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博尔纳病病毒诱导的小鼠神经紊乱:新生小鼠感染会导致免疫病理学变化。

Borna disease virus-induced neurological disorder in mice: infection of neonates results in immunopathology.

作者信息

Hallensleben W, Schwemmle M, Hausmann J, Stitz L, Volk B, Pagenstecher A, Staeheli P

机构信息

Abteilung Virologie, Institut für Medizinische Mikrobiologie & Hygiene, Universität Freiburg, Germany.

出版信息

J Virol. 1998 May;72(5):4379-86. doi: 10.1128/JVI.72.5.4379-4386.1998.

Abstract

Borna disease virus (BDV) is a neurotropic nonsegmented negative-stranded RNA virus that persistently infects warm-blooded animals. In horses and other natural animal hosts, infections with BDV cause meningoencephalitis and behavioral disturbances. Experimental infection of adult mice takes a nonsymptomatic course, an observation previously believed to indicate that this animal species is not suitable for pathogenesis studies. We now demonstrate that BDV frequently induces severe neurological disease in infected newborn mice. Signs of neurological disease were first observed 4 to 6 weeks after intracerebral infection. They included a characteristic nonphysiological position of the hind limbs at an early stage of the disease and paraparesis at a later stage. Histological examination revealed large numbers of perivascular and meningeal inflammatory cells in brains of diseased mice and, unexpectedly, no increase in immunoreactivity to glial fibrillar acidic protein. The incidence and severity of BDV-induced disease varied dramatically among mouse strains. While only 13% of the infected C57BL/6 mice showed disease symptoms, which were mostly transient, more than 80% of the infected MRL mice developed severe neurological disorder. In spite of these differences in susceptibility to disease, BDV replicated to comparable levels in the brains of mice of the various strains used. Intracerebral infections of newborn beta2-microglobulin-deficient C57BL/6 and MRL mice, which both lack CD8+ T cells, did not result in meningoencephalitis or neurological disease, indicating that the BDV-induced neurological disorder in mice is a cytotoxic T-cell-mediated immunopathological process. With this new animal model it should now be possible to characterize the disease-inducing immune response to BDV in more detail.

摘要

博尔纳病病毒(BDV)是一种嗜神经性非节段性负链RNA病毒,可长期感染温血动物。在马和其他天然动物宿主中,BDV感染会导致脑膜脑炎和行为障碍。成年小鼠的实验性感染过程无症状,此前人们认为这一观察结果表明该动物物种不适合用于发病机制研究。我们现在证明,BDV经常在受感染的新生小鼠中诱发严重的神经疾病。脑内感染后4至6周首次观察到神经疾病症状。这些症状包括疾病早期后肢特征性的非生理性姿势以及后期的轻瘫。组织学检查显示,患病小鼠大脑中有大量血管周围和脑膜炎症细胞,出乎意料的是,胶质纤维酸性蛋白的免疫反应性并未增加。BDV诱发疾病的发生率和严重程度在小鼠品系中差异很大。虽然只有13%的受感染C57BL/6小鼠出现疾病症状,且大多为短暂性症状,但超过80%的受感染MRL小鼠出现了严重的神经紊乱。尽管在疾病易感性方面存在这些差异,但BDV在所用各品系小鼠的大脑中复制到了相当的水平。对缺乏CD8 + T细胞的新生β2微球蛋白缺陷型C57BL/6和MRL小鼠进行脑内感染,并未导致脑膜脑炎或神经疾病,这表明小鼠中BDV诱发的神经紊乱是一种细胞毒性T细胞介导的免疫病理过程。有了这个新的动物模型,现在应该有可能更详细地描述对BDV的致病免疫反应。

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