实验室减毒狂犬病病毒通过诱导基质金属蛋白酶 8 促进血脑屏障开放。
Lab-Attenuated Rabies Virus Facilitates Opening of the Blood-Brain Barrier by Inducing Matrix Metallopeptidase 8.
机构信息
State Key Laboratory of Agricultural Microbiology, Huazhong Agricultural Universitygrid.35155.37, Wuhan, China.
Key Laboratory of Preventive Veterinary Medicine of Hubei Province, College of Veterinary Medicine, Huazhong Agricultural Universitygrid.35155.37, Wuhan, China.
出版信息
J Virol. 2022 Sep 14;96(17):e0105022. doi: 10.1128/jvi.01050-22. Epub 2022 Aug 25.
Infection with laboratory-attenuated rabies virus (RABV), but not wild-type (wt) RABV, can enhance the permeability of the blood-brain barrier (BBB), which is considered a key determinant for RABV pathogenicity. A previous study showed that the enhancement of BBB permeability is directly due not to RABV infection but to virus-induced inflammatory molecules. In this study, the effect of the matrix metallopeptidase (MMP) family on the permeability of the BBB during RABV infection was evaluated. We found that the expression level of MMP8 was upregulated in mice infected with lab-attenuated RABV but not with wt RABV. Lab-attenuated RABV rather than wt RABV activates inflammatory signaling pathways mediated by the nuclear factor κB (NF-κB) and mitogen-activated protein kinase (MAPK) pathways. Activated NF-κB (p65) and AP-1 (c-Fos) bind to the MMP8 promoter, resulting in upregulation of its transcription. Analysis of mouse brains infected with the recombinant RABV expressing MMP8 indicated that MMP8 enhanced BBB permeability, leading to infiltration of inflammatory cells into the central nervous system (CNS). In brain-derived endothelial cells, treatment with MMP8 recombinant protein caused the degradation of tight junction (TJ) proteins, and the application of an MMP8 inhibitor inhibited the degradation of TJ proteins after RABV infection. Furthermore, an experiment using an MMP8 inhibitor during RABV infection demonstrated that BBB opening was diminished. In summary, our data suggest that the infection of lab-attenuated RABV enhances the BBB opening by upregulating MMP8. The ability to change BBB permeability was associated with the pathogenicity of RABV. BBB permeability was enhanced by infection with lab-attenuated RABV instead of wt RABV, allowing immune cells to infiltrate into the CNS. We found that MMP8 plays an important role in enhancing BBB permeability by degradation of TJ proteins during RABV infection. Using an MMP8 selective inhibitor restores the reduction of TJ proteins. We reveal that MMP8 is upregulated via the MAPK and NF-κB inflammatory pathways, activated by lab-attenuated RABV infection but not wt RABV. Our findings suggest that MMP8 has a critical role in modulating the opening of the BBB during RABV infection, which provides fresh insight into developing effective therapeutics for rabies and infection with other neurotropic viruses.
实验室减毒狂犬病病毒(RABV)感染而非野生型(wt)RABV 感染可增强血脑屏障(BBB)的通透性,这被认为是 RABV 致病性的关键决定因素。先前的研究表明,BBB 通透性的增强不是直接由于 RABV 感染,而是由于病毒诱导的炎症分子。在这项研究中,评估了基质金属蛋白酶(MMP)家族在 RABV 感染期间对 BBB 通透性的影响。我们发现,感染实验室减毒 RABV 的小鼠中 MMP8 的表达水平上调,但感染 wt RABV 的小鼠中则没有。实验室减毒 RABV 而不是 wt RABV 激活了核因子κB(NF-κB)和丝裂原活化蛋白激酶(MAPK)途径介导的炎症信号通路。激活的 NF-κB(p65)和 AP-1(c-Fos)与 MMP8 启动子结合,导致其转录上调。分析感染表达 MMP8 的重组 RABV 的小鼠脑组织表明,MMP8 增强了 BBB 的通透性,导致炎症细胞浸润中枢神经系统(CNS)。在脑源性内皮细胞中,用 MMP8 重组蛋白处理导致紧密连接(TJ)蛋白降解,并且在用 RABV 感染后应用 MMP8 抑制剂抑制 TJ 蛋白的降解。此外,在 RABV 感染期间使用 MMP8 抑制剂的实验表明,BBB 开放减少。总之,我们的数据表明,实验室减毒 RABV 通过上调 MMP8 增强 BBB 开放。改变 BBB 通透性的能力与 RABV 的致病性有关。感染实验室减毒 RABV 而非 wt RABV 可增强 BBB 通透性,使免疫细胞浸润中枢神经系统。我们发现,在 RABV 感染过程中,MMP8 通过降解 TJ 蛋白在增强 BBB 通透性方面发挥重要作用。使用 MMP8 选择性抑制剂可恢复 TJ 蛋白的减少。我们揭示 MMP8 通过 MAPK 和 NF-κB 炎症途径上调,由实验室减毒 RABV 感染激活,但 wt RABV 不激活。我们的研究结果表明,MMP8 在 RABV 感染期间调节 BBB 开放中起关键作用,这为开发狂犬病和其他神经嗜性病毒感染的有效治疗方法提供了新的见解。
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