Paparounas K, O'Hanlon G M, O'Leary C P, Rowan E G, Willison H J
University Department of Neurology, Institute of Neurological Sciences, Southern General Hospital, Glasgow, Scotland, UK.
Brain. 1999 May;122 ( Pt 5):807-16. doi: 10.1093/brain/122.5.807.
The neurophysiological effects of nine neuropathy-associated human anti-ganglioside antisera, three monoclonal antibodies to ganglioside GM1 (GM1) and of the cholera toxin B subunit (a GM1 ligand) were studied on mouse sciatic nerve in vitro. GM1 antisera and monoclonal antibodies from patients with chronic motor neuropathies and Guillain-Barre syndrome, and GQ1b/ disialosyl antisera and monoclonal antibodies from patients with chronic ataxic neuropathies and Miller Fisher syndrome were studied. In vitro recording, for up to 6 h, of compound nerve action potentials, latencies, rise times and stimulus thresholds from isolated desheathed sciatic nerve was performed in the presence of antiganglioside antibodies and fresh human serum as an additional source of complement. No changes were observed over this time course, with 4-6 h values for all electrophysiological parameters being within 15% of the starting values for both normal and antibody containing sera and for the cholera toxin B subunit. Parallel experiments on identically prepared desheathed nerves performed with 0.5 nM saxitoxin led to complete conduction block within 10 min of application. Under identical conditions to those used for electrophysiological recordings, quantitative immunohistological evaluation revealed a significant increase in IgM (immunoglobulin M) deposition at nodes of Ranvier from 5.3+/-3.1% to 28.7+/-8.4% (mean+/-SEM) of desheathed nerves exposed to three normal and three antibody containing sera, respectively (P < 0.03). Complement activation was seen at 100% of normal and 79% of disease-associated IgM positive nodes of Ranvier. These data indicate that anti-ganglioside antibodies can diffuse into a desheathed nerve, bind to nodes of Ranvier and fix complement in vitro without resulting in any overt physiological deterioration of the nerve over 4-6 h. This suggests that the node of Ranvier is relatively resistant to acute antiganglioside antibody mediated injury over this time scale and that anti-ganglioside antibodies and the cholera toxin B subunit are unlikely to have major direct pharmacological effects on nodal function, at least in comparison with the effect of saxitoxin. This in vitro sciatic nerve model appears of limited use for analysing electrophysiologically the effects of anti-ganglioside antibodies on nerve function, possibly because its short-term viability and isolation from circulating systemic factors do not permit the evolution of an inflammatory lesion of sufficient magnitude to induce overt electrophysiological abnormalities. In vivo models may be more suitable for identifying the effects of these antibodies on nerve conduction.
在体外对小鼠坐骨神经研究了九种与神经病相关的人抗神经节苷脂抗血清、三种针对神经节苷脂GM1(GM1)的单克隆抗体以及霍乱毒素B亚单位(一种GM1配体)的神经生理效应。研究了来自慢性运动神经病和格林-巴利综合征患者的GM1抗血清和单克隆抗体,以及来自慢性共济失调性神经病和米勒-费希尔综合征患者的GQ1b/二唾液酸抗血清和单克隆抗体。在抗神经节苷脂抗体和作为补体额外来源的新鲜人血清存在的情况下,对分离的去鞘坐骨神经的复合神经动作电位、潜伏期、上升时间和刺激阈值进行长达6小时的体外记录。在这段时间内未观察到变化,所有电生理参数在4 - 6小时时的值,对于正常血清和含抗体血清以及霍乱毒素B亚单位,均在起始值的15%以内。用0.5 nM石房蛤毒素对同样制备的去鞘神经进行的平行实验在应用后10分钟内导致完全传导阻滞。在与电生理记录相同的条件下,定量免疫组织学评估显示,暴露于三种正常血清和三种含抗体血清的去鞘神经中,郎飞结处IgM(免疫球蛋白M)沉积分别从5.3±3.1%显著增加到28.7±8.4%(平均值±标准误)(P < 0.03)。在100%的正常郎飞结和79%与疾病相关的IgM阳性郎飞结处可见补体激活。这些数据表明,抗神经节苷脂抗体可扩散进入去鞘神经,结合到郎飞结并在体外固定补体,而在4 - 6小时内不会导致神经出现任何明显的生理恶化。这表明在这个时间尺度上,郎飞结相对抵抗急性抗神经节苷脂抗体介导的损伤,并且抗神经节苷脂抗体和霍乱毒素B亚单位至少与石房蛤毒素的作用相比,不太可能对节点功能有主要的直接药理作用。这种体外坐骨神经模型在电生理分析抗神经节苷脂抗体对神经功能的影响方面似乎用途有限,可能是因为其短期存活能力以及与循环系统因素的隔离不允许发展出足够严重的炎症病变以诱导明显的电生理异常。体内模型可能更适合确定这些抗体对神经传导的影响。
