潜伏期与 PDQ 项目显著相关,CEP 振幅与自律神经测量相关(r = 0.688,调整后 p = 0.008;r = 0.619,调整后 p = 0.024)。此外,FD(增益范围)和 PNP 患者(损耗范围)的机械痛阈值差异显著(p = 0.01)。自律神经系统功能异常与当前疼痛、神经病理性体征和症状以及自律神经系统功能异常有关,而后者并未反映在 QST 参数中。因此,与 QST 相比,CEPs 似乎能提供更广泛的感觉神经系统信息。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cold-evoked potentials in Fabry disease and polyneuropathy
Fabry disease (FD) causes cold-evoked pain and impaired cold perception through small fiber damage, which also occurs in polyneuropathies (PNP) of other origins. The integrity of thinly myelinated fibers and the spinothalamic tract is assessable by cold-evoked potentials (CEPs). In this study, we aimed to assess the clinical value of CEP by investigating its associations with pain, autonomic measures, sensory loss, and neuropathic signs.CEPs were examined at the hand and foot dorsum of patients with FD (n = 16) and PNP (n = 21) and healthy controls (n = 23). Sensory phenotyping was performed using quantitative sensory testing (QST). The painDETECT questionnaire (PDQ), FabryScan, and measures for the autonomic nervous system were applied. Group comparisons and correlation analyses were performed.CEPs of 87.5% of the FD and 85.7% of the PNP patients were eligible for statistical analysis. In all patients combined, CEP data correlated significantly with cold detection loss, PDQ items, pain, and autonomic measures. Abnormal CEP latency in FD patients was associated with an abnormal heart frequency variability item (r = −0.684; adjusted p = 0.04). In PNP patients, CEP latency correlated significantly with PDQ items, and CEP amplitude correlated with autonomic measures (r = 0.688, adjusted p = 0.008; r = 0.619, adjusted p = 0.024). Furthermore, mechanical pain thresholds differed significantly between FD (gain range) and PNP patients (loss range) (p = 0.01).Abnormal CEPs were associated with current pain, neuropathic signs and symptoms, and an abnormal function of the autonomic nervous system. The latter has not been mirrored by QST parameters. Therefore, CEPs appear to deliver a wider spectrum of information on the sensory nervous system than QST alone.
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