脊髓疾病的体感诱发电位。

Neurologie et psychiatrie Pub Date : 1989-07-01
A Constantinovici
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引用次数: 0

摘要

对115例脊髓疾病(多发性硬化症、肌萎缩性侧索硬化症、颈椎病、亚急性合并变性、脊髓炎、脊髓损伤、肿瘤)患者的体感诱发电位(sep)进行了研究。在顶骨、脊柱(颈椎或腰椎)和Erb点三个水平记录sep。估计中枢传导时间(N9-N13和腰椎电位(LP): LP- p37)。当胫骨神经受到刺激时,最敏感的测试(95%的异常)是皮层记录的sep。间隔时间LP-P37增加,sep延迟或不可记录和不同步(在多神经病变的情况下,只有潜伏期增加,而波形正常)。在50例明确形式的多发性硬化症(MS)患者中,96%的病例宫颈电位N13异常。只有64%(32例)的正中神经刺激的皮质sep异常。10例肌萎缩侧索硬化症(ALS)患者中,6例(20%)患者对下肢刺激的皮质sep异常,仅有2例患者N13和N20异常。15例脊髓型颈椎病患者中,除2例外,其余患者胫神经刺激的sep均异常,N9-N13延迟。5例亚急性合并退行性变患者对胫神经刺激均有异常的sep。15例炎性脊髓疾病患者均出现sep异常,中枢传导时间延迟。5例脊髓损伤患者病灶上方无sep。在15例肿瘤压迫性sep患者中,依赖于神经刺激的敏感根压迫以及下肢sep均出现异常。
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Somatosensory evoked potentials in spinal cord diseases.

Somatosensory evoked potentials (SEPs) were studied in 115 patients with spinal cord diseases (multiple sclerosis, amyotrophic lateral sclerosis, cervical myelopathy, subacute combined degeneration, myelitis, spinal cord injury, tumours). The SEPs were recorded at three levels: parietal, spinal (cervical or lumbar), and at the Erb point. The central conduction time was also estimated (N9-N13 and lumbar potential (LP): LP-P37). The most sensitive test (95% abnormalities) was represented by the cortical recording of the SEPs when the tibial nerve was stimulated. The interval LP-P37 was increased, the SEPs being delayed or unrecordable and desynchronized (in cases of polyneuropathies only the latency was increased whereas the waveform was normal). In 50 patients with definite form of multiple sclerosis (MS) abnormalities of the cervical potential N13 were obtained in 96% of cases. The cortical SEPs to the median nerve stimulation were abnormal in 64% of cases only (32 patients). Of 10 patients with amyotrophic lateral sclerosis (ALS), cortical SEPs to the lower limb stimulation were abnormal in 6 patients (20%) and only 2 patients had also abnormal N13 and N20. Of 15 patients with cervical myelopathy, SEPs to the tibial nerve stimulation were abnormal and N9-N13 delayed in all but 2 patients. All the 5 patients with subacute combined degeneration had abnormal SEPs to the tibial nerve stimulation. In all the 15 patients with inflammatory spinal cord diseases, the SEPs were abnormal and the central conduction time was delayed. In 5 cases with spinal cord injury the SEPs were absent above the lesion. In 15 patients with tumoral compression SEPs to the stimulation of the nerve dependent on the sensitive root compressed as well as the lower limb SEPs were abnormal.

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