首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Activation of terminal components of complement in patients with Guillain-Barré syndrome and other demyelinating neuropathies.
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Activation of terminal components of complement in patients with Guillain-Barré syndrome and other demyelinating neuropathies.

机译:Guillain-Barré综合征和其他脱髓鞘性神经病患者补体末端成分的激活。

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摘要

In the present study, the role of antiperipheral nerve myelin antibody (anti-PNM Ab) in demyelination by generating the terminal attack complex (C5b-9) of complement was explored in patients with Guillain-Barré syndrome (GBS) and other demyelinating neuropathies. The presence in serum of SC5b-9, an inactive C5b-9 containing S protein, was assessed quantitatively by enzyme-linked immunosorbent assay using an antibody (Ab) to neoantigens expressed on C9 when complexed with C5b-8 or after tubular polymerization. SC5b-9 was detected in all 19 GBS, four patients with paraprotein-associated neuropathy and five of six patients with chronic recurrent polyneuritis. No SC5b-9 was detected in 10 normal controls. Kinetic studies from six GBS patients showed the highest values of SC5b-9 on the 3rd to 5th d of admission; in contrast, the anti-PNM Ab were highest on the day of admission. Anti-PNM Ab fell rapidly to very low levels by the 15th to 20th d. SC5b-9 declined with similar kinetics to undetectable levels by the 30th d. Levels of Ab and SC5b-9 did not quantitatively correlate with soluble immune complexes in these patients' serum. Membrane-bound C5b-9 was also detected by immunohistochemistry in the peripheral nerves from a GBS patient. These results, which show a relationship between levels of complement-fixing anti-PNM Ab and the tissue-damaging C5b-9 complex, suggest that peripheral nerve myelin may serve as the target for Ab-mediated complement attack.
机译:在本研究中,在患有格林巴利综合征(GBS)和其他脱髓鞘性神经病的患者中,探索了通过产生补体的终末攻击复合物(C5b-9)来消除周围神经髓鞘抗体(anti-PNM Ab)的作用。当与C5b-8复合或在管状聚合后,使用抗C9上表达的新抗原的抗体(Ab),通过酶联免疫吸附法定量评估血清SC5b-9(一种含有S蛋白的无活性C5b-9)的存在。在全部19个GBS,4个伴副蛋白相关性神经病的患者和6例慢性复发性多发性神经炎患者中,有5例检测到SC5b-9。在10个正常对照中未检测到SC5b-9。对6名GBS患者的动力学研究显示,入院后第3至第5天SC5b-9的值最高。相反,抗PNM抗体在入院当天最高。抗PNM抗体在第15至20天迅速降至非常低的水平。到第30天时,SC5b-9的动力学下降至不可检测的水平。这些患者血清中的Ab和SC5b-9水平与可溶性免疫复合物没有定量相关性。还通过免疫组织化学在GBS患者的外周神经中检测到了膜结合的C5b-9。这些结果表明补体结合抗PNM Ab的水平与组织破坏性C5b-9复合物之间的关系,表明外周神经髓磷脂可能充当Ab介导的补体攻击的靶标。

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