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Apocynin and ebselen reduce influenza A virus-induced lung inflammation in cigarette smoke-exposed mice

机译:apocynin和ebselen减少暴露于香烟烟雾的小鼠中甲型流感病毒引起的肺部炎症

摘要

Influenza A virus (IAV) infections are a common cause of acute exacerbations of chronic obstructive pulmonary disease (AECOPD). Oxidative stress is increased in COPD, IAV-induced lung inflammation and AECOPD. Therefore, we investigated whether targeting oxidative stress with the Nox2 oxidase inhibitors and ROS scavengers, apocynin and ebselen could ameliorate lung inflammation in a mouse model of AECOPD. Male BALB/c mice were exposed to cigarette smoke (CS) generated from 9 cigarettes per day for 4 days. On day 5, mice were infected with 1 × 104.5 PFUs of the IAV Mem71 (H3N1). BALF inflammation, viral titers, superoxide production and whole lung cytokine, chemokine and protease mRNA expression were assessed 3 and 7 days post infection. IAV infection resulted in a greater increase in BALF inflammation in mice that had been exposed to CS compared to non-smoking mice. This increase in BALF inflammation in CS-exposed mice caused by IAV infection was associated with elevated gene expression of pro-inflammatory cytokines, chemokines and proteases, compared to CS alone mice. Apocynin and ebselen significantly reduced the exacerbated BALF inflammation and pro-inflammatory cytokine, chemokine and protease expression caused by IAV infection in CS mice. Targeting oxidative stress using apocynin and ebselen reduces IAV-induced lung inflammation in CS-exposed mice and may be therapeutically exploited to alleviate AECOPD.
机译:甲型流感病毒(IAV)感染是慢性阻塞性肺疾病(AECOPD)急性加重的常见原因。 COPD,IAV引起的肺部炎症和AECOPD中的氧化应激增加。因此,我们研究了用Nox2氧化酶抑制剂和ROS清道夫,载脂蛋白和依布硒啉靶向氧化应激能否改善AECOPD小鼠模型的肺部炎症。将雄性BALB / c小鼠暴露于每天9支香烟产生的香烟烟雾(CS)中,持续4天。在第5天,小鼠感染了1×104.5 PFU的IAV Mem71(H3N1)。感染后3天和7天,评估BALF炎症,病毒滴度,超氧化物产生以及全肺细胞因子,趋化因子和蛋白酶mRNA表达。与不吸烟的小鼠相比,IAV感染导致接触CS的小鼠的BALF炎症增加更大。与单独CS小鼠相比,IAV感染引起的CS暴露小鼠中BALF炎症的这种增加与促炎细胞因子,趋化因子和蛋白酶的基因表达升高有关。 Apocynin和ebselen显着减轻了CS小鼠中IAV感染引起的加重的BALF炎症以及促炎性细胞因子,趋化因子和蛋白酶的表达。使用载脂蛋白和依布硒啉靶向氧化应激可减少CS暴露小鼠中IAV诱导的肺部炎症,可用于治疗以减轻AECOPD。

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