Interplaying factors that effect multiple sclerosis causation and sustenance.

ISRN Neurology Pub Date : 2012-01-01 DOI:10.5402/2012/851541
Emanuel Calenoff
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引用次数: 8

Abstract

The author hypothesized that multiple sclerosis (MS) is a humoral autoimmune disease, caused by faulty interplay between myelin-specific, dimeric IgE, specifically competing non-IgE antibodies and IgE-triggered degranulating mast cells. The principal fault was believed to be insufficient quantity of protective, specific non-IgE antibodies. Also conjectured was the possibility of an unexpected and adverse immune suppression caused by none-MS pharmaceuticals being consumed by patients for their MS or for other conditions. To test both hypotheses, a mimotopic, peptide antigen-based, serum immunoassay was developed to measure dimer-bound IgE excess among MS patients, wherein the IgE specifically complexes with two or more myelin surface epitopes at an interval of 40-100 Angstroms, a separation critical for mast cell degranulation and cell damaging effect. MS test sensitivity and specificity, when analyzing five previously untreated patients for dimeric IgE presence, was 100%. In direct comparison, twenty age- and gender-matched female and male control subjects were test negative. Analysis of 35 multiple sclerosis patients, who were concomitantly being treated with potentially immunosuppressive pharmaceuticals, appeared to show the substances' negative effect upon MS causation, progression, or specific immunoassay performance. Therefore, MS is likely an autoimmune disease caused by IgE-mediated mast cell degranulation possibly in conjunction with immunosuppressive agents.

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影响多发性硬化症病因和维持的相互作用因素。
作者假设多发性硬化症(MS)是一种体液性自身免疫性疾病,由髓磷脂特异性二聚体IgE、特异性竞争的非IgE抗体和IgE触发的脱颗粒肥大细胞之间的错误相互作用引起。主要的缺陷被认为是保护性的特异性非ige抗体数量不足。还推测,由于患者因多发性硬化症或其他疾病而服用非多发性硬化症药物,可能会导致意想不到的不良免疫抑制。为了验证这两种假设,研究人员开发了一种基于肽抗原的血清免疫分析法来测量多发性硬化患者中二聚体结合的IgE过量,其中IgE特异性地以40-100埃的间隔与两个或多个髓鞘表面表位复合物,这是肥大细胞脱颗粒和细胞损伤作用的关键分离。MS试验的敏感性和特异性,在分析五名未接受治疗的二聚体IgE存在的患者时,为100%。在直接比较中,20名年龄和性别匹配的女性和男性对照者检测为阴性。对35名同时接受潜在免疫抑制药物治疗的多发性硬化症患者的分析,似乎显示了这些物质对多发性硬化症的病因、进展或特异性免疫测定性能的负面影响。因此,MS可能是一种由ige介导的肥大细胞脱颗粒可能与免疫抑制剂联合引起的自身免疫性疾病。
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