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爱泼斯坦-巴尔病毒的BHRF1与人类原癌基因bcl2同源,对B细胞的转化或体外病毒复制并非必不可少。

BHRF1 of Epstein-Barr virus, which is homologous to human proto-oncogene bcl2, is not essential for transformation of B cells or for virus replication in vitro.

作者信息

Lee M A, Yates J L

机构信息

Department of Human Genetics, Roswell Park Cancer Institute, Buffalo, New York 14263.

出版信息

J Virol. 1992 Apr;66(4):1899-906. doi: 10.1128/JVI.66.4.1899-1906.1992.

Abstract

The Epstein-Barr virus (EBV) genome contains an open reading frame, BHRF1, that encodes a presumptive membrane protein with sequence similarity to the proto-oncogene bcl2, which is linked to human B-cell follicular lymphoma. Potential roles for BHRF1 in EBV's ability to growth transform human B cells and to replicate in B cells in culture were investigated by generating EBV mutants that lack most of the open reading frame. This was accomplished by recombination of plasmids carrying mutations in BHRF1 with the transformation-defective EBV strain P3HR1. Because BHRF1 resides close to the deletion in P3HR1 that renders this strain transformation defective, B-cell transformation could be used to select for recombination events in the region. B-cell clones were established by recombinants which lacked most of the BHRF1 open reading frame, although most of these initial B-cell transformants also carried nonrecombinant (BHRF1+) P3HR1 genomes, at levels ranging from a fraction of a copy to four copies per cell. Secondary B-cell transformants that lacked BHRF1+ EBV at detectable levels were found to release transforming, BHRF1-deficient EBV at levels that were within the normal range for EBV-immortalized B-cell clones. These studies demonstrate that BHRF1 is nonessential for growth transformation of B cells and for virus replication and release from these cells in culture.

摘要

爱泼斯坦-巴尔病毒(EBV)基因组包含一个开放阅读框BHRF1,它编码一种推测的膜蛋白,该蛋白与原癌基因bcl2在序列上具有相似性,而bcl2与人类B细胞滤泡性淋巴瘤有关。通过产生缺失大部分开放阅读框的EBV突变体,研究了BHRF1在EBV生长转化人类B细胞以及在培养的B细胞中复制能力方面的潜在作用。这是通过将携带BHRF1突变的质粒与转化缺陷型EBV毒株P3HR1进行重组来实现的。由于BHRF1位于P3HR1中导致该毒株转化缺陷的缺失区域附近,因此可以利用B细胞转化来选择该区域的重组事件。通过缺乏大部分BHRF1开放阅读框的重组体建立了B细胞克隆,尽管这些最初的B细胞转化体中的大多数还携带非重组(BHRF1+)P3HR1基因组,每个细胞中的拷贝数从一小部分到四个拷贝不等。发现缺乏可检测水平的BHRF1+ EBV的第二代B细胞转化体释放出具有转化能力、缺乏BHRF1的EBV,其水平在EBV永生化B细胞克隆的正常范围内。这些研究表明,BHRF1对于B细胞的生长转化以及病毒在培养细胞中的复制和释放并非必需。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cb82/288977/f5bbd3a2c61e/jvirol00166-0088-a.jpg

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