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黄病毒是嗜神经性的,但它们如何入侵中枢神经系统?

Flaviviruses are neurotropic, but how do they invade the CNS?

机构信息

Institute of Infection and Immunity, Henry Wellcome Building, University Hospital of Wales, Cardiff University, Cardiff CF14 4XN, United Kingdom.

出版信息

J Infect. 2014 Sep;69(3):203-15. doi: 10.1016/j.jinf.2014.05.010. Epub 2014 May 29.

Abstract

Flaviruses (FV) are RNA viruses carried by mosquitoes. Neurological signs including acute encephalitis, meningitis and acute flaccid paralysis develop in a small percentage of infected individuals; long term sequlae are, Parkinsonism, dystonias and cognitive changes. FV neuroinfection is neurotropic involving subcortical nuclei (substantia nigra and thalamus) anterior horn neurons and neocortex. Glycosylation of the FV E envelope protein is one determinant of neuroinvasion, increasing both axonal and trans-epithelial transportation. Neutralizing antibodies against the E and NS proteins prevents FV uptake into several cell types, including axons. CD8+ T cells are vital for clearance of WNF infected cells from the CNS, whereas TLR-3 and TLR-7 mediated anti-virus response through increased serum inflammatory cytokines to disrupt the BBB providing infected leucocytes and free virus access to the CNS (so called Trojan horse) Cellular virus attachment factors, promoting FV cell entry are widely distributed and include DC-SIGN (that detects complex carbohydrate molecules); Glycosamino glycans (GAG), Heparan sulphate(HSPG) Semaphorin 7A, Low Density Lipid receptors (LDLR); these are not FV specific virus entry receptors. The FV also crosses epithelial and endothelial barriers by disrupting Tight Junction complexes to increase BBB permeability. This review describes the multiple pathways responsible for the neuroinvasive properties of the Flaviviruses.

摘要

黄病毒(FV)是由蚊子携带的 RNA 病毒。少数感染个体中会出现包括急性脑炎、脑膜炎和急性弛缓性麻痹在内的神经系统症状;长期后遗症为帕金森病、肌张力障碍和认知改变。FV 神经感染具有嗜神经性,涉及皮质下核(黑质和丘脑)、前角神经元和新皮质。FV E 包膜蛋白的糖基化是神经入侵的一个决定因素,增加了轴突和跨上皮运输。针对 E 和 NS 蛋白的中和抗体可防止 FV 进入包括轴突在内的几种细胞类型。CD8+T 细胞对于清除 WNF 感染的中枢神经系统细胞至关重要,而 TLR-3 和 TLR-7 通过增加血清炎症细胞因子来破坏血脑屏障,为感染的白细胞和游离病毒进入中枢神经系统提供途径(所谓的特洛伊木马),从而介导抗病毒反应。细胞病毒附着因子,促进 FV 细胞进入,广泛分布并包括 DC-SIGN(可检测复杂碳水化合物分子);糖胺聚糖(GAG)、硫酸乙酰肝素(HSPG)、Semaphorin 7A、低密度脂蛋白受体(LDLR);这些不是 FV 特异性的病毒进入受体。FV 还通过破坏紧密连接复合物增加血脑屏障通透性,穿过上皮和内皮屏障。本综述描述了黄病毒具有神经侵袭性的多种途径。

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