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Differential Host Immune Responses after Infection with Wild-Type or Lab-Attenuated Rabies Viruses in Dogs

机译:在狗中感染野生型或实验室减毒的狂犬病病毒后的差异宿主免疫反应

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摘要

Rabies virus (RABV) induces encephalomyelitis in humans and animals. One of the major problems with rabies is that the infected individuals most often do not develop virus neutralizing antibodies (VNA). In this study we have investigated the host immune response to RABV infection in dogs, using a live-attenuated (TriGAS) or a wild-type (wt) (DRV-NG11) RABV isolated from a rabid dog.Methodology/Principal FindingsThe experimental infection of dogs with TriGAS induced high levels of VNA in the serum, whereas wt RABV infection did not. Dogs infected with TriGAS developed antibodies against the virus including its glycoprotein, whereas dogs infected with DRV-NG11 only developed rabies antibodies that are presumably specific for the nucleoprotein, (N) and not the glycoprotein (G). We show that infection with TriGAS induces early activation of B cells in the draining lymph nodes and persistent activation of DCs and B cells in the blood. On the other hand, infection with DRV-NG11 fails to induce the activation of DCs and B cells and further reduces CD4 T cell production. Further, we show that intrathecal (IT) immunization of TriGAS not only induced high levels of VNA in the serum but also in the CSF while intramuscular (IM) immunization of TriGAS induced VNA only in the serum. In addition, high levels of total protein and WBC were detected in the CSF of IT immunized dogs, indicating the transient enhancement of blood-brain barrier (BBB) permeability, which is relevant to the passage of immune effectors from periphery into the CNS.
机译:狂犬病病毒(RABV)诱发人和动物的脑脊髓炎。狂犬病的主要问题之一是,受感染的人最常不发展病毒中和抗体(VNA)。在这项研究中,我们使用从狂犬病犬中分离的活减毒(TriGAS)或野生型(wt)(DRV-NG11)RABV调查了犬对RABV感染的宿主免疫反应。方法/主要发现患有TriGAS的犬只可诱导血清中高水平的VNA,而野生型RABV感染则不会。被TriGAS感染的狗产生了针对包括其糖蛋白在内的病毒的抗体,而被DRV-NG11感染的狗仅产生了狂犬病抗体,这种狂犬病抗体可能对核蛋白(N)而非糖蛋白(G)具有特异性。我们显示,用TriGAS感染可诱导引流淋巴结中B细胞的早期活化以及血液中DC和B细胞的持续活化。另一方面,DRV-NG11的感染不能诱导DC和B细胞的激活,并进一步减少CD4 T细胞的产生。此外,我们显示TriGAS的鞘内(IT)免疫不仅诱导血清中高水平的VNA,而且在脑脊液中诱导,而TriGAS的肌内(IM)免疫仅诱导血清中的VNA。另外,在IT免疫的狗的脑脊液中检测到高水平的总蛋白和白细胞,表明血脑屏障(BBB)通透性的瞬时增强,这与免疫效应子从外周进入中枢神经系统有关。

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