气道上皮细胞核因子-κB活性的不同功能调节二氧化氮诱导的急性肺损伤。
Distinct functions of airway epithelial nuclear factor-kappaB activity regulate nitrogen dioxide-induced acute lung injury.
作者信息
Ather Jennifer L, Alcorn John F, Brown Amy L, Guala Amy S, Suratt Benjamin T, Janssen-Heininger Yvonne M W, Poynter Matthew E
机构信息
Department of Pathology, University of Vermont, Burlington, VT 05405, USA.
出版信息
Am J Respir Cell Mol Biol. 2010 Oct;43(4):443-51. doi: 10.1165/rcmb.2008-0416OC. Epub 2009 Nov 9.
Reactive oxidants such as nitrogen dioxide (NO(2)) injure the pulmonary epithelium, causing airway damage and inflammation. We previously demonstrated that nuclear factor-κ B (NF-κB) activation within airway epithelial cells occurs in response to NO(2) inhalation, and is critical for lipopolysaccharide-induced or antigen-induced inflammatory responses. Here, we investigated whether manipulation of NF-κB activity in lung epithelium affected severe lung injuries induced by NO(2) inhalation. Wild-type C57BL/6J, CC10-IκBα(SR) transgenic mice with repressed airway epithelial NF-κB function, or transgenic mice expressing a doxycycline-inducible, constitutively active I κ B kinase β (CC10-rTet-(CA)IKKβ) with augmented NF-κB function in airway epithelium, were exposed to toxic levels of 25 ppm or 50 ppm NO(2) for 6 hours a day for 1 or 3 days. In wild-type mice, NO(2) caused the activation of NF-κB in airway epithelium after 6 hours, and after 3 days resulted in severe acute lung injury, characterized by neutrophilia, peribronchiolar lesions, and increased protein, lactate dehydrogenase, and inflammatory cytokines. Compared with wild-type mice, neutrophilic inflammation and elastase activity, lung injury, and several proinflammatory cytokines were significantly suppressed in CC10-IκBα(SR) mice exposed to 25 or 50 ppm NO(2). Paradoxically, CC10-rTet-(CA)IKKβ mice that received doxycycline showed no further increase in NO(2)-induced lung injury compared with wild-type mice exposed to NO(2), instead displaying significant reductions in histologic parameters of lung injury, despite elevations in several proinflammatory cytokines. These intriguing findings demonstrate distinct functions of airway epithelial NF-κB activities in oxidant-induced severe acute lung injury, and suggest that although airway epithelial NF-κB activities modulate NO(2)-induced pulmonary inflammation, additional NF-κB-regulated functions confer partial protection from lung injury.
诸如二氧化氮(NO₂)等反应性氧化剂会损伤肺上皮细胞,导致气道损伤和炎症。我们之前证明,气道上皮细胞内的核因子κB(NF-κB)激活是对吸入NO₂的反应,并且对于脂多糖诱导或抗原诱导的炎症反应至关重要。在此,我们研究了肺上皮细胞中NF-κB活性的调控是否会影响由吸入NO₂引起的严重肺损伤。野生型C57BL/6J小鼠、气道上皮NF-κB功能受抑制的CC10-IκBα(SR)转基因小鼠,或在气道上皮中NF-κB功能增强、表达强力霉素诱导的组成型活性IκB激酶β(CC10-rTet-(CA)IKKβ)的转基因小鼠,每天暴露于25 ppm或50 ppm的有毒水平NO₂中6小时,持续1天或3天。在野生型小鼠中,NO₂在6小时后导致气道上皮中NF-κB激活,3天后导致严重的急性肺损伤,其特征为中性粒细胞增多、细支气管周围病变以及蛋白质、乳酸脱氢酶和炎性细胞因子增加。与野生型小鼠相比,暴露于25或50 ppm NO₂的CC10-IκBα(SR)小鼠的中性粒细胞炎症和弹性蛋白酶活性、肺损伤以及几种促炎细胞因子均显著受到抑制。矛盾的是,与暴露于NO₂的野生型小鼠相比,接受强力霉素的CC10-rTet-(CA)IKKβ小鼠在NO₂诱导的肺损伤方面没有进一步增加,尽管几种促炎细胞因子有所升高,但肺损伤的组织学参数却显著降低。这些有趣的发现证明了气道上皮NF-κB活性在氧化剂诱导的严重急性肺损伤中的不同功能,并表明尽管气道上皮NF-κB活性调节NO₂诱导的肺部炎症,但NF-κB调节的其他功能可提供部分肺损伤保护。
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