Properdin deficiency protects from 5‐fluorouracil‐induced small intestinal mucositis in a complement activation‐independent, interleukin‐10‐dependent mechanism

Umang Jain, Craig Midgen, Trent M. Woodruff, Wilhelm J. Schwaeble, C. Stover, Andrew W. Stadnyk
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引用次数: 12

Abstract

Intestinal mucositis is a serious complication of chemotherapy that leads to significant morbidity that may require dose or drug adjustments. Specific mitigating strategies for mucositis are unavailable, due partly to an incomplete understanding of the pathogenic mechanisms. We have previously shown an effect of properdin, a positive regulator of complement activation, in models of colitis. Here we use properdin‐deficient (PKO) mice to interrogate the role of properdin and complement in small intestinal mucositis. Mucositis was induced by five daily injections of 5‐fluorouracil (5‐FU) in wild‐type (WT), PKO, interleukin (IL)‐10–/– and properdin/IL‐10–/– double knock‐out (DKO) mice. At the time of euthanasia their jejunum was collected for histology, immunohistochemistry and cytokine and complement activation measurements. Complement became activated in mice receiving 5‐FU, indicated by increased intestinal levels of C3a and C5a. Compared to WT, PKO mice experienced significantly less mucositis, despite C3a levels as high as inflamed WT mice and slightly less C5a. Conversely, PKO mice had higher intestinal levels of IL‐10. IL‐10 expression was mainly by epithelial cells in both uninflamed and inflamed PKO mice. IL‐10–/– mice proved to be highly susceptible to mucositis and DKO mice were equally susceptible, demonstrating that a lack of properdin does not protect mice lacking IL‐10. We interpret our findings to indicate that, to a significant extent, the inflammation of mucositis is properdin‐dependent but complement activation‐independent. Additionally, the benefit achieved in the absence of properdin is associated with increased IL‐10 levels, and IL‐10 is important in limiting mucositis.
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Properdin缺乏通过补体激活独立、白细胞介素- 10依赖机制保护5 -氟尿嘧啶诱导的小肠黏膜炎
肠黏膜炎是化疗的严重并发症,可导致严重的发病率,可能需要调整剂量或药物。由于对致病机制的不完全了解,目前尚无针对粘膜炎的具体缓解策略。我们之前已经在结肠炎模型中显示了补体激活的正调节因子properdin的作用。在这里,我们使用properdin‐deficient (PKO)小鼠来研究properdin和补体在小肠黏膜炎中的作用。在野生型(WT)、PKO、白介素(IL)‐10 - / -和properdin/IL‐10 - / -双敲除(DKO)小鼠中,每日5次注射5‐氟尿嘧啶(5‐FU)诱导粘膜炎。在安乐死时收集它们的空肠进行组织学,免疫组织化学和细胞因子和补体活化测定。补体在接受5‐FU的小鼠中被激活,表明肠道中C3a和C5a水平升高。与WT相比,PKO小鼠的粘膜炎明显减少,尽管C3a水平与炎症WT小鼠一样高,C5a略低。相反,PKO小鼠的肠道IL - 10水平较高。IL - 10在未发炎和发炎的PKO小鼠中主要通过上皮细胞表达。IL - 10 - / -小鼠被证明对粘膜炎高度敏感,DKO小鼠也同样敏感,这表明缺乏properdin并不能保护缺乏IL - 10的小鼠。我们解释我们的研究结果表明,在很大程度上,粘膜炎的炎症是适当依赖于补体激活的,而不是补体激活的。此外,在没有properdin的情况下获得的益处与IL - 10水平的增加有关,IL - 10在限制粘膜炎方面很重要。
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