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鉴定小神经胶质细胞上日本脑炎病毒假定受体分子。

Characterization of putative Japanese encephalitis virus receptor molecules on microglial cells.

机构信息

Department of Biochemistry, Chulalongkorn University, Bangkok, Thailand.

出版信息

J Med Virol. 2012 Apr;84(4):615-23. doi: 10.1002/jmv.23248.

DOI:10.1002/jmv.23248
PMID:22337301
Abstract

Japanese encephalitis virus (JEV) a mosquito-borne flavivirus is a major cause of viral encephalitis in Asia. While the principle target cells for JEV in the central nervous system are believed to be neurons, microglia are activated in response to JEV and have been proposed to act as a long lasting virus reservoir. Viral attachment to a host cell is the first step of the viral entry process and is a critical mediator of tissue tropism. This study sought to identify molecules associated with JEV entry to microglial cells. Virus overlay protein-binding assay (VOPBA) and liquid chromatography-mass spectrometry (LC/MS/MS) identified the 37/67 kDa high-affinity laminin receptor protein and nucleolin as a potential JEV-binding proteins. These proteins were subsequently investigated for a contribution to JEV entry to mouse microglial BV-2 cells together with other possible candidate receptor molecules including Hsp70, Hsp90, GRP78, CD14, and CD4. In antibody mediated inhibition of infection experiments, both anti-laminin receptor and anti-CD4 antibodies significantly reduced virus entry while anti-Hsp70 and 90 antibodies produced a slight reduction. Significant inhibition of virus entry (up to 80%) was observed in the presence of lipopolysaccharide (LPS) which resulted in a complete down-regulation of CD4 and moderate down-regulation of CD14. These results suggest that multiple receptor proteins may mediate the entry of JEV to microglial cells, with CD4 playing a major role.

摘要

日本脑炎病毒(JEV)是一种通过蚊子传播的黄病毒,是亚洲病毒性脑炎的主要病因。虽然 JEV 在中枢神经系统中的主要靶细胞被认为是神经元,但小胶质细胞在 JEV 反应中被激活,并被提议作为持久的病毒储库。病毒附着到宿主细胞是病毒进入过程的第一步,是组织嗜性的关键介质。本研究旨在鉴定与 JEV 进入小胶质细胞相关的分子。病毒覆盖蛋白结合测定(VOPBA)和液相色谱-质谱联用(LC/MS/MS)鉴定了 37/67 kDa 高亲和力层粘连蛋白受体蛋白和核仁素作为潜在的 JEV 结合蛋白。随后,研究了这些蛋白质在 JEV 进入小鼠小胶质细胞 BV-2 细胞中的作用,以及其他可能的候选受体分子,包括 Hsp70、Hsp90、GRP78、CD14 和 CD4。在抗体介导的感染抑制实验中,抗层粘连蛋白受体和抗 CD4 抗体均显著降低了病毒进入,而抗 Hsp70 和 Hsp90 抗体仅产生轻微降低。在脂多糖(LPS)存在下观察到病毒进入的显著抑制(高达 80%),导致 CD4 完全下调和 CD14 中度下调。这些结果表明,多种受体蛋白可能介导 JEV 进入小胶质细胞,其中 CD4 起主要作用。

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