Jeyaseelan Samithamby, Young Scott K, Fessler Michael B, Liu Yuhong, Malcolm Kenneth C, Yamamoto Masahiro, Akira Shizuo, Worthen G Scott
Division of Respiratory Infections, Department of Medicine, National Jewish Medical and Research Center, 1400 Jackson Street Neustadt D-403, Denver, CO 80206, USA.
J Immunol. 2007 Mar 1;178(5):3153-60. doi: 10.4049/jimmunol.178.5.3153.
Bacterial pneumonia remains a serious disease and is associated with neutrophil recruitment. Innate immunity is pivotal for the elimination of bacteria, and TLRs are essential in this process. Toll/IL-1R domain-containing adaptor inducing IFN-beta (TRIF) is an adaptor for TLR3 and TLR4, and is associated with the MyD88-independent cascade. However, the importance of TRIF in immune responses against pulmonary bacterial pathogens is not well understood. We investigated the involvement of TRIF in a murine model of Escherichia coli pneumonia. TRIF(-/-) mice infected with E. coli display attenuated neutrophil migration; NF-kappaB activation; and TNF-alpha, IL-6, and LPS-induced C-X-C chemokine production in the lungs. In addition, E. coli-induced phosphorylation of JNK, ERK, and p38 MAPK was detected in bone marrow-derived macrophages (BMMs) of TRIF(+/+) mice, but attenuated in BMMs of TRIF(-/-) mice. Furthermore, E. coli-induced TNF-alpha and IL-6 production was attenuated in BMMs of TRIF(-/-) mice. E. coli LPS-induced late MAPK activation, and TNF-alpha and IL-6 production were abolished in BMMs of TRIF(-/-) mice. Moreover, TRIF is not required for LPS-induced neutrophil influx, and keratinocyte cell-derived chemokine, MIP-2, and LPS-induced C-X-C chemokine production in the lungs. Using TLR3(-/-) mice, we ruled out the role of TLR3-mediated TRIF-dependent neutrophil influx during E. coli pneumonia. A TLR4-blocking Ab inhibited E. coli-induced TNF-alpha and IL-6 in BMMs of both TRIF(-/-) and TRIF(+/+) mice, suggesting that TRIF-mediated signaling involves TLR4. We also found that TRIF is critical to control E. coli burden in the lungs and E. coli dissemination. Thus, rapid activation of TRIF-dependent TLR4-mediated signaling cascade serves to augment pulmonary host defense against a Gram-negative pathogen.
细菌性肺炎仍然是一种严重的疾病,与中性粒细胞募集有关。固有免疫对于清除细菌至关重要,而Toll样受体(TLRs)在此过程中必不可少。含Toll/白细胞介素-1受体结构域的接头蛋白诱导干扰素-β(TRIF)是TLR3和TLR4的接头蛋白,与不依赖髓样分化因子88(MyD88)的级联反应相关。然而,TRIF在针对肺部细菌病原体的免疫反应中的重要性尚未得到充分了解。我们研究了TRIF在大肠杆菌肺炎小鼠模型中的作用。感染大肠杆菌的TRIF基因敲除(TRIF(-/-))小鼠表现出中性粒细胞迁移减弱、核因子κB(NF-κB)激活减弱以及肺中肿瘤坏死因子-α(TNF-α)、白细胞介素-6(IL-6)和脂多糖(LPS)诱导的CXC趋化因子产生减少。此外,在TRIF基因野生型(TRIF(+/+))小鼠的骨髓来源巨噬细胞(BMMs)中检测到大肠杆菌诱导的应激活化蛋白激酶(JNK)、细胞外信号调节激酶(ERK)和p38丝裂原活化蛋白激酶(MAPK)磷酸化,但在TRIF(-/-)小鼠的BMMs中减弱。此外,TRIF(-/-)小鼠的BMMs中大肠杆菌诱导的TNF-α和IL-6产生减弱。TRIF(-/-)小鼠的BMMs中大肠杆菌LPS诱导的晚期MAPK激活以及TNF-α和IL-6产生被消除。此外,LPS诱导的中性粒细胞流入、角质形成细胞衍生趋化因子、巨噬细胞炎性蛋白-2(MIP-2)以及肺中LPS诱导的CXC趋化因子产生并不需要TRIF。使用TLR3基因敲除(TLR3(-/-))小鼠,我们排除了TLR3介导的TRIF依赖性中性粒细胞流入在大肠杆菌肺炎中的作用。一种TLR4阻断抗体抑制了TRIF(-/-)和TRIF(+/+)小鼠的BMMs中大肠杆菌诱导的TNF-α和IL-6,这表明TRIF介导的信号传导涉及TLR4。我们还发现TRIF对于控制肺中的大肠杆菌负荷和大肠杆菌播散至关重要。因此,TRIF依赖性TLR4介导的信号级联反应的快速激活有助于增强肺部对革兰氏阴性病原体的宿主防御。
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