Department of Microbiology and Immunology, University of Rochester School of Medicine and Dentistry, Rochester, NY 14642, USA.
Virology. 2010 May 10;400(2):224-32. doi: 10.1016/j.virol.2010.02.001. Epub 2010 Feb 25.
Influenza virus leads to acute respiratory disease resulting in seasonal epidemics and periodic pandemics. Little is known about the signaling events that regulate host defense to influenza. One particular pathway, the c-Jun amino-terminal kinase (JNK) cascade is activated following influenza infection and blocking JNK leads to enhanced viral replication. We hypothesize that Mixed Lineage Kinase 3 (MLK3), an upstream regulator of JNK, is involved in the host response to influenza. To test this, wild-type and MLK3-/- mice were infected with pathogenic strain of influenza A virus, A/PR/8/34 (PR8). Although, cellular and humoral immune responses were similar between wild-type and MLK3-/- hosts, the viral load in the lungs was comparatively higher in MLK3-/- mice at day 8 post-infection. Consistent with this, MLK3-/- murine lung fibroblast and epithelial cells had prolonged survival and increased virion production following infection compared to wild-type. These findings support a role for MLK3 in viral production during influenza infection.
流感病毒可导致急性呼吸道疾病,引发季节性流行和周期性大流行。目前人们对调节宿主防御流感的信号事件知之甚少。一条特定的信号通路,即 c-Jun 氨基末端激酶(JNK)级联反应,在流感感染后被激活,而阻断 JNK 会导致病毒复制增强。我们假设混合谱系激酶 3(MLK3),JNK 的上游调节因子,参与宿主对流感的反应。为了验证这一点,野生型和 MLK3-/-小鼠感染了致病性流感 A 病毒株 A/PR/8/34(PR8)。尽管野生型和 MLK3-/-宿主的细胞和体液免疫反应相似,但在感染后 8 天,MLK3-/-小鼠肺部的病毒载量明显更高。与此一致的是,与野生型相比,MLK3-/-小鼠的肺成纤维细胞和上皮细胞在感染后存活时间延长,病毒粒子生成增加。这些发现支持 MLK3 在流感感染期间病毒产生中的作用。
