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中枢神经系统细胞群体受到免疫系统不同分支的保护,免受病毒诱导的病理损害。

CNS cell populations are protected from virus-induced pathology by distinct arms of the immune system.

作者信息

Drescher K M, Murray P D, David C S, Pease L R, Rodriguez M

机构信息

Department of Immunology, Mayo Medical School, Rochester, MN 55901, USA.

出版信息

Brain Pathol. 1999 Jan;9(1):21-31. doi: 10.1111/j.1750-3639.1999.tb00206.x.

Abstract

The basis for the distinct patterns of brain pathology in individuals experiencing virus-induced encephalitis may be related to either the tropism of the virus or the host's response to virus infection of the central nervous system (CNS). In these studies we used Theiler's murine encephalomyelitis virus (TMEV) and a series of mice deficient in various immune system components (alpha/beta T cells, antibody, Class I MHC, and Class II MHC) to examine the hypothesis that discrete populations of CNS cells are protected differentially from virus infection by distinct arms of the immune response. Here we demonstrate that the Class I-mediated immune response provided more protection from areas of the brain (brainstem, corpus callosum and cerebellum) with abundant white matter as there was significantly more disease in these areas in beta2m -/- (Class I-deficient) mice as compared to A beta(0) (Class II-deficient) mice. In contrast, the striatum, with an abundance of neurons, was protected from virus-induced pathology primarily by antibody. In addition, we determined that antibody and alpha/beta T cells provided protection from severe deficits and death during the acute phase of the disease. The data presented here support the hypothesis that distinct immune system components function to protect discrete areas of the CNS from virus-induced pathology.

摘要

个体在经历病毒诱导的脑炎时出现不同脑病理模式的基础,可能与病毒的嗜性或宿主对中枢神经系统(CNS)病毒感染的反应有关。在这些研究中,我们使用了泰勒氏鼠脑脊髓炎病毒(TMEV)和一系列缺乏各种免疫系统成分(α/β T细胞、抗体、I类主要组织相容性复合体和II类主要组织相容性复合体)的小鼠,来检验这一假设:中枢神经系统细胞的不同群体受到免疫反应不同分支对病毒感染的差异性保护。在此我们证明,I类介导的免疫反应对脑内白质丰富的区域(脑干、胼胝体和小脑)提供了更多保护,因为与Aβ(0)(II类缺陷)小鼠相比,β2m -/-(I类缺陷)小鼠在这些区域的疾病明显更多。相反,富含神经元的纹状体主要通过抗体免受病毒诱导的病理损害。此外,我们确定抗体和α/β T细胞在疾病急性期提供了保护,防止严重缺陷和死亡。此处呈现的数据支持这一假设:不同的免疫系统成分发挥作用,保护中枢神经系统的不同区域免受病毒诱导的病理损害。

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