不同毒力的狂犬病病毒通过 MAPK 和 NF-κB 通路在体内和体外调节炎症反应。

Rabies viruses of different virulence regulates inflammatory responses both in vivo and in vitro via MAPK and NF-κB pathway.

机构信息

Key Laboratory of Medical Virology, Ministry of Health, National Institute for Viral Disease Control and Prevention, NHC Key Laboratory of Biosafety, Chinese Center for Disease Control and Prevention, Beijing, 102206, China; Pathogenic Microbiology Institute, Tianjin Centers for Disease Control and Prevention, Tianjin, 300011, China.

出版信息

Mol Immunol. 2020 Sep;125:70-82. doi: 10.1016/j.molimm.2020.06.011. Epub 2020 Jul 8.

DOI:10.1016/j.molimm.2020.06.011

PMID:32652362

Abstract

Immune responses and central nervous system dysfunction are two main factors to be considered during rabies virus (RABV) infection. However, the mechanisms by which RABV strains of different virulence regulate with chemokine expression and the signaling pathways responsible for the immune responses in the terminal stage of infection both in vivo and in vitro have not been fully elucidated. In this study, we found low expression levels of proinflammatory chemokines in the mouse brain upon infection with street RABV strains (CXZ17 and HN10) at the late stage of infection. We also examined the difference in inflammatory response upon infection with RABV strains of different virulence in a mouse model. We found that the expression of proinflammatory chemokines increased to a varying degree upon infection with street RABV (CXZ17 and HN10) or laboratory-fixed RABV (CVS-11, aG, and CTN); CXCL10, CCL5, and CCL2 were the most significantly upregulated chemokines in brain tissue and microglial BV-2 cells in response to infection with RABV strains of different virulence. Our data also demonstrate significant activation of the MAPK and NF-κB pathways in mouse brain tissue at the late stage of RABV infection. We also found (i) low phosphorylation signals of MAPK and NF-κB p65 in neuronal cells upon infection with CXZ17 and HN10 in the mouse brain and (ii) strong phosphorylation signals in cerebrovascular endothelial cells and neuronal cells upon CTN or aG infection. Moreover, we quantified the nuclear localization status of MAPK signals and NF-κB p65 upon infection with CVS-11, aG, and CTN in BV-2 cells in vitro. We also found (i) that the activation of the p38, ERK1/2, and NF-κB p65 pathway, which stimulates CXCL10, CCL5, and CCL2 expression upon infection with RABV strains of different virulence (aG, CTN, and CVS-11), is triggered after virus entry into BV-2 cells and (ii) that the expression of CXCL10, CCL5, and CCL2 is required for the activation of NF-κB, p38, and ERK1/2, but not JNK. Overall, our study provides insight into the regulation of inflammatory responses mediated by MAPK and NF-κB in the mouse brain and in microglial cells upon RABV infection of different virulence.

摘要

免疫反应和中枢神经系统功能障碍是狂犬病病毒（RABV）感染时需要考虑的两个主要因素。然而，不同毒力的 RABV 株如何调节趋化因子的表达，以及体内和体外感染终末期负责免疫反应的信号通路，尚未完全阐明。在这项研究中，我们发现感染街毒株（CXZ17 和 HN10）后，小鼠大脑中的促炎趋化因子表达水平较低。我们还检查了不同毒力的 RABV 株感染小鼠模型中炎症反应的差异。我们发现，感染街毒株（CXZ17 和 HN10）或实验室固定毒株（CVS-11、aG 和 CTN）后，促炎趋化因子的表达均有不同程度的增加；CXCL10、CCL5 和 CCL2 是对不同毒力的 RABV 株感染反应最显著上调的趋化因子，在脑组织和小胶质细胞 BV-2 细胞中。我们的数据还表明，在 RABV 感染的晚期，MAPK 和 NF-κB 通路在小鼠脑组织中显著激活。我们还发现：（i）在感染 CXZ17 和 HN10 后，神经元细胞中的 MAPK 和 NF-κB p65 的磷酸化信号较弱；（ii）在感染 CTN 或 aG 后，脑血管内皮细胞和神经元细胞中的磷酸化信号较强。此外，我们还定量了 MAPK 信号和 NF-κB p65 在体外感染 CVS-11、aG 和 CTN 后在 BV-2 细胞中的核定位状态。我们还发现：（i）感染不同毒力的 RABV 株（aG、CTN 和 CVS-11）后，激活 MAPK 信号通路和 NF-κB p65，刺激 CXCL10、CCL5 和 CCL2 的表达，是在病毒进入 BV-2 细胞后触发的；（ii）CXCL10、CCL5 和 CCL2 的表达对于 NF-κB、p38 和 ERK1/2 的激活是必需的，但对于 JNK 则不是必需的。总的来说，我们的研究提供了对不同毒力的 RABV 感染后，小鼠大脑和小胶质细胞中 MAPK 和 NF-κB 介导的炎症反应的调节的深入了解。