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CD46在CD46转基因小鼠麻疹病毒感染中的作用

Role of CD46 in measles virus infection in CD46 transgenic mice.

作者信息

Blixenkrone-Møller M, Bernard A, Bencsik A, Sixt N, Diamond L E, Logan J S, Wild T F

机构信息

Immunité et Vaccination, Ex-Bâtiment Institut Pasteur de Lyon, Avenue Tony Garnier, Lyon Cedex 07, 69365, France.

出版信息

Virology. 1998 Sep 30;249(2):238-48. doi: 10.1006/viro.1998.9301.

Abstract

The susceptibility of CD46 (human membrane cofactor protein) transgenic mice to measles virus (MV) infection was investigated. Cell cultures (lung and kidney) established from transgenic and control mice showed that although both could be infected only those from the CD46+ mice gave fusion. A complete round of replication with the release of infectious virus was detected exclusively in the transgenic cell cultures whose permissiveness to MV was markedly less than that of Vero cells. The ability of MV to replicate in vivo in mice was studied using both vaccine and laboratory-adapted wild-type strains of virus. After intraperitoneal and intranasal inoculations of transgenic mice, virus replication could not be detected. In contrast intracerebral inoculation induced infection in both transgenic and nontransgenic mice. Our results from in vitro infection studies support the hypothesis that CD46 is a major host cell factor involved in the MV-induced fusion process and MV entry. The studies further indicate that MV tropism is not governed solely by the expression of the CD46 gene and that the high efficiency of the replicative cycles characteristic of fully permissive host cells requires additional factors, which are lacking in both transgenic and nontransgenic mice.

摘要

研究了CD46(人膜辅因子蛋白)转基因小鼠对麻疹病毒(MV)感染的易感性。从转基因小鼠和对照小鼠建立的细胞培养物(肺和肾)显示,虽然两者都能被感染,但只有来自CD46 +小鼠的细胞培养物出现融合。仅在对MV的易感性明显低于Vero细胞的转基因细胞培养物中检测到一轮完整的病毒复制并释放出感染性病毒。使用疫苗株和实验室适应的野生型病毒株研究了MV在小鼠体内的复制能力。对转基因小鼠进行腹腔内和鼻内接种后,未检测到病毒复制。相反,脑内接种在转基因和非转基因小鼠中均诱导感染。我们体外感染研究的结果支持以下假设:CD46是参与MV诱导的融合过程和MV进入的主要宿主细胞因子。研究进一步表明,MV的嗜性不仅仅由CD46基因的表达决定,完全允许的宿主细胞特征性的高效复制周期需要其他因素,而转基因和非转基因小鼠均缺乏这些因素。

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