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关于EB病毒包膜及病毒决定膜抗原(MA)多肽的观察

Observations on the EB virus envelope and virus-determined membrane antigen (MA) polypeptides.

作者信息

North J R, Morgan A J, Epstein M A

出版信息

Int J Cancer. 1980 Aug;26(2):231-40. doi: 10.1002/ijc.2910260216.

Abstract

Experiments have been carried out to identify the polypeptide components of the Epstein-Barr (EB) virus-determined membrane antigen (MA) complex. Cells were radioiodinated using lactoperoxidase and the 125I-labelled surface antigens, released by Triton X100, were analysed by sodium dodecyl sulphate polyacrylamide gel electrophoresis (SDS-PAGE) after complexing either with human sera having anti-MA activity or with a rabbit antiserum to EB virus. Using cells carrying EB virus isolated from four different conditions, including for the first time nasopharyngeal carcinoma (NPC), we have demonstrated four major polypeptides. One, with a molecular weight of 85,000, was remarkedly constant irrespective of the cell line from which it came; two, with molecular weights varying from 240,000 to 270,000 and from 320,000 to 340,000, showed minor differences in mobility apparently depending on the species of origin of the cells (human or marmoset), rather than disparity between strains of virus. A fourth component, of 160,000 daltons, was found on only two of the cell lines studied. In addition, it has been shown for the first time that the same polypeptides composing the MA complex are present on the viral envelope itself. The fact that the rabbit antiserum to EV virus recognized only the two highest molecular weight MA components, yet showed virus-neutralizing activity, indicates the importance of these two polypeptides for use in a vaccine designed to induce virus-neutralizing antibodies.

摘要

已开展实验以鉴定爱泼斯坦-巴尔(EB)病毒决定的膜抗原(MA)复合物的多肽成分。使用乳过氧化物酶对细胞进行放射性碘化,经Triton X100释放的125I标记表面抗原,在与具有抗MA活性的人血清或兔抗EB病毒血清复合后,通过十二烷基硫酸钠聚丙烯酰胺凝胶电泳(SDS-PAGE)进行分析。利用从四种不同条件下分离出EB病毒的细胞,包括首次使用的鼻咽癌(NPC)细胞,我们已证实有四种主要多肽。一种分子量为85,000,无论其来源的细胞系如何,该多肽都显著恒定;另外两种分子量分别在240,000至270,000以及320,000至340,000之间,其迁移率存在细微差异,这显然取决于细胞的来源物种(人或狨猴),而非病毒株之间的差异。在仅研究的两种细胞系中发现了第四种分子量为160,000道尔顿的成分。此外,首次表明构成MA复合物的相同多肽也存在于病毒包膜本身。兔抗EB病毒血清仅识别两种分子量最高的MA成分,但却显示出病毒中和活性,这一事实表明这两种多肽对于用于诱导病毒中和抗体的疫苗很重要。

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