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慢性炎症性脱髓鞘性多发性神经病(CIDP)中的神经传导异常

[Nerve conduction abnormalities in chronic inflammatory demyelinating polyneuropathy (CIDP)].

作者信息

Baba M

机构信息

Department of Neurology, Faculty of Medicine, University of Hirosaki.

出版信息

Rinsho Shinkeigaku. 1991 Dec;31(12):1333-6.

PMID:1817802
Abstract

Changes in compound muscle action potentials (CMAPs) were evaluated in 13 cases with CIDP by using inching-stimulation technique. The presence of electrophysiological multifocal lesion distinguished CIDP from hereditary demyelinating neuropathy (HDN). The size of each CIDP lesion was sometimes as small as a few millimeters, showing a decrease in CMAP amplitude proximally. No HDN cases revealed such focal changes. It is thus important to demonstrate small lesions with CMAP changes of demyelination-type in diagnosis of CIDP. Decrease in amplitude of proximally-evoked CMAP is essential but sometimes inadequate to determine partial conduction block, because HDN may show decrease in CMAP amplitude, up to 45%, by elbow stimulation as compare to one by wrist stimulation in our series. In determining partial conduction block a standard two-point stimulation can cause an error, because that threshold is quite high over a demyelinated segment, and that a cross stimulation may occur when high voltage stimulation is applied. Multiple-sites stimulation is the most reliable technique to demonstrate convincing changes in CMAPs over small demyelinating lesions. Revival of blocked motor fibers introduces new units to CMAP. In most cases some increase in CMAP amplitude occur first, because remyelinated fibers are slowly-conducting. Some units with shorter latency occasionally revived first, which suggests a possibility of conduction block without morphological background.

摘要

采用逐点刺激技术评估了13例慢性炎性脱髓鞘性多发性神经病(CIDP)患者复合肌肉动作电位(CMAP)的变化。电生理多灶性病变的存在将CIDP与遗传性脱髓鞘性神经病(HDN)区分开来。CIDP每个病变的大小有时小至几毫米,表现为近端CMAP波幅降低。HDN病例未显示出这种局灶性变化。因此,在CIDP诊断中,通过CMAP变化来显示小病变很重要。近端诱发的CMAP波幅降低是必要的,但有时不足以确定部分传导阻滞,因为在我们的系列研究中,HDN通过肘部刺激与腕部刺激相比,CMAP波幅可降低达45%。在确定部分传导阻滞时,标准的两点刺激可能会导致错误,因为在脱髓鞘节段阈值相当高,并且施加高压刺激时可能会发生交叉刺激。多点刺激是显示小脱髓鞘病变处CMAP令人信服变化的最可靠技术。被阻滞的运动纤维的恢复为CMAP引入了新的成分。在大多数情况下,CMAP波幅首先会有一些增加,因为再髓鞘化的纤维传导缓慢。一些潜伏期较短的成分偶尔会首先恢复,这表明存在无形态学背景的传导阻滞的可能性。

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