Zhang Xiaowei, Zheng Zhenhua, Liu Xijuan, Shu Bo, Mao Panyong, Bai Bingke, Hu Qinxue, Luo Minhua, Ma Xiaohe, Cui Zongqiang, Wang Hanzhong
Key Laboratory of Special Pathogens and Biosafety, Center for Emerging Infectious Diseases, Wuhan Institute of Virology, Chinese Academy of Sciences, Xiaohongshan No.44, Wuhan, 430071, China.
State Key Laboratory of Virology, Wuhan Institute of Virology, Chinese Academy of Sciences, Xiaohongshan No.44, Wuhan, 430071, China.
J Neuroinflammation. 2016 Aug 30;13(1):209. doi: 10.1186/s12974-016-0665-9.
Tick-borne encephalitis virus (TBEV) is one of the most important flaviviruses that targets the central nervous system (CNS) and causes encephalitides in humans. Although neuroinflammatory mechanisms may contribute to brain tissue destruction, the induction pathways and potential roles of specific chemokines in TBEV-mediated neurological disease are poorly understood.
BALB/c mice were intracerebrally injected with TBEV, followed by evaluation of chemokine and cytokine profiles using protein array analysis. The virus-infected mice were treated with the CC chemokine antagonist Met-RANTES or anti-RANTES mAb to determine the role of RANTES in affecting TBEV-induced neurological disease. The underlying signaling mechanisms were delineated using RANTES promoter luciferase reporter assay, siRNA-mediated knockdown, and pharmacological inhibitors in human brain-derived cell culture models.
In a mouse model, pathological features including marked inflammatory cell infiltrates were observed in brain sections, which correlated with a robust up-regulation of RANTES within the brain but not in peripheral tissues and sera. Antagonizing RANTES within CNS extended the survival of mice and reduced accumulation of infiltrating cells in the brain after TBEV infection. Through in vitro studies, we show that virus infection up-regulated RANTES production at both mRNA and protein levels in human brain-derived cell lines and primary progenitor-derived astrocytes. Furthermore, IRF-3 pathway appeared to be essential for TBEV-induced RANTES production. Site mutation of an IRF-3-binding motif abrogated the RANTES promoter activity in virus-infected brain cells. Moreover, IRF-3 was activated upon TBEV infection as evidenced by phosphorylation of TBK1 and IRF-3, while blockade of IRF-3 activation drastically reduced virus-induced RANTES expression.
Our findings together provide insights into the molecular mechanism underlying RANTES production induced by TBEV, highlighting its potential importance in the process of neuroinflammatory responses to TBEV infection.
蜱传脑炎病毒(TBEV)是最重要的黄病毒之一,可靶向中枢神经系统(CNS)并导致人类脑炎。尽管神经炎症机制可能导致脑组织破坏,但特定趋化因子在TBEV介导的神经系统疾病中的诱导途径和潜在作用仍知之甚少。
将TBEV脑内注射到BALB/c小鼠中,随后使用蛋白质阵列分析评估趋化因子和细胞因子谱。用CC趋化因子拮抗剂Met-RANTES或抗RANTES单克隆抗体处理病毒感染的小鼠,以确定RANTES在影响TBEV诱导的神经系统疾病中的作用。在人脑来源的细胞培养模型中,使用RANTES启动子荧光素酶报告基因测定、siRNA介导的敲低和药理学抑制剂来阐明潜在的信号传导机制。
在小鼠模型中,在脑切片中观察到包括明显炎性细胞浸润在内的病理特征,这与脑内RANTES的强烈上调相关,但在外周组织和血清中未观察到。在中枢神经系统内拮抗RANTES可延长小鼠存活时间,并减少TBEV感染后脑中浸润细胞的积累。通过体外研究,我们发现病毒感染在人脑来源的细胞系和原代祖细胞来源的星形胶质细胞中,在mRNA和蛋白质水平上均上调了RANTES的产生。此外,IRF-3途径似乎对于TBEV诱导的RANTES产生至关重要。IRF-3结合基序的位点突变消除了病毒感染的脑细胞中RANTES启动子活性。此外,TBEV感染后IRF-3被激活,表现为TBK1和IRF-3的磷酸化,而阻断IRF-3激活可显著降低病毒诱导的RANTES表达。
我们的研究结果共同揭示了TBEV诱导RANTES产生的分子机制,突出了其在TBEV感染神经炎症反应过程中的潜在重要性。
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