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Transcriptional Changes in Canine Distemper Virus-Induced Demyelinating Leukoencephalitis Favor a Biphasic Mode of Demyelination

机译:犬瘟热病毒引起的脱髓鞘性白质脑炎的转录变化有利于双相脱髓鞘模式。

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摘要

Canine distemper virus (CDV)-induced demyelinating leukoencephalitis in dogs (Canis familiaris) is suggested to represent a naturally occurring translational model for subacute sclerosing panencephalitis and multiple sclerosis in humans. The aim of this study was a hypothesis-free microarray analysis of the transcriptional changes within cerebellar specimens of five cases of acute, six cases of subacute demyelinating, and three cases of chronic demyelinating and inflammatory CDV leukoencephalitis as compared to twelve non-infected control dogs. Frozen cerebellar specimens were used for analysis of histopathological changes including demyelination, transcriptional changes employing microarrays, and presence of CDV nucleoprotein RNA and protein using microarrays, RT-qPCR and immunohistochemistry. Microarray analysis revealed 780 differentially expressed probe sets. The dominating change was an up-regulation of genes related to the innate and the humoral immune response, and less distinct the cytotoxic T-cell-mediated immune response in all subtypes of CDV leukoencephalitis as compared to controls. Multiple myelin genes including myelin basic protein and proteolipid protein displayed a selective down-regulation in subacute CDV leukoencephalitis, suggestive of an oligodendrocyte dystrophy. In contrast, a marked up-regulation of multiple immunoglobulin-like expressed sequence tags and the delta polypeptide of the CD3 antigen was observed in chronic CDV leukoencephalitis, in agreement with the hypothesis of an immune-mediated demyelination in the late inflammatory phase of the disease. Analysis of pathways intimately linked to demyelination as determined by morphometry employing correlation-based Gene Set Enrichment Analysis highlighted the pathomechanistic importance of up-regulated genes comprised by the gene ontology terms “viral replication” and “humoral immune response” as well as down-regulated genes functionally related to “metabolite and energy generation”.
机译:犬瘟热病毒(CDV)引起的犬脱髓鞘性白质脑炎(Canis熟悉)被建议代表人类亚急性硬化性全脑炎和多发性硬化症的自然转化模型。这项研究的目的是与12只未感染的对照犬相比,对5例急性,6例亚急性脱髓鞘和3例慢性脱髓鞘和炎性CDV白质脑炎小脑标本中的转录变化进行无假设的微阵列分析。 。冷冻的小脑标本用于分析组织病理学变化,包括脱髓鞘,使用微阵列的转录变化以及使用微阵列,RT-qPCR和免疫组化的CDV核蛋白RNA和蛋白质的存在。微阵列分析揭示了780个差异表达的探针组。主要变化是与先天和体液免疫反应有关的基因上调,与对照组相比,在所有亚型CDV白质脑炎中,细胞毒性T细胞介导的免疫反应的区别较小。多种髓鞘基因,包括髓鞘碱性蛋白和蛋白脂蛋白,在亚急性CDV白脑炎中表现出选择性下调,提示少突胶质细胞营养不良。相反,在慢性CDV白质脑炎中观察到多个免疫球蛋白样表达的序列标签和CD3抗原的δ多肽显着上调,这与该疾病晚期炎症阶段免疫介导的脱髓鞘的假设相符。 。使用基于相关的基因集富集分析,通过形态计量学确定与脱髓鞘密切相关的途径,强调了由基因本体术语“病毒复制”和“体液免疫反应”以及下调构成的上调基因的病理机制重要性在功能上与“代谢物和能量产生”有关的基因。

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