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伪狂犬病病毒UL36衣壳蛋白与UL37蛋白存在物理相互作用。

Pseudorabies virus UL36 tegument protein physically interacts with the UL37 protein.

作者信息

Klupp Barbara G, Fuchs Walter, Granzow Harald, Nixdorf Ralf, Mettenleiter Thomas C

机构信息

Institute of Molecular Biology, Friedrich-Loeffler-Institutes, Federal Research Centre for Virus Diseases of Animals, D-17498 Insel Riems, Germany.

出版信息

J Virol. 2002 Mar;76(6):3065-71. doi: 10.1128/jvi.76.6.3065-3071.2002.

Abstract

The UL36 open reading frame encoding the tegument protein ICP1/2 represents the largest open reading frame in the genome of herpes simplex virus type 1 (HSV-1). Polypeptides homologous to the HSV-1 UL36 protein are present in all subfamilies of HERPESVIRIDAE: We sequenced the UL36 gene of the alphaherpesvirus pseudorabies virus (PrV) and prepared a monospecific polyclonal rabbit antiserum against a bacterial glutathione S-transferase (GST)-UL36 fusion protein for identification of the protein. The antiserum detected a >300-kDa protein in PrV-infected cells and in purified virions. Interestingly, in coprecipitation analyses using radiolabeled infected-cell extracts, the anti-UL36 serum reproducibly coprecipitated the UL37 tegument protein, and antiserum directed against the UL37 protein coprecipitated the UL36 protein. This physical interaction could be verified using yeast two-hybrid analysis which demonstrated that the UL37 protein interacts with a defined region within the amino-terminal part of the UL36 protein. By use of immunogold labeling, capsids which accumulate in the cytoplasm in the absence of the UL37 protein (B. G. Klupp, H. Granzow, E. Mundt, and T. C. Mettenleiter, J. Virol. 75:8927-8936, 2001) as well as wild-type intracytoplasmic and extracellular virions were decorated by the anti-UL36 antiserum, whereas perinuclear primary enveloped virions were not. We postulate that the physical interaction of the UL36 protein, which presumably constitutes the innermost layer of the tegument (Z. Zhou, D. Chen, J. Jakana, F. J. Rixon, and W. Chiu, J. Virol. 73:3210-3218, 1999), with the UL37 protein is an important early step in tegumentation during virion morphogenesis in the cytoplasm.

摘要

编码被膜蛋白ICP1/2的UL36开放阅读框是单纯疱疹病毒1型(HSV-1)基因组中最大的开放阅读框。与HSV-1 UL36蛋白同源的多肽存在于疱疹病毒科的所有亚科中:我们对甲型疱疹病毒伪狂犬病病毒(PrV)的UL36基因进行了测序,并制备了一种针对细菌谷胱甘肽S-转移酶(GST)-UL36融合蛋白的单特异性多克隆兔抗血清,用于该蛋白的鉴定。该抗血清在PrV感染的细胞和纯化的病毒粒子中检测到一种分子量大于300 kDa的蛋白。有趣的是,在使用放射性标记的感染细胞提取物进行的共沉淀分析中,抗UL36血清可重复性地共沉淀出UL37被膜蛋白,而针对UL37蛋白的抗血清则共沉淀出UL36蛋白。这种物理相互作用可以通过酵母双杂交分析得到证实,该分析表明UL37蛋白与UL36蛋白氨基末端部分的一个特定区域相互作用。通过免疫金标记,在缺乏UL37蛋白时积聚在细胞质中的衣壳(B.G.Klupp、H.Granzow、E.Mundt和T.C.Mettenleiter,《病毒学杂志》75:8927-8936,2001年)以及野生型胞质内和胞外病毒粒子都被抗UL36抗血清标记,而核周初级包膜病毒粒子则没有。我们推测,可能构成被膜最内层的UL36蛋白与UL37蛋白的物理相互作用是细胞质中病毒粒子形态发生过程中被膜形成的一个重要早期步骤。

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