首页> 外文期刊>European journal of neurology: the official journal of the European Federation of Neurological Societies >Persistent mucosal damage and risk of epilepsy in people with celiac disease
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Persistent mucosal damage and risk of epilepsy in people with celiac disease

机译:患有乳糜泻患者的持续粘膜损伤和癫痫风险

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Background and purpose Celiac disease (CD) is associated with an increased risk of developing epilepsy, a risk that persists after CD diagnosis. A significant proportion of patients with CD have persistent villous atrophy (VA) on follow‐up biopsy. The objective of this study was to determine whether persistent VA on follow‐up biopsy affected long‐term epilepsy risk and epilepsy‐related hospital emergency admissions. Methods This was a nationwide cohort study. We identified all people in Sweden with histological evidence of CD who underwent a follow‐up small intestinal biopsy (1969–2008). We compared those with persistent VA with those who showed histological improvement, assessing the development of epilepsy and related emergency hospital admissions (defined according to relevant International Classification of Diseases codes in the Swedish Patient Register). Cox regression analysis was used to assess outcome measures. Results Villous atrophy was present in 43% of 7590 people with CD who had a follow‐up biopsy. The presence of persistent VA was significantly associated with a reduced risk of developing newly‐diagnosed epilepsy (hazard ratio, 0.61; 95% confidence interval, 0.38–0.98). On stratified analysis, this effect was primarily amongst males (hazard ratio, 0.35; 95% confidence interval, 0.15–0.80). Among the 58 patients with CD with a prior diagnosis of epilepsy, those with persistent VA were less likely to visit an emergency department with epilepsy (hazard ratio, 0.37; 95% confidence interval, 0.09–1.09). Conclusions In a population‐based study of individuals with CD, persisting VA on follow‐up biopsy was associated with reduced future risk of developing epilepsy but did not influence emergency epilepsy‐related hospital admissions. The mechanism as to why persistent VA confers this benefit requires further exploration.
机译:背景论和目的腹腔疾病(CD)与发育癫痫的风险增加有关,这种风险持续存在于CD诊断后。大部分CD患者在随访活组织检查中具有持续的绒毛萎缩(VA)。本研究的目的是确定持续的VA是否对随访活组织检查影响受到长期癫痫风险和癫痫相关的医院应急录取。方法这是全国范围的队列研究。我们鉴定了瑞典的所有人,其中包含CD的组织学证据,他们接受了后续小肠活检(1969-2008)。我们将那些持久的VA与那些表现出组织学改进的人进行比较,评估癫痫和相关的急诊医院招生的发展(根据瑞典患者登记册的相关国际疾病规范分类定义)。 COX回归分析用于评估结果措施。结果绒毛萎缩以7590名患有后续活检的CD占7590人的43%。持续性VA的存在显着与开发新诊断的癫痫(危险比,0.61; 95%置信区间,0.38-0.98)的风险显着相关。在分层分析上,这种效果主要是雄性(危险比,0.35; 95%置信区间,0.15-0.80)。在58例CD患者中,患有癫痫的癫痫患者,VA持久性的人不太可能访问癫痫(危险比,0.37; 95%置信区间,0.09-1.09)。结论在患有CD的个体的基于人群的研究中,持续存在于随访活组织检查的VA与减少未来发育癫痫的风险降低,但没有影响紧急癫痫相关的医院录取。为什么持久性VA赋予这种福利的机制需要进一步的探索。

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