Nenci Arianna, Becker Christoph, Wullaert Andy, Gareus Ralph, van Loo Geert, Danese Silvio, Huth Marion, Nikolaev Alexei, Neufert Clemens, Madison Blair, Gumucio Deborah, Neurath Markus F, Pasparakis Manolis
Institute for Genetics, University of Cologne, Zülpicher Strasse 47, 50674 Cologne, Germany.
Nature. 2007 Mar 29;446(7135):557-61. doi: 10.1038/nature05698. Epub 2007 Mar 14.
Deregulation of intestinal immune responses seems to have a principal function in the pathogenesis of inflammatory bowel disease. The gut epithelium is critically involved in the maintenance of intestinal immune homeostasis-acting as a physical barrier separating luminal bacteria and immune cells, and also expressing antimicrobial peptides. However, the molecular mechanisms that control this function of gut epithelial cells are poorly understood. Here we show that the transcription factor NF-kappaB, a master regulator of pro-inflammatory responses, functions in gut epithelial cells to control epithelial integrity and the interaction between the mucosal immune system and gut microflora. Intestinal epithelial-cell-specific inhibition of NF-kappaB through conditional ablation of NEMO (also called IkappaB kinase-gamma (IKKgamma)) or both IKK1 (IKKalpha) and IKK2 (IKKbeta)-IKK subunits essential for NF-kappaB activation-spontaneously caused severe chronic intestinal inflammation in mice. NF-kappaB deficiency led to apoptosis of colonic epithelial cells, impaired expression of antimicrobial peptides and translocation of bacteria into the mucosa. Concurrently, this epithelial defect triggered a chronic inflammatory response in the colon, initially dominated by innate immune cells but later also involving T lymphocytes. Deficiency of the gene encoding the adaptor protein MyD88 prevented the development of intestinal inflammation, demonstrating that Toll-like receptor activation by intestinal bacteria is essential for disease pathogenesis in this mouse model. Furthermore, NEMO deficiency sensitized epithelial cells to tumour-necrosis factor (TNF)-induced apoptosis, whereas TNF receptor-1 inactivation inhibited intestinal inflammation, demonstrating that TNF receptor-1 signalling is crucial for disease induction. These findings demonstrate that a primary NF-kappaB signalling defect in intestinal epithelial cells disrupts immune homeostasis in the gastrointestinal tract, causing an inflammatory-bowel-disease-like phenotype. Our results identify NF-kappaB signalling in the gut epithelium as a critical regulator of epithelial integrity and intestinal immune homeostasis, and have important implications for understanding the mechanisms controlling the pathogenesis of human inflammatory bowel disease.
肠道免疫反应失调似乎在炎症性肠病的发病机制中起主要作用。肠道上皮细胞在维持肠道免疫稳态中起着关键作用——作为分隔肠腔细菌和免疫细胞的物理屏障,并表达抗菌肽。然而,控制肠道上皮细胞这一功能的分子机制仍知之甚少。在此,我们表明转录因子NF-κB作为促炎反应的主要调节因子,在肠道上皮细胞中发挥作用,以控制上皮完整性以及黏膜免疫系统与肠道微生物群之间的相互作用。通过条件性敲除NEMO(也称为IkappaB激酶-γ(IKKγ))或IKK1(IKKα)和IKK2(IKKβ)这两个对NF-κB激活至关重要的IKK亚基,在肠道上皮细胞中特异性抑制NF-κB会自发地在小鼠中引发严重的慢性肠道炎症。NF-κB缺乏导致结肠上皮细胞凋亡、抗菌肽表达受损以及细菌向黏膜的移位。同时,这种上皮缺陷引发了结肠中的慢性炎症反应,最初由先天免疫细胞主导,但后来也涉及T淋巴细胞。编码衔接蛋白MyD88的基因缺乏可阻止肠道炎症的发展,表明肠道细菌激活Toll样受体对于该小鼠模型中的疾病发病机制至关重要。此外,NEMO缺乏使上皮细胞对肿瘤坏死因子(TNF)诱导的凋亡敏感,而TNF受体-1失活抑制肠道炎症,表明TNF受体-1信号传导对于疾病诱导至关重要。这些发现表明肠道上皮细胞中的原发性NF-κB信号缺陷会破坏胃肠道中的免疫稳态,导致类似炎症性肠病的表型。我们的结果确定肠道上皮中的NF-κB信号传导是上皮完整性和肠道免疫稳态的关键调节因子,对理解控制人类炎症性肠病发病机制具有重要意义。
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