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仓鼠多瘤病毒的衣壳蛋白编码基因及病毒衣壳的特性

Capsid protein-encoding genes of hamster polyomavirus and properties of the viral capsid.

作者信息

Siray H, Ozel M, Jandrig B, Voronkova T, Jia W, Zocher R, Arnold W, Scherneck S, Krüger D H, Ulrich R

机构信息

Institute of Virology, Charité Medical School, Humboldt University, Berlin, Germany.

出版信息

Virus Genes. 1999;18(1):39-47. doi: 10.1023/a:1008017201999.

Abstract

On the basis of its genome organization the hamster polyomavirus (HaPV) is closely related to the murine polyomavirus Py. But HaPV infection, in contrast to Py infection, gives rise to two different tumor types; depending on the hamster strain used for infection, HaPV induces either epitheliomas or lymphomas. Although the HaPV virions were shown to be similar to those of Py and SV40, more precise information about the structure and protein composition of the HaPV capsid was still missing. Here we describe the primary structure of the capsid protein-encoding HaPV genes and the structure and protein composition of the HaPV capsid. Virions isolated from epitheliomas in HaPV-infected hamsters were shown by electron microscopy to be spherical particles with the typical icosahedral structure of polyomaviruses. However, in contrast to the capsids of SV40 and Py, a T = 7 laevo symmetry of HaPV capsids was observed. Separation of HaPV virions in SDS polyacrylamide gels and Western blotting with VP1-specific antisera identified VP1 as the major capsid protein species corresponding in its molecular weight to the predicted value of 41.8 kDa. Because of the presence of two potential translational initiation sites in the VP1 gene, the N-terminal amino acid sequence of virion VP1 was determined and found to start at the second initiation site. The amino acid homologies of HaPV capsid proteins shared with Py varied between 65.5% (VP1), 45.4% (VP3) and 44.6% (VP2), whereas the homologies to the relevant proteins of other polyomaviruses were found to range between 49.6-57.9% for VP1 and 28.9-41% for VP2/VP3.

摘要

基于其基因组结构,仓鼠多瘤病毒(HaPV)与小鼠多瘤病毒Py密切相关。但与Py感染不同,HaPV感染会引发两种不同的肿瘤类型;根据用于感染的仓鼠品系不同,HaPV可诱发上皮瘤或淋巴瘤。尽管已证明HaPV病毒粒子与Py和SV40的病毒粒子相似,但关于HaPV衣壳的结构和蛋白质组成的更精确信息仍然缺失。在此,我们描述了编码衣壳蛋白的HaPV基因的一级结构以及HaPV衣壳的结构和蛋白质组成。通过电子显微镜观察发现,从感染HaPV的仓鼠上皮瘤中分离出的病毒粒子是具有多瘤病毒典型二十面体结构的球形颗粒。然而,与SV40和Py的衣壳不同,观察到HaPV衣壳具有T = 7左旋对称性。在SDS聚丙烯酰胺凝胶中分离HaPV病毒粒子并用VP1特异性抗血清进行蛋白质印迹分析,确定VP1为主要衣壳蛋白种类,其分子量与预测值41.8 kDa相符。由于VP1基因中存在两个潜在的翻译起始位点,因此确定了病毒粒子VP1的N端氨基酸序列,并发现其从第二个起始位点开始。HaPV衣壳蛋白与Py的氨基酸同源性在65.5%(VP1)、45.4%(VP3)和44.6%(VP2)之间变化,而与其他多瘤病毒相关蛋白的同源性对于VP1为49.6 - 57.9%,对于VP2/VP3为28.9 - 41%。

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