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Crohn’s Disease Patients in Remission Display an Enhanced Intestinal IgM+ B Cell Count in Concert with a Strong Activation of the Intestinal Complement System

机译:克罗恩病缓解期患者显示肠道IgM + B细胞计数增加同时肠道补体系统强烈激活

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摘要

Inflammatory bowel disease (IBD) is an umbrella term that comprises Crohn’s disease (CD) and ulcerative colitis (UC). Both entities are characterized by a disturbed mucosal immune response and an imbalance of intestinal microbiota composition. The complement system (C) plays a critical role in the detection, and clearance of bacteria and dysregulation of single complement components has been linked to IBD. Here, we asked if the C contributes to distinct subtypes of inflammation observed in CD and UC. We performed systematical expression analyses of the intestinal C in IBD patients and controls. Immunohistochemistry or immunoblot experiments were performed to verify qPCR data. Activity of the three activation pathways of C was studied in sera samples. In CD patients a strong upregulation of the C was observed enabling the definition of unique expression patterns being associated either with remission or active disease. These data were reflected by an enhanced C activation in sera and fecal samples. An excessive mucosal presence of immunoglobulin M (IgM) and CR2/CD21 positive B cells in concert with decreased fecal IgA level was identified in CD patients in remission. These findings point to an exacerbated induction of the intestinal C that may potentially be involved in the etiology of CD.
机译:炎性肠病(IBD)是一个笼统的术语,包含克罗恩氏病(CD)和溃疡性结肠炎(UC)。这两个实体的特征都在于粘膜免疫反应紊乱和肠道菌群组成失衡。补体系统(C)在检测中起关键作用,细菌清除和单个补体成分失调与IBD有关。在这里,我们问C是否有助于CD和UC中观察到的不同炎症亚型。我们对IBD患者和对照的肠道C进行了系统表达分析。进行了免疫组织化学或免疫印迹实验以验证qPCR数据。在血清样品中研究了C的三个激活途径的活性。在CD患者中,观察到C的强烈上调,从而可以定义与缓解或活动性疾病相关的独特表达模式。这些数据通过血清和粪便样品中增强的C活化来反映。在缓解的CD患者中,发现粘膜中存在过多的免疫球蛋白M(IgM)和CR2 / CD21阳性B细胞,以及粪便IgA水平降低。这些发现表明,肠道C的加剧可能与CD的病因有关。

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