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Neurotoxic potential of reactive astrocytes in canine distemper demyelinating leukoencephalitis

机译:犬瘟热脱髓鞘白细胞炎的活性星形胶质细胞的神经毒性潜力

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Canine distemper virus (CDV) causes a fatal demyelinating leukoencephalitis in young dogs resembling human multiple sclerosis. Astrocytes are the main cellular target of CDV and undergo reactive changes already in pre-demyelinating brain lesions. Based on their broad range of beneficial and detrimental effects in the injured brain reactive astrogliosis is in need of intensive investigation. The aim of the study was to characterize astrocyte plasticity during the course of CDV-induced demyelinating leukoencephalitis by the aid of immunohistochemistry, immunofluorescence and gene expression analysis. Immunohistochemistry revealed the presence of reactive glial fibrillary acidic protein (GFAP)sup+/sup astrocytes with increased survivin and reduced aquaporin 4, and glutamine synthetase protein levels, indicating disturbed blood brain barrier function, glutamate homeostasis and astrocyte maladaptation, respectively. Gene expression analysis revealed 81 differentially expressed astrocyte-related genes with a dominance of genes associated with neurotoxic A1-polarized astrocytes. Accordingly, acyl-coA synthetase long-chain family member 5sup+/sup/GFAPsup+/sup, and serglycinsup+/sup/GFAPsup+/sup cells, characteristic of A1-astrocytes, were found in demyelinating lesions by immunofluorescence. In addition, gene expression revealed a dysregulation of astrocytic function including disturbed glutamate homeostasis and altered immune function. Observed findings indicate an astrocyte polarization towards a neurotoxic phenotype likely contributing to lesion initiation and progression in canine distemper leukoencephalitis.
机译:犬瘟热病毒(CDV)导致类似人类多发性硬化症的幼犬致命的脱髓鞘白细胞炎。星形胶质细胞是CDV的主要细胞靶标,并且已经在预脱髓鞘脑病变中经历了反应性变化。基于其在受伤的脑反应十分术中的广泛的有益和不利影响,需要强化调查。该研究的目的是通过免疫组织化学,免疫荧光和基因表达分析来表征CDV诱导的脱髓鞘性白细胞炎的星形细胞塑性。免疫组织化学揭示了活性胶质纤维酸性蛋白(GFAP) + 星形胶质细胞,随着Survivin增加和降低的水素4,以及谷氨酰胺合成酶蛋白水平,表明血脑屏障功能紊乱,谷氨酸稳态和星形胶质细胞不良治疗。基因表达分析揭示了81种差异表达的星形胶质细胞相关基因,其主要是与神经毒性A1-偏振星形细胞相关的基因的主导。因此,酰基-CoA合成酶长链家族构件5 + / gfap + ,以及血糖素 + / sup> / gfap + 通过免疫荧光在脱髓鞘病变中发现了A1-星形胶质细胞的特征。此外,基因表达揭示了星形胶质细胞功能的缺点,包括令人不安的谷氨酸稳态和改变的免疫功能。观察结果表明,对于神经毒性表型的星形胶质细胞极化可能导致病变引发和犬瘟热的白细胞炎的进展。

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