Ganglioside as a neurotrophic drug has been hitherto widely used in China, although Guillain-Barré syndrome (GBS) following intravenous ganglioside treatment was reported in Europe several decades ago. We identified 7 patients who developed GBS after intravenous use of gangliosides (ganglioside+ group) and compared their clinical data with those of 77 non-ganglioside-associated GBS patients (ganglioside− group) in 2013, aiming at gaining the distinct features of ganglioside-associated GBS. Although the mean age, protein levels in cerebrospinal fluid (CSF) and frequency of cranial nerve involvement were similar between the two groups, the Hughes Functional Grading Scale (HFGS) score and the Medical Research Council (MRC) sum score at nadir significantly differed (4.9±0.4 vs 3.6±1.0; 7.7±5.5 vs 36.9±14.5, both p<0.001), indicating a higher disease severity of ganglioside-associated GBS. A higher ratio of patients with ganglioside-associated GBS required mechanical ventilation (85.7% vs 15.6%, p<0.01). The short-term prognosis of ganglioside-associated GBS, as measured by the HFGS score and the MRC sum score at discharge, was poorer (4.3±0.5 vs 2.8±1.1; 17.3±12.9 vs 46.0±13.9, both p<0.001). All the patients in the ganglioside+ group presented an axonal form of GBS, namely acute motor axonal neuropathy (AMAN). When compared with the AMAN patients in the ganglioside− group, more severe functional deficits at nadir and poorer recovery after standard treatment were still prominent in ganglioside-associated GBS. Anti-GM1 and anti-GT1a antibodies were detectable in patients with AMAN while not in patients with the demyelinating subtype of GBS. The concentrations of these antibodies in patients with AMAN were insignificantly different between the ganglioside+ and ganglioside− groups. In sum, ganglioside-associated GBS may be a devastating side effect of intravenous use of gangliosides, which usually manifests a more severe clinical course and poorer outcome.
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机译:尽管几十年前在欧洲已经报道了静脉注射神经节苷脂治疗后的格林-巴利综合征(GBS),但迄今为止,神经节苷脂作为一种神经营养药物已在中国广泛使用。我们确定了7位静脉注射神经节苷脂后发生GBS的患者(神经节苷脂+组),并将他们的临床资料与2013年77例非神经节苷脂相关的GBS患者(神经节苷脂-组)进行了比较,旨在了解神经节苷脂相关的独特特征GBS。尽管两组的平均年龄,脑脊液(CSF)的蛋白质水平和颅神经受累的频率相似,但休斯功能分级量表(HFGS)得分和医学研究理事会(MRC)总得分最低点明显不同( 4.9±0.4 vs 3.6±1.0; 7.7±5.5 vs 36.9±14.5,均p <0.001),表明神经节苷脂相关GBS的疾病严重程度更高。神经节苷脂相关的GBS患者需要机械通气的比例更高(85.7%对15.6%,p <0.01)。神经节苷脂相关GBS的短期预后较差,通过HFGS评分和MRC总评分在出院时较差(4.3±0.5 vs 2.8±1.1; 17.3±12.9 vs 46.0±13.9,均p <0.001)。神经节苷脂+组中的所有患者均表现为轴突形式的GBS,即急性运动轴突神经病(AMAN)。与神经节苷脂组的AMAN患者相比,在与神经节苷脂相关的GBS中,最低点的严重功能缺陷和标准治疗后恢复较差仍然很明显。在AMAN患者中可检测到抗GM1和抗GT1a抗体,而在GBS脱髓鞘亚型患者中则未检测到。在AMAN患者中,这些抗体的浓度在神经节苷脂+和神经节苷脂-组之间无显着差异。总之,与神经节苷脂相关的GBS可能是静脉内使用神经节苷脂的毁灭性副作用,通常表现出更为严重的临床病程和较差的预后。
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