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神经致病性弗氏鼠白血病病毒新变种的独特序列和病灶嗜性

Unique sequence and lesional tropism of a new variant of neuropathogenic friend murine leukemia virus.

作者信息

Takase-Yoden S, Watanabe R

机构信息

Institute of Life Science, Soka University, Hachioji, Tokyo, Japan.

出版信息

Virology. 1997 Jul 7;233(2):411-22. doi: 10.1006/viro.1997.8619.

Abstract

FrC6 murine leukemia virus (MuLV) is a replication-competent, neuropathogenic variant derived from Friend MuLV (F-MuLV) complex. The A8 virus (a molecular clone of the FrC6 virus) induced marked spongiform degeneration in the brain similar to the FrC6 virus, but only mild lesions were found in the spinal cord. In contrast, PVC211 virus, which is also a neuropathogenic F-MuLV variant, caused marked spongiform degeneration in the spinal cord. Virus recovery from the spinal cord of A8 virus-infected rat was the same as that of PVC211-infected rat, indicating that there is no direct correlation between the titer of virus and the intensity of lesions. Furthermore, rats infected with the A8 virus at 3 weeks of age did not undergo spongiform degeneration, although recovery of high titer of virus occurred in the central nervous system (CNS). Studies using chimeric viruses between the A8 virus and nonneuropathogenic F-MuLV clone 57 also indicated that the sequences responsible for virus titers in the CNS and neuropathogenicity are different. The chimeric virus studies proved that the env gene and the LTR and/or 5' leader sequence of A8 are critical for the induction of neuropathogenicity. These sequences in A8 and PVC211 were compared, focusing in on the sites that account for neurovirulence and viral lesional tropism.

摘要

FrC6小鼠白血病病毒(MuLV)是一种具有复制能力的神经致病性变异株,源自Friend MuLV(F-MuLV)复合体。A8病毒(FrC6病毒的分子克隆)在脑中诱导出明显的海绵状变性,类似于FrC6病毒,但在脊髓中仅发现轻度病变。相比之下,同样是神经致病性F-MuLV变异株的PVC211病毒,在脊髓中引起明显的海绵状变性。从感染A8病毒的大鼠脊髓中回收的病毒与感染PVC211病毒的大鼠相同,这表明病毒滴度与病变强度之间没有直接相关性。此外,3周龄感染A8病毒的大鼠未发生海绵状变性,尽管在中枢神经系统(CNS)中出现了高滴度病毒的回收。使用A8病毒与非神经致病性F-MuLV克隆57之间的嵌合病毒进行的研究还表明,负责中枢神经系统中病毒滴度和神经致病性的序列是不同的。嵌合病毒研究证明,A8的env基因以及LTR和/或5'前导序列对于神经致病性的诱导至关重要。对A8和PVC211中的这些序列进行了比较,重点关注了导致神经毒力和病毒损伤嗜性的位点。

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