首页> 外文期刊>Journal of Virology >Attenuated rabies virus activates, while pathogenic rabies virus evades, the host innate immune responses in the central nervous system
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Attenuated rabies virus activates, while pathogenic rabies virus evades, the host innate immune responses in the central nervous system

机译:减毒狂犬病毒激活,而狂犬病毒致病性躲避,主持人先天在中枢神经系统的免疫反应

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Rabies virus (RV) induces encephalomyelitis in humans and animals. However, the pathogenic mechanism of rabies is not fully understood. To investigate the host responses to RV infection, we examined and compared the pathology, particularly the inflammatory responses, and the gene expression profiles in the brains of mice infected with wild-type (wt) virus silver-haired bat RV (SHBRV) or laboratory-adapted virus B2C, using a mouse genomic array (Affymetrix). Extensive inflammatory responses were observed in animals infected with the attenuated RV, but little or no inflammatory responses were found in mice infected with wt RV. Furthermore, attenuated RV induced the expression of the genes involved in the innate immune and antiviral responses, especially those related to the alpha/beta interferon (IFN-alpha/beta) signaling pathways and inflammatory chemokines. For the IFN-alpha/beta signaling pathways, many of the interferon regulatory genes, such as the signal transduction activation transducers and interferon regulatory factors, as well as the effector genes, for example, 2'-5'-oligoadenylate synthetase and myxovirus proteins, are highly induced in mice infected with attenuated RV. However, many of these genes were not up-regulated in mice infected with wt SHBRV. The data obtained by microarray analysis were confirmed by real-time PCR. Together, these data suggest that attenuated RV activates, while pathogenic RV evades, the host innate immune and antiviral responses.
机译:狂犬病毒(RV)诱发脑脊髓炎人类和动物。狂犬病是机制不完全清楚。调查RV感染的宿主反应,我们检查和病理相比,特别是炎症反应,基因表达谱在老鼠的大脑野生型(wt)病毒感染满头银发蝙蝠房车(SHBRV)或laboratory-adapted病毒B2C,使用鼠标基因阵列(Affymetrix)。广泛的炎症反应观察动物感染了减毒房车,但是很少或没有炎症反应被发现老鼠感染wt房车。房车诱导相关基因的表达在先天免疫和抗病毒反应,尤其是那些与α/β有关干扰素(IFN-alpha /β)信号通路和炎症趋化因子。IFN-alpha /β信号通路,许多干扰素调控基因,如信号转导激活传感器和干扰素调节因子,以及效应的基因,例如,2 ' 5 ' -oligoadenylate合成酶和myxovirus蛋白质,是高度诱导衰减RV感染的老鼠。然而,许多这些基因上调小鼠感染了wt SHBRV。微阵列分析获得的数据实时PCR证实了。建议减毒房车激活,而宿主先天免疫和致病性房车躲避抗病毒反应。

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