首页> 美国卫生研究院文献>Journal of Visualized Experiments : JoVE >Intracerebroventricular and Intravascular Injection of Viral Particles and Fluorescent Microbeads into the Neonatal Brain
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Intracerebroventricular and Intravascular Injection of Viral Particles and Fluorescent Microbeads into the Neonatal Brain

机译:脑室内和血管内向新生儿脑内注射病毒颗粒和荧光微珠

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摘要

In the study on the pathogenesis of viral encephalitis, the infection method is critical. The first of the two main infectious routes to the brain is the hematogenous route, which involves infection of the endothelial cells and pericytes of the brain. The second is the intracerebroventricular (ICV) route. Once within the central nervous system (CNS), viruses may spread to the subarachnoid space, meninges, and choroid plexus via the cerebrospinal fluid. In experimental models, the earliest stages of CNS viral distribution are not well characterized, and it is unclear whether only certain cells are initially infected. Here, we have analyzed the distribution of cytomegalovirus (CMV) particles during the acute phase of infection, termed primary viremia, following ICV or intravascular (IV) injection into the neonatal mouse brain. In the ICV injection model, 5 µl of murine CMV (MCMV) or fluorescent microbeads were injected into the lateral ventricle at the midpoint between the ear and eye using a 10-µl syringe with a 27 G needle. In the IV injection model, a 1-ml syringe with a 35 G needle was used. A transilluminator was used to visualize the superficial temporal (facial) vein of the neonatal mouse. We infused 50 µl of MCMV or fluorescent microbeads into the superficial temporal vein. Brains were harvested at different time points post-injection. MCMV genomes were detected using the in situ hybridization method. Fluorescent microbeads or green fluorescent protein expressing recombinant MCMV particles were observed by fluorescent microscopy. These techniques can be applied to many other pathogens to investigate the pathogenesis of encephalitis.
机译:在病毒性脑炎发病机制的研究中,感染方法至关重要。通往脑部的两种主要传染途径中的第一种是血源性途径,其涉及脑部的内皮细胞和周细胞的感染。第二种是脑室内(ICV)途径。一旦进入中枢神经系统(CNS),病毒可能会通过脑脊髓液扩散到蛛网膜下腔,脑膜和脉络丛。在实验模型中,CNS病毒分布的最早阶段没有得到很好的表征,目前尚不清楚是否仅最初感染了某些细胞。在这里,我们分析了感染ICV或将血管内(IV)注入新生小鼠大脑后的急性感染期巨细胞病毒(CMV)颗粒的分布,称为急性病毒血症。在ICV注射模型中,使用带有27 G针头的10 µl注射器将5 µl鼠CMV(MCMV)或荧光微珠注射到耳朵和眼睛之间中点的侧脑室。在IV注射模型中,使用了带有35 G针头的1 ml注射器。使用透照器来可视化新生小鼠的颞颞(面)静脉。我们向颞浅静脉注入50 µl MCMV或荧光微珠。在注射后的不同时间点收获大脑。使用原位杂交方法检测MCMV基因组。通过荧光显微镜观察到表达荧光微珠或绿色荧光蛋白的重组MCMV颗粒。这些技术可以应用于许多其他病原体,以研究脑炎的发病机理。

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