首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Amplification of integrated viral DNA sequences in polyoma virus-transformed cells.
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Amplification of integrated viral DNA sequences in polyoma virus-transformed cells.

机译:在多瘤病毒转化细胞中整合病毒DNA序列的扩增。

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摘要

Polyoma virus (Py) transformation of rat cells requires integration of viral genomes into the host DNA, which generally occurs in a partial or full head-to-tail tandem arrangement. The instability of this structure was previously demonstrated by the high rate of loss of integrated Py genomes in the presence of viral large tumor (T) antigen. We now show that integrated Py DNA sequences can also undergo amplification. We studied two rat cell lines transformed by the ts-a Py mutant, which codes for a thermolabile large T antigen. In a derivative of the ts-a H6A cell line, we have observed loss of full-length Py DNA molecules from the integrated tandem ("curing"), accompanied by the creation of new tandem repeats of two segments of viral DNA corresponding to 38% and 10% of the viral genome, each containing the origin of DNA replication. In the ts-a H3A cell line, which contains an integrated partial tandem of about 1.3 viral genomes with three distinct deletions, propagation at 33 degrees C resulted in the generation of full tandem repeats of a 94% Py DNA "unit" (including two 3% deletions), an 85% "unit" (including a 3% and the 12% deletion), or both. Amplification of integrated viral DNA was not observed in cells propagated at 39.5 degrees C, the nonpermissive temperature for large T antigen function. Amplification of integrated Py DNA sequences thus requires an active large T antigen and can generate a full tandem of integrated viral DNA molecules long after the initial integration event.
机译:大鼠细胞的多瘤病毒(Py)转化需要将病毒基因组整合到宿主DNA中,这通常以部分或完全头尾串联的方式发生。以前,在存在病毒性大肿瘤(T)抗原的情况下,整合Py基因组的高丢失率证明了这种结构的不稳定性。现在我们显示整合的Py DNA序列也可以进行扩增。我们研究了由ts-a Py突变体转化的两种大鼠细胞系,该突变体编码不耐热的大T抗原。在ts-a H6A细胞系的衍生物中,我们观察到了完整的串联Py DNA分子从整合的串联结构中丢失(“固化”),并伴随着病毒DNA的两个片段的新串联重复序列的产生,相应于38病毒基因组的%和10%,每个都包含DNA复制的起点。在ts-a H3A细胞系中,该细胞系包含约1.3个病毒基因组的整合的部分串联结构,具有三个明显的缺失,在33°C繁殖导致产生94%Py DNA“单位”(包括两个)的完整串联结构重复序列3%的删除),85%的“单位”(包括3%和12%的删除),或两者兼而有之。在39.5摄氏度(大T抗原功能的非许可温度)下繁殖的细胞中未观察到整合病毒DNA的扩增。因此,整合的Py DNA序列的扩增需要有活性的大T抗原,并且可以在最初的整合事件发生后很长一段时间内产生完整串联的整合的病毒DNA分子。

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