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Anti-peripheral myelin antibody in patients with demyelinating neuropathy: quantitative and kinetic determination of serum antibody by complement component 1 fixation.

机译:脱髓鞘性神经病患者的抗外周髓磷脂抗体:补体成分1固定定量和动力学测定血清抗体。

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摘要

The role of anti-peripheral nerve myelin antibody (anti-PNM Ab) in the pathogenesis of acquired demyelination of peripheral nerve is unclear, in part, due to the poor correlation between antibody and disease activity. Previous studies show that only 27-50% of patients with acute demyelinating neuropathy or Guillain-Barré syndrome (GBS) had serum Abs to peripheral nerve or PNM as demonstrated by consumption of hemolytic activity of serum complement 1 (C1) fixation and transfer assay, quantitative determinations of anti-PNM Ab showed significantly high titers in the serum of patients with GBS, chronic and recurrent polyneuritis, and paraproteinemia associated with peripheral neuropathy. All 11 patients with acute-phase GBS had Ab titers 6-56 times higher than controls. In 6 GBS patients, serial Ab determinations showed that titers were highest on admission, fell rapidly the first week, and became undetectable or barely detectable by the third week. Declining Ab titers coincided with cessation of clinical progression. In 3 GBS patients, depletion of serum IgM lowered anti-PNM Ab titers significantly, whereas IgG depletion failed to produce a similar effect. This study shows that the C1 fixation and transfer assay is a sensitive method to detect anti-PNM Ab in the serum of patients with a variety of demyelinating neuropathies and provides good correlation between Ab level and the clinical course of GBS patients. It may provide important information about the pathogenesis of the demyelinating neuropathies.
机译:抗周围神经髓鞘抗体(anti-PNM Ab)在获得性周围神经脱髓鞘的发病机制中的作用尚不清楚,部分原因是抗体与疾病活性之间的相关性较差。先前的研究显示,只有27-50%的急性脱髓鞘性神经病或Guillain-Barré综合征(GBS)的患者对周围神经或PNM具有血清Abs,这是通过消耗血清补体1(C1)固定和转移测定的溶血活性来证明的,抗PNM Ab的定量测定显示,患有GBS,慢性和复发性多发性神经炎以及与周围神经病相关的副蛋白血症的患者血清中的滴度明显较高。所有11例急性期GBS患者的Ab滴度均比对照组高6-56倍。在6名GBS患者中,Ab的连续测定表明,滴度在入院时最高,在第一周迅速下降,到第三周变得不可检测或几乎不可检测。抗体滴度下降与临床进展停止同时发生。在3名GBS患者中,血清IgM的消耗显着降低了抗PNM Ab的效价,而IgG的消耗未能产生相似的作用。这项研究表明,C1固定和转移测定法是检测患有多种脱髓鞘性神经病的患者血清中抗PNM Ab的灵敏方法,并且在Ab水平与GBS患者的临床病程之间具有良好的相关性。它可能提供有关脱髓鞘性神经病的发病机制的重要信息。

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