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实验性杜文黑格病毒感染后小鼠脑转录组分析显示先天免疫反应和焦亡性细胞死亡途径的激活。

Analysis of Mouse Brain Transcriptome After Experimental Duvenhage Virus Infection Shows Activation of Innate Immune Response and Pyroptotic Cell Death Pathway.

作者信息

Koraka Penelope, Martina Byron E E, van den Ham Henk-Jan, Zaaraoui-Boutahar Fatiha, van IJcken Wilfred, Roose Jouke, van Amerongen Geert, Andeweg Arno, Osterhaus Albertus D M E

机构信息

Department of Viroscience, Erasmus Medical Centre, Rotterdam, Netherlands.

Viroclinics Biosciences B.V., Rotterdam, Netherlands.

出版信息

Front Microbiol. 2018 Mar 20;9:397. doi: 10.3389/fmicb.2018.00397. eCollection 2018.

Abstract

Rabies is an important neglected disease, characterized by invariably fatal encephalitis. Several studies focus on understanding the pathogenic mechanisms of the prototype lyssavirus rabies virus (RABV) infection, and little is known about the pathogenesis of rabies caused by other lyssaviruses. We sought to characterize the host response to Duvenhage virus infection and compare it with responses observed during RABV infection by gene expression profiling of brains of mice with the respective infections. We found in both infections differentially expressed genes leading to increased expression of type I interferons (IFNs), chemokines, and proinflammatory cytokines. In addition several genes of the IFN signaling pathway are up-regulated, indicating a strong antiviral response and activation of the negative feedback mechanism to limit type I IFN responses. Furthermore we provide evidence that in the absence of significant neuronal apoptotic death, cell death of neurons is mediated via the pyroptotic pathway in both infections. Taken together, we have identified several genes and/or pathways for both infections that could be used to explore novel approaches for intervention strategies against rabies.

摘要

狂犬病是一种重要的被忽视疾病,其特征是引发必死无疑的脑炎。多项研究聚焦于了解典型狂犬病病毒(RABV)感染的致病机制,而对于其他狂犬病病毒所致狂犬病的发病机制却知之甚少。我们试图通过对感染相应病毒的小鼠大脑进行基因表达谱分析,来描述宿主对杜文海格病毒感染的反应,并将其与狂犬病病毒感染期间观察到的反应进行比较。我们发现在两种感染中均存在差异表达基因,这些基因导致I型干扰素(IFN)、趋化因子和促炎细胞因子的表达增加。此外,IFN信号通路的几个基因上调,表明存在强烈的抗病毒反应以及限制I型IFN反应的负反馈机制的激活。此外,我们提供的证据表明,在没有明显神经元凋亡性死亡的情况下,两种感染中神经元的细胞死亡均通过焦亡途径介导。综上所述,我们已经确定了两种感染的几个基因和/或途径,可用于探索针对狂犬病的新型干预策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d2f7/5869263/2c7ef63bd8db/fmicb-09-00397-g001.jpg

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