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Human neonatal lymphocytes immortalized after microinjection of Epstein-Barr virus DNA.

机译:在对Epstein-Barr病毒DNA的微注射后,人新生儿淋巴细胞永生化。

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Epstein-Barr virus (EBV) is a highly efficient acute transforming agent in human cells, provided that the intact virus is used. To investigate the ability of viral DNA alone to transform cells, we introduced the EBV genome into human lymphocytes. After microinjection of EBV DNA into neonatal B lymphocytes, we established a cell line that in early passages contained multiple viral fragments. This cell line retained sequences from the short, unique (Us) region of the EBV genome and sequences from EcoRI-E. The viral sequences were not expressed; however, the cells expressed a 2.3-kilobase polyadenylated message homologous to the c-fgr oncogene, a cellular locus believed to be activated by EBV infection [M. S. C. Cheah, T. J. Ley, S. R. Tronick, and K. C. Robbins, Nature (London) 319:238-240.]. The cell line was monoclonal with rearrangement at the immunoglobulin locus and had a reciprocal translocation t(1;7)(p34;q34) and a deletion of sequences within the locus for the beta chain of the T-cell receptor. The close proximity of the translocation to the chromosomal loci for c-fgr on chromosome 1 and the T-cell receptor beta chain on chromosome 7 suggests that structural alteration of these genes was critical to this transformation event.
机译:Epstein-Barr病毒(EBV)是一种高效的人细胞急性转化剂,条件是使用完整的病毒。为了探讨单独的病毒DNA的能力转化细胞,我们将EBV基因组引入人淋巴细胞。在将EBV DNA微注射到新生儿B淋巴细胞后,我们建立了一种在早期通道中含有多个病毒片段的细胞系。该细胞系从EBV基因组的短,独特(US)区域和来自EcoRI-e的序列的序列保留。未表达病毒序列;然而,细胞表达了2.3千碱基的多腺苷酸化消息与C-FGR癌基因同源,据信被EBV感染激活的细胞基因座[M. S. C. C. Cheah,T.J.Ley,S. R. Tonick和K.C.Crobins,Nature(伦敦)319:238-240。]。细胞系是单克隆的,具有在免疫球蛋白基因座的重排,并且具有往复转移T(1; 7)(P34; Q34),以及缺失T细胞受体的β链内的轨迹内的序列。在染色体1和染色体上的T细胞受体β链上的C-FGR染色体基因座的紧密接近7表明这些基因的结构改变对该转化事件至关重要。

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