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Allergic inflammation alters the lung microbiome and hinders synergistic co-infection with H1N1 influenza virus and Streptococcus pneumoniae in C57BL/6 mice

机译:过敏性炎症改变了肺部微生物组,在C57BL / 6小鼠中患有H1N1流感病毒和链球菌肺炎的肺癌和阻碍协同感染

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Asthma is a chronic airways condition that can be exacerbated during respiratory infections. Our previous work, together with epidemiologic findings that asthmatics were less likely to suffer from severe influenza during the 2009 pandemic, suggest that additional complications of influenza such as increased susceptibility to bacterial superinfection, may be mitigated in allergic hosts. To test this hypothesis, we developed a murine model of 'triple-disease' in which mice rendered allergic to Aspergillus fumigatus were co-infected with influenza A virus and Streptococcus pneumoniae seven days apart. Significant alterations to known synergistic effects of co-infection were noted in the allergic mice including reduced morbidity and mortality, bacterial burden, maintenance of alveolar macrophages, and reduced lung inflammation and damage. The lung microbiome of allergic mice differed from that of non-allergic mice during co-infection and antibiotic-induced perturbation to the microbiome rendered allergic animals susceptible to severe morbidity. Our data suggest that responses to co-infection in allergic hosts likely depends on the immune and microbiome states and that antibiotics should be used with caution in individuals with underlying chronic lung disease.
机译:哮喘是一种慢性气道病症,可在呼吸道感染期间加剧。我们以前的工作与流行病学结果一起,哮喘患者在2009年大流行期间患有严重流感的可能性,表明流感的额外并发症如增加对细菌超育的易感性,可能在过敏宿主中减轻。为了测试这一假设,我们开发了一种“三疾病”的小鼠模型,其中对叶绿犬病过敏的小鼠与流感病毒和肺炎链球菌相隔七天。在过敏小鼠中注意到对共同感染的已知协同作用的显着改变,包括降低发病率和死亡率,细菌负担,肺泡巨噬细胞的维持,降低肺炎和损伤。过敏小鼠的肺部微生物组在共感染和抗生素诱导的微生物组中扰动的非过敏小鼠的肺部微生物组在微生物组中的过敏性动物的扰动不同。我们的数据表明,对过敏宿主中的共同感染的反应可能取决于免疫和微生物组,并且抗生素应在患有慢性肺病的个体中慎用。

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