P193 患有炎症性肠病的疲劳患者表现出不同的全身抗体表位汇集

M. G. Griesbaum, T. Vogl, S. Andreu-Sánchez, S. Klompus, I. N. Kalka, S. Leviatan, H. V. van Dullemen, M. Visschedijk, E. Festen, K. N. Faber, G. Dijkstra, A. Weinberger, E. Segal, R. Weersma, A. R. Bourgonje
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引用次数: 0

摘要

炎症性肠病(IBD)患者经常会感到疲劳,高达 80% 的活动期患者和大约 50% 的静止期患者会感到疲劳。IBD 相关性疲劳的确切病因往往不明,这使得临床治疗非常具有挑战性。在这项研究中,我们旨在探讨静止期 IBD 患者是否会出现特异性全身抗体反应,这将有助于深入了解疲劳背后的免疫反应。 我们利用噬菌体展示免疫沉淀测序(PhIP-Seq)技术,针对 344,000 个合理选择的多肽抗原,对 327 例 IBD 患者(156 例克罗恩病 [CD];171 例溃疡性结肠炎 [UC])的全身抗体表位谱进行了分析。疲劳严重程度采用 10 分李克特量表进行评估,从 1 分(无疲劳感)到 10 分(疲劳严重程度最高)不等。IBD静止期的定义为取样时的临床(哈维-布拉德肖指数[HBI]<5或简单临床结肠炎活动指数[SCCAI]<2.5)和生化缓解(C反应蛋白[CRP]<5 mg/L)。在对年龄、性别和吸烟等潜在混杂因素进行调整后,进行了多变量逻辑回归分析,以确定疲劳与全身抗体反应之间的关联。 共有105种不同的抗体结合肽与疲劳有关(标称P值<0.05),尽管没有一种抗体通过了多重比较调整。在这些抗体中,有 50 种(47.6%)在高度疲劳患者(第四四分位数,Q4)中出现频率较低,而有 55 种(52.4%)在高度疲劳患者中出现频率高于低度疲劳患者(第一四分位数,Q1)。在高度疲劳患者中,抗体反应主要针对病毒抗原,尤其是爱泼斯坦-巴氏病毒(EBV)的几种抗原,以及细菌抗原,包括链球菌和葡萄球菌的功能蛋白。疲劳的 CD 患者对过敏原、葡萄球菌、绿脓杆菌和志贺氏杆菌的全身抗体反应较高。疲劳的 UC 患者对单纯疱疹病毒(HSV)和流感病毒的抗体反应频率较高,而对过敏原和链球菌的反应较低。在对静止期 IBD 患者进行重复分析时,这些结果基本保持不变。 这项研究可能表明,病毒抗原(尤其是 EBV)在 IBD 患者疲劳的病理生理学中可能发挥作用。不过,还需要更大规模的确证研究来验证这些发现。PhIP-Seq可能是研究疲劳等复杂症状背后的免疫反应的一种有价值的策略。
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P193 Fatigued patients with Inflammatory Bowel Disease exhibit distinct systemic antibody epitope repertoires
Patients with inflammatory bowel diseases (IBD) frequently experience fatigue, affecting up to 80% of those with active disease and approximately 50% with quiescent disease. The exact cause of IBD-associated fatigue is often unknown, making clinical management very challenging. In this study we aimed to explore whether patients with quiescent IBD reporting fatigue exhibit specific systemic antibody responses, which could provide insight into immune reactivities underlying fatigue. Systemic antibody epitope repertoires were profiled in 327 patients with IBD (156 Crohn’s disease [CD]; 171 ulcerative colitis [UC]) leveraging phage-display immunoprecipitation sequencing (PhIP-Seq) against 344,000 rationally selected peptide antigens. Fatigue severity was assessed on a 10-point Likert scale, ranging from 1 (no fatigue) to 10 (highest fatigue severity). Quiescent IBD was defined as clinical (Harvey-Bradshaw Index [HBI] <5 or Simple Clinical Colitis Activity Index [SCCAI] <2.5) and biochemical remission (C-reactive protein [CRP] <5 mg/L) at time of sampling. Multivariable logistic regression analyses, allowing adjustment for potential confounding factors e.g. age, sex, and smoking, were performed to identify associations between fatigue and systemic antibody responses. A total of 105 different antibody-bound peptides were associated with fatigue (nominal P-value<0.05), albeit none passed adjustment for multiple comparisons. Among these antibodies, 50 (47.6%) were found to be less frequent in highly fatigued patients (fourth quartile, Q4), while 55 (52.4%) were identified as more frequent in highly fatigued patients compared to those with low fatigue scores (first quartile, Q1). Among highly fatigued patients, antibody responses were primarily directed towards viral antigens, notably several antigens from Epstein-Barr virus (EBV), as well as bacterial antigens, including functional proteins from Streptococcus and Staphylococcus species. Fatigued patients with CD exhibited elevated systemic antibody responses against allergens, Staphylococcus, Pseudomonas aeruginosa, and Shigella spp. Fatigued patients with UC showed higher frequencies of antibody responses against herpes simplex virus (HSV), influenza viruses, and few responses against allergens and Streptococcus bacteria. These results remained materially unchanged when repeating analyses in patients with quiescent IBD. This study may suggest a potential role of viral antigens, particularly EBV, in the pathophysiology of fatigue in patients with IBD. However, larger confirmatory studies are needed to validate these findings. PhIP-Seq may represent a valuable strategy to approach the investigation of immune responses underlying complex symptoms such as fatigue.
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