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逆行轴突运输:肠道病毒71型在小鼠中的主要传播途径。

Retrograde axonal transport: a major transmission route of enterovirus 71 in mice.

作者信息

Chen Che-Szu, Yao Yi-Chuan, Lin Shin-Chao, Lee Yi-Ping, Wang Ya-Fang, Wang Jen-Ren, Liu Ching-Chuan, Lei Huan-Yao, Yu Chun-Keung

机构信息

Department of Microbiology and Immunology, College of Medicine, National Cheng Kung University, Tainan, Taiwan 70101, Republic of China.

出版信息

J Virol. 2007 Sep;81(17):8996-9003. doi: 10.1128/JVI.00236-07. Epub 2007 Jun 13.

Abstract

Inoculation of enterovirus 71 (EV71) by the oral (p.o.), intramuscular (i.m.), or intracranial route resulted in brain infection, flaccid paralysis, pulmonary dysfunction, and death of 7-day-old mice. The lag time of disease progression indicated that neuroinvasion from the inoculation sites was a prerequisite for the development of the clinical signs. Although EV71 p.o. inoculation led to a persistent viremia and a transient increase in blood-brain barrier permeability at the early stage of the infection, only low levels of virus, which led to neither severe infection nor clinical illness, could be detected in the brain, suggesting that hematogenous transport might not represent a major transmission route. In the spinal cord, following both p.o. and hind limb i.m. inoculation, the virus first appeared and increased rapidly in the lower segments, especially at the anterior horn areas, and then spread to the upper segments and brain in the presence of viremia. A reverse pattern, with the virus being first detected in the upper segment, was observed when the virus was i.m. inoculated in the forelimb. Colchicine, a fast axonal transport inhibitor, but not sciatic nerve transection reduced EV71 neuroinvasion in a dose-dependent manner, indicating a neuronal transmission of the virus.

摘要

通过口服(p.o.)、肌肉注射(i.m.)或颅内途径接种肠道病毒71型(EV71)可导致7日龄小鼠发生脑感染、弛缓性麻痹、肺功能障碍及死亡。疾病进展的延迟时间表明,从接种部位发生神经侵袭是出现临床症状的先决条件。尽管口服EV71接种在感染早期导致持续性病毒血症及血脑屏障通透性短暂增加,但在脑中仅能检测到低水平病毒,既未导致严重感染也未引发临床疾病,这表明血行传播可能并非主要传播途径。在脊髓中,口服接种及后肢肌肉注射接种后,病毒首先出现在下段,尤其是前角区域,并迅速增多,然后在病毒血症存在的情况下扩散至上段及脑部。当在前肢进行肌肉注射接种病毒时,观察到相反模式,即病毒首先在上段被检测到。秋水仙碱是一种快速轴突运输抑制剂,而非坐骨神经横断术,以剂量依赖方式降低了EV71神经侵袭,表明病毒存在神经元传播。

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