Hausmann J, Hallensleben W, de la Torre J C, Pagenstecher A, Zimmermann C, Pircher H, Staeheli P
Department of Virology, Institut für Medizinische Mikrobiologie und Hygiene, Universität Freiburg, D-79008 Freiburg, Germany.
Proc Natl Acad Sci U S A. 1999 Aug 17;96(17):9769-74. doi: 10.1073/pnas.96.17.9769.
Infection of neonates with Borna disease virus (BDV) induces severe meningoencephalitis and neurological disorder in wild-type but not in beta(2)-microglobulin-deficient mice of strain MRL (H-2(k)). Temporary in vivo depletion of CD8(+) T cells delayed BDV-induced disease for several weeks. Depletion of CD4(+) T cells had a similar beneficial effect, indicating that the BDV-induced neurological disorder in mice is a CD4(+) T cell-dependent immunopathological process that is mediated by CD8(+) T cells. Lymphocytes prepared from brains of diseased mice were mainly from the CD8(+) T cell subset. They showed up-regulation of activation markers and exerted strong MHC I-restricted cytotoxic activity against target cells expressing the BDV nucleoprotein p40. Infection of B10.BR (H-2(k)) or congenic C57BL/10 (H-2(b)) mice resulted in symptomless, lifelong persistence of BDV in the brain. Superinfection with a recombinant vaccinia virus expressing BDV p40 but not with other vaccinia viruses induced severe neurological disease and encephalitis in persistently infected B10.BR mice but not in persistently infected C57BL/10 mice, indicating that the disease-inducing T cell response is restricted to the nucleoprotein of BDV in H-2(k) mice. Our results demonstrate that the cellular arm of the immune system may ignore the presence of a replicating virus in the central nervous system until proper antigenic stimulation at a peripheral site triggers the antiviral response.
新生小鼠感染博尔纳病病毒(BDV)会在野生型小鼠中引发严重的脑膜脑炎和神经紊乱,但在MRL(H-2(k))品系的β2-微球蛋白缺陷小鼠中则不会。体内暂时清除CD8+ T细胞可使BDV诱导的疾病延迟数周。清除CD4+ T细胞也有类似的有益效果,这表明小鼠中BDV诱导的神经紊乱是一个由CD8+ T细胞介导的、依赖CD4+ T细胞的免疫病理过程。从患病小鼠大脑中制备的淋巴细胞主要来自CD8+ T细胞亚群。它们表现出激活标志物的上调,并对表达BDV核蛋白p40的靶细胞具有强大的MHC I限制性细胞毒性活性。B10.BR(H-2(k))或同基因C57BL/10(H-2(b))小鼠感染后,BDV会在大脑中无症状地终身持续存在。用表达BDV p40的重组痘苗病毒进行重复感染,但用其他痘苗病毒则不会,这会在持续感染的B10.BR小鼠中引发严重的神经疾病和脑炎,但在持续感染的C57BL/10小鼠中则不会,这表明在H-2(k)小鼠中,诱导疾病的T细胞反应仅限于BDV的核蛋白。我们的结果表明,免疫系统的细胞分支可能会忽略中枢神经系统中复制病毒的存在,直到外周部位受到适当的抗原刺激触发抗病毒反应。