Role of inflammation in gastrointestinal tract in aetiology and pathogenesis of idiopathic parkinsonism

Clive Weller , Norman Oxlade , Sylvia M. Dobbs , R. John Dobbs , André Charlett , Ingvar T. Bjarnason
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引用次数: 56

Abstract

Idiopathic parkinsonism (IP) is a common disorder, conventionally regarded as neurodegenerative. Its cardinal features, poverty and slowness of movement, muscle rigidity, postural abnormality and a characteristic tremor, are associated with loss of dopaminergic neurones in the substantia nigra of the brain. Genetic factors explain only a minority of cases, and a common toxic environmental insult remains elusive. We propose that IP is a systemic disorder resulting from a ubiquitous peripheral infection, and that only the tip of the iceberg comes to diagnosis. There is evidence for inflammatory/immune activation peripherally and in the brain. We have used statistical modelling to explore links with non-specific and specific systemic markers of inflammation/infection in IP probands, and explore whether their partners and siblings have a frank or pre-presentation parkinsonian state. Critical to this approach is continuous objective measures of the facets of IP. Hypotheses on causality and mechanism are based on the statistical models. There is pathological and clinical evidence for direct involvement of the gastrointestinal tract in IP. The candidacy of Helicobacter pylori infection as a trigger event or driving infection is relatively high. We have found that eliminating infection in late parkinsonism with cachexia, a stage usually considered intractable, can result in a U-turn. However, eradication therapy may not provide a complete solution. Persistence of antibody against cytotoxin-associated antigen (CagA), increases the predicted probability of being labelled as having parkinsonism. Evidence for autoimmunity and immunocompromise is used to build schemes for the natural history. We conclude that current classifications of neuropsychiatric disease may not prove the best with respect to defining sub-clinical disease, prophylaxis or halting progression.

胃肠道炎症在特发性帕金森病病因和发病机制中的作用
特发性帕金森病(IP)是一种常见的疾病,通常被认为是神经退行性疾病。它的主要特征是运动迟缓、肌肉僵硬、姿势异常和特征性震颤,这些都与大脑黑质中多巴胺能神经元的丧失有关。遗传因素只能解释少数病例,而常见的有毒环境损害仍然难以捉摸。我们认为IP是一种由普遍存在的外周感染引起的全身性疾病,而且只有冰山一角被诊断出来。有证据表明外周和大脑中存在炎症/免疫激活。我们使用统计模型来探索IP先知者与非特异性和特异性全身炎症/感染标志物的联系,并探索他们的伴侣和兄弟姐妹是否有明显的或表现前的帕金森病状态。这种方法的关键在于持续客观地衡量知识产权的各个方面。关于因果关系和机制的假设是基于统计模型的。有病理和临床证据表明直接累及胃肠道的IP。幽门螺杆菌感染作为触发事件或驱动感染的可能性相对较高。我们发现,消除带有恶病质的晚期帕金森病的感染,通常被认为是难以治愈的阶段,可以导致病情的180度大转弯。然而,根除疗法可能不能提供一个完整的解决方案。抗细胞毒素相关抗原(CagA)抗体的持续存在,增加了被标记为患有帕金森病的预测概率。自身免疫和免疫损害的证据被用来建立自然历史的方案。我们的结论是,目前的神经精神疾病分类在定义亚临床疾病、预防或阻止进展方面可能不是最好的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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