SV40基因组在人类细胞系中稳定整合之前的事件。

S P Hwang, R S Kucherlapati
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引用次数: 17

摘要

我们在转化的人成纤维细胞系的非克隆群体中检测了整合SV40序列的组织。检测小鼠B82细胞与人GM847细胞的体细胞杂交,检测SV40 t抗原的表达和个体人染色体的存在。结果表明,SV40基因组位于人类7号染色体上。对亲本人细胞系进行限制性内切酶酶切和印迹杂交,发现其含有多个正常和有缺陷的SV40拷贝串联整合到宿主基因组中。对几种T-ag+杂交细胞系的类似分析表明,不同杂交细胞系(即原始群体的不同细胞)的整合病毒序列非常密切相关,但并不总是相同的。对GM847亚克隆的分析也显示出这种差异。基于这些结果,我们假设在初始整合事件之后,病毒以及侧翼宿主DNA序列变得不稳定,并受到缺失和重排的影响。这种短暂的结构不稳定性之后,SV40的高度稳定整合在这些细胞或其杂交衍生物中维持至少数百代细胞。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Events preceding stable integration of SV40 genomes in a human cell line.

We have examined the organization of integrated SV40 sequences in an uncloned population of a transformed human fibroblast cell line. Somatic cell hybrids between mouse B82 cells and human GM847 cells were examined for SV40 T-antigen expression and individual human chromosome presence. This analysis revealed that a functional SV40 genome is located on human chromosome 7. Restriction endonuclease digestion followed by blot hybridization of the parental human cell line revealed that it contains multiple normal and defective SV40 copies integrated into the host genome in tandem. A similar analysis of several T-ag+ hybrid cell lines indicated that the integrated viral sequences in different hybrid cell lines (thus in different cells of the original population) are very closely related but not always identical. Analysis of subclones of GM847 also revealed such differences. Based upon these results, we postulate that following the initial integration event, viral as well as the flanking host DNA sequences become unstable and are subject to deletions and rearrangements. This short-lived structural instability is followed by highly stable integration of SV40 which is maintained in these cells or their hybrid derivatives for at least hundreds of cell generations.

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