Rauer Mathias, Götz Jürgen, Schuppli Daniel, Staeheli Peter, Hausmann Jürgen
Department of Virology, Institute for Medical Microbiology and Hygiene, University of Freiburg, D-79104 Freiburg, Germany.
J Virol. 2004 Apr;78(7):3621-32. doi: 10.1128/jvi.78.7.3621-3632.2004.
The nucleoprotein (N) of Borna disease virus (BDV) is the major target of the disease-inducing antiviral CD8 T-cell response in the central nervous system of mice. We established two transgenic mouse lines which express BDV-N in either neurons (Neuro-N) or astrocytes (Astro-N). Despite strong transgene expression, neurological disease or gross behavioral abnormalities were not observed in these animals. When Neuro-N mice were infected as adults, replication of BDV was severely impaired and was restricted to brain areas with a low density of transgene-expressing cells. Notably, the virus failed to replicate in the transgene-expressing granular and pyramidal neurons of the hippocampus (which are usually the preferred host cells of BDV). When Neuro-N mice were infected within the first 5 days of life, replication of BDV was not suppressed in most neurons, presumably because the onset of transgene expression in the brain occurred after these cells became infected with BDV. Astro-N mice remained susceptible to BDV infection, but they were resistant to BDV-induced neurological disorder. Unlike their nontransgenic littermates, Neuro-N mice with persistent BDV infection did not develop neurological disease after immunization with a vaccinia virus vector expressing BDV-N. In contrast to the situation in wild-type mice, this treatment also failed to induce N-specific CD8 T cells in the spleens of both transgenic mouse lines. Thus, while resistance to BDV infection in N-expressing neurons appeared to result from untimely expression of a viral nucleocapsid component, the resistance to BDV-induced neuropathology probably resulted from immunological tolerance.
博尔纳病病毒(BDV)的核蛋白(N)是小鼠中枢神经系统中引发疾病的抗病毒CD8 T细胞反应的主要靶点。我们建立了两个转基因小鼠品系,它们分别在神经元(Neuro-N)或星形胶质细胞(Astro-N)中表达BDV-N。尽管转基因表达强烈,但在这些动物中未观察到神经疾病或明显的行为异常。当Neuro-N小鼠成年后被感染时,BDV的复制受到严重损害,并局限于转基因表达细胞密度低的脑区。值得注意的是,该病毒未能在海马体中转基因表达颗粒神经元和锥体神经元中复制(这些神经元通常是BDV的首选宿主细胞)。当Neuro-N小鼠在出生后的前5天内被感染时,BDV在大多数神经元中的复制并未受到抑制,大概是因为大脑中转基因表达的开始发生在这些细胞被BDV感染之后。Astro-N小鼠仍然易受BDV感染,但它们对BDV诱导的神经紊乱具有抗性。与它们的非转基因同窝小鼠不同,持续感染BDV的Neuro-N小鼠在用表达BDV-N的痘苗病毒载体免疫后并未出现神经疾病。与野生型小鼠的情况相反,这种处理也未能在两个转基因小鼠品系的脾脏中诱导出N特异性CD8 T细胞。因此,虽然在表达N的神经元中对BDV感染的抗性似乎是由于病毒核衣壳成分的表达时间不当所致,但对BDV诱导的神经病理学的抗性可能是由于免疫耐受。