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甲型肝炎病毒蛋白2B和2BC诱导的膜通透性以及甲型肝炎病毒2BC的蛋白水解加工

Membrane permeability induced by hepatitis A virus proteins 2B and 2BC and proteolytic processing of HAV 2BC.

作者信息

Jecht M, Probst C, Gauss-Müller V

机构信息

Institute for Medical Microbiology and Hygiene, Medical University of Lübeck, Germany.

出版信息

Virology. 1998 Dec 5;252(1):218-27. doi: 10.1006/viro.1998.9451.

Abstract

The ability to rearrange membranes is a unique feature of nonstructural proteins 2B, 2C, and 2BC of some picornaviruses. To analyze in detail membrane binding of the respective proteins of hepatitis A virus (HAV), they were transiently expressed in the vaccinia/T7 system, and their effect on membrane permeability was studied using beta-galactosidase as reporter. Although 2C had no effect, the significantly increased reporter activity observed in the extracellular space of 2B- and 2BC-expressing cells points to a specific effect of HAV proteins 2B and 2BC on membrane permeability. In biochemical fractionation studies, HAV 2C and 2BC showed properties of intregral membrane proteins, whereas 2B was associated with membranes as a peripheral protein. Proteinase 3C-mediated cleavage of precursor 2BC in vivo was most efficient when the enzyme was coexpressed in its precursor forms P3 or 3ABC, which both include the membrane-anchoring domain 3A. 3ABC showed the same solubility pattern as 2BC, suggesting that colocalization of 2BC and 3ABC might be required for the efficient liberation of 2B and 2C and occurs on membranes that have been proposed as the site of viral RNA replication.

摘要

重排膜的能力是一些小核糖核酸病毒非结构蛋白2B、2C和2BC的独特特征。为了详细分析甲型肝炎病毒(HAV)各蛋白与膜的结合情况,它们在痘苗/T7系统中瞬时表达,并以β-半乳糖苷酶作为报告基因研究它们对膜通透性的影响。尽管2C没有作用,但在表达2B和2BC的细胞胞外空间中观察到报告基因活性显著增加,这表明HAV蛋白2B和2BC对膜通透性有特定作用。在生化分级分离研究中,HAV 2C和2BC表现出整合膜蛋白的特性,而2B作为外周蛋白与膜相关。当蛋白酶3C以其前体形式P3或3ABC共表达时,体内3C介导的前体2BC的切割效率最高,P3和3ABC都包含膜锚定结构域3A。3ABC与2BC表现出相同的溶解模式,这表明2BC和3ABC的共定位可能是有效释放2B和2C所必需的,并且发生在被认为是病毒RNA复制位点的膜上。

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