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Genetic restriction of murine hepatitis virus type 3 expression in liver and brain: comparative study in BALB/c and C3H mice by immunochemistry and hybridization in situ

机译:小鼠肝和脑中3型肝炎病毒表达的遗传限制:通过免疫化学和原位杂交在BALB / c和C3H小鼠中的比较研究

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摘要

To study the host-dependent genetic variations in murine hepatitis virus type 3 (MHV 3) induced diseases, we localized the sites of MHV 3 (Mill Hill strain) expression within liver and brain by immunohistochemistry or hybridization in situ. Two strains of mice were studied: BALB/c mice, which develop an acute and lethal hepatitis and C3H mice which develop a chronic brain infection. In BALB/c mice, viral RNA and antigens appeared during the first 24 h post infection (p.i.) in liver, whereas viral RNA was barely detectable in brain, up until death at day 3 p.i. In C3H mice, viral RNA and antigens were detected simultaneously in liver and brain only at day 2 p.i. In brain, the virus was detected in meningeal and ependymal cells and in perivascular cortical areas (days 5 and 7 p.i.). After day 49, the virus was no longer detected in brain parenchyma, but persisted in meningeal cells. Two host-dependent genetic differences in viral processing were observed in the liver: (1) the virus was first detected in Kupffer cells in BALB/c mice and mostly in hepatocytes in C3H mice; (2) in BALB/c mice, the 180 kDa S viral glycoprotein appeared more frequently cleaved in 90 kDa form than in C3H mice.
机译:为了研究鼠源性3型肝炎病毒(MHV 3)引起的宿主依赖性遗传变异,我们通过免疫组织化学或原位杂交在肝和脑中定位了MHV 3(米尔山毒株)表达的位点。研究了两种小鼠品系:BALB / c小鼠,其发展为急性和致死性肝炎,C3H小鼠,其发展为慢性脑部感染。在BALB / c小鼠中,病毒RNA和抗原在感染后(p.i.)的最初24小时内出现在肝脏中,而直到在p.i第3天死亡时才在脑中检测到病毒RNA。在C3H小鼠中,仅在p.i第2天同时在肝和脑中同时检测到病毒RNA和抗原。在脑中,在脑膜和室管膜细胞以及血管周皮层区域(p.i.第5天和第7天)中检测到病毒。第49天后,在脑实质中不再检测到该病毒,而是在脑膜细胞中持续存在。在肝脏中观察到两个宿主依赖的病毒加工遗传差异:(1)该病毒首先在BALB / c小鼠的Kupffer细胞中发现,而在C3H小鼠的肝细胞中首先发现; (2)在BALB / c小鼠中,以90 kDa的形式出现的180 kDa S病毒糖蛋白的裂解频率比C3H小鼠更高。

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