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首页> 外文期刊>Journal of neuroinflammation >Transcriptional profile and Epstein-Barr virus infection status of laser-cut immune infiltrates from the brain of patients with progressive multiple sclerosis
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Transcriptional profile and Epstein-Barr virus infection status of laser-cut immune infiltrates from the brain of patients with progressive multiple sclerosis

机译:进行性多发性硬化症患者大脑激光切割的免疫浸润液的转录特征和爱泼斯坦-巴尔病毒感染状况

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BackgroundIt is debated whether multiple sclerosis (MS) might result from an immunopathological response toward an active Epstein-Barr virus (EBV) infection brought into the central nervous system (CNS) by immigrating B cells. Based on this model, a relationship should exist between the local immune milieu and EBV infection status in the MS brain. To test this hypothesis, we analyzed expression of viral and cellular genes in brain-infiltrating immune cells. MethodsTwenty-three postmortem snap-frozen brain tissue blocks from 11 patients with progressive MS were selected based on good RNA quality and prominent immune cell infiltration. White matter perivascular and intrameningeal immune infiltrates, including B cell follicle-like structures, were isolated from brain sections using laser capture microdissection. Enhanced PCR-based methods were used to investigate expression of 75 immune-related genes and 6 EBV genes associated with latent and lytic infection. Data were analyzed using univariate and multivariate statistical methods. ResultsGenes related to T cell activation, cytotoxic cell-mediated (or type 1) immunity, B cell growth and differentiation, pathogen recognition, myeloid cell function, type I interferon pathway activation, and leukocyte recruitment were found expressed at different levels in most or all MS brain immune infiltrates. EBV genes were detected in brain samples from 9 of 11 MS patients with expression patterns suggestive of in situ activation of latent infection and, less frequently, entry into the lytic cycle. Comparison of data obtained in meningeal and white matter infiltrates revealed higher expression of genes related to interferonγ production, B cell differentiation, cell proliferation, lipid antigen presentation, and T cell and myeloid cell recruitment, as well as more widespread EBV infection in the meningeal samples. Multivariate analysis grouped genes expressed in meningeal and white matter immune infiltrates into artificial factors that were characterized primarily by genes involved in type 1 immunity effector mechanisms and type I interferon pathway activation. ConclusionThese results confirm profound in situ EBV deregulation and suggest orchestration of local antiviral function in the MS brain, lending support to a model of MS pathogenesis that involves EBV as possible antigenic stimulus of the persistent immune response in the central nervous system.
机译:背景争论是否多发性硬化症(MS)可能是由于对B细胞迁移引起的对中枢神经系统(CNS)引起的主动爱泼斯坦-巴尔病毒(EBV)感染的免疫病理反应所致。基于此模型,MS脑中的局部免疫环境与EBV感染状态之间应存在关系。为了验证这一假设,我们分析了在脑浸润性免疫细胞中病毒和细胞基因的表达。方法基于良好的RNA质量和明显的免疫细胞浸润,从11例进行性MS患者中选择了23例死后速冻脑组织块。使用激光捕获显微切割术从大脑切片中分离出包括B细胞滤泡样结构在内的白质血管周围和脑膜内免疫浸润物。基于增强PCR的方法用于研究与潜伏性和裂解性感染相关的75个免疫相关基因和6个EBV基因的表达。使用单变量和多变量统计方法分析数据。结果发现与T细胞活化,细胞毒性细胞介导的(或1型)免疫,B细胞生长和分化,病原体识别,髓样细胞功能,I型干扰素途径活化和白细胞募集有关的基因在大多数或全部中均以不同水平表达MS脑部免疫浸润。在11名MS患者中,有9名患者的大脑样本中检测到EBV基因,其表达模式暗示了潜在感染的原位活化,并且进入溶胞周期的频率较低。对脑膜和白质浸润液中获得的数据进行比较,发现与干扰素γ产生,B细胞分化,细胞增殖,脂质抗原呈递,T细胞和髓样细胞募集有关的基因表达更高,并且在脑膜样品中出现了更广泛的EBV感染。多变量分析将脑膜和白质免疫浸润中表达的基因分组为人工因子,其主要特征在于参与1型免疫效应机制和I型干扰素途径激活的基因。结论这些结果证实了原位EBV的深度失调,并提示了MS脑局部抗病毒功能的编排,这为MS发病机制模型提供了支持,该模型涉及EBV作为中枢神经系统持续免疫反应的可能抗原刺激。

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