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疫苗株与野生型腮腺炎病毒株在发育中大鼠脑内的神经毒力比较。

Comparison of the neurovirulence of a vaccine and a wild-type mumps virus strain in the developing rat brain.

作者信息

Rubin S A, Pletnikov M, Carbone K M

机构信息

DVP/OVRR, Center for Biologics Evaluation and Research, Food and Drug Administration, Bethesda, Maryland 20892, USA.

出版信息

J Virol. 1998 Oct;72(10):8037-42. doi: 10.1128/JVI.72.10.8037-8042.1998.

Abstract

Prior to the adoption of widespread vaccination programs, mumps virus was the leading cause of virus-induced central nervous system (CNS) disease. Mumps virus-associated CNS complications in vaccinees continue to be reported; outside the United States, some of these complications have been attributed to vaccination with insufficiently attenuated neurovirulent vaccine strains. The development of potentially neurovirulent, live, attenuated mumps virus vaccines stems largely from the lack of an animal model that can reliably predict the neurovirulence of mumps virus vaccine candidates in humans. The lack of an effective safety test with which to measure mumps virus neurovirulence has also hindered analysis of the neuropathogenesis of mumps virus infection and the identification of molecular determinants of neurovirulence. In this report we show, for the first time, that mumps virus infection of the neonatal rat leads to developmental abnormalities in the cerebellum due to cerebellar granule cell migration defects. The incidence of the cerebellar abnormalities and other neuropathological and clinical outcomes of mumps virus infection of the neonatal rat brain demonstrated the ability of this model to distinguish neurovirulent (Kilham) from nonneurovirulent (Jeryl Lynn) mumps virus strains. Thus, this neonatal rat model may prove useful in evaluating the neurovirulence potential of new live, attenuated vaccine strains and may also be of value in elucidating the molecular basis of mumps virus neurovirulence.

摘要

在广泛接种疫苗计划实施之前,腮腺炎病毒是病毒引起的中枢神经系统(CNS)疾病的主要病因。疫苗接种者中与腮腺炎病毒相关的中枢神经系统并发症仍有报道;在美国以外的地区,其中一些并发症被归因于接种了减毒不足的神经毒力疫苗株。具有潜在神经毒力的减毒活腮腺炎病毒疫苗的研发很大程度上源于缺乏一种能够可靠预测腮腺炎病毒候选疫苗在人类中神经毒力的动物模型。缺乏一种有效的安全测试来衡量腮腺炎病毒的神经毒力也阻碍了对腮腺炎病毒感染神经发病机制的分析以及神经毒力分子决定因素的鉴定。在本报告中,我们首次表明,新生大鼠感染腮腺炎病毒会因小脑颗粒细胞迁移缺陷导致小脑发育异常。新生大鼠脑部感染腮腺炎病毒后小脑异常以及其他神经病理学和临床结果的发生率表明,该模型能够区分神经毒力(基尔汉姆株)和非神经毒力(杰里尔·林恩株)的腮腺炎病毒株。因此,这种新生大鼠模型可能在评估新的减毒活疫苗株的神经毒力潜力方面有用,也可能在阐明腮腺炎病毒神经毒力的分子基础方面具有价值。

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