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重组蜱传脑炎病毒E蛋白以可溶性和颗粒性形式的合成与分泌。

Synthesis and secretion of recombinant tick-borne encephalitis virus protein E in soluble and particulate form.

作者信息

Allison S L, Stadler K, Mandl C W, Kunz C, Heinz F X

机构信息

Institute of Virology, University of Vienna, Austria.

出版信息

J Virol. 1995 Sep;69(9):5816-20. doi: 10.1128/JVI.69.9.5816-5820.1995.

Abstract

A quantitative study was performed to investigate the requirements for secretion of recombinant soluble and particulate forms of the envelope glycoprotein E of tick-borne encephalitis (TBE) virus. Full-length E and a carboxy terminally truncated anchor-free form were expressed in COS cells in the presence and absence of prM, the precursor of the viral membrane protein M. Formation of a heteromeric complex with prM was found to be necessary for efficient secretion of both forms of E, whereas only low levels of anchor-free E were secreted in the absence of prM. The prM-mediated transport function could also be provided by coexpression of prM and E from separate constructs, but a prM-to-E ratio of greater than 1:1 did not further enhance secretion. Full-length E formed stable intracellular heterodimers with prM and was secreted as a subviral particle, whereas anchor-free E was not associated with particles and formed a less stable complex with prM, suggesting that prM interacts with both the ectodomain and anchor region of E.

摘要

进行了一项定量研究,以调查蜱传脑炎(TBE)病毒包膜糖蛋白E的重组可溶性和颗粒形式分泌的要求。在存在和不存在病毒膜蛋白M的前体prM的情况下,在COS细胞中表达全长E和羧基末端截短的无锚定形式。发现与prM形成异源复合物对于两种形式的E的有效分泌是必要的,而在不存在prM的情况下仅分泌低水平的无锚定E。prM介导的转运功能也可以通过从单独的构建体中共表达prM和E来提供,但prM与E的比例大于1:1并不会进一步增强分泌。全长E与prM形成稳定的细胞内异二聚体,并作为亚病毒颗粒分泌,而无锚定E不与颗粒相关,并与prM形成不太稳定的复合物,这表明prM与E的胞外域和锚定区域都相互作用。

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