首页> 美国卫生研究院文献>Journal of Virology >Control elements situated downstream of the major transcriptional start site are sufficient for highly efficient polyomavirus late transcription.
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Control elements situated downstream of the major transcriptional start site are sufficient for highly efficient polyomavirus late transcription.

机译:位于主要转录起始位点下游的控制元件足以实现高效的多瘤病毒后期转录。

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摘要

In a transient expression assay in mouse fibroblasts in which neither replication nor T-antigen synthesis occurred, the polyomavirus late promoter functioned faithfully and even more efficiently than the simian virus 40 early promoter. Surprisingly, the DNA sequences upstream of the main transcriptional start sites were not required to obtain the high mRNA level observed. It appeared to result from the combined action of a basal promoter element within the A enhancer domain and of a more downstream element, located in the VP3 intron and abutting the late splice donor. We also show that although an enhancer region was required, enhancer function per se was not. Instead, it appeared that only a defined subset of the DNA-protein interactions necessary for enhancer function was involved in late promoter activity.
机译:在小鼠成纤维细胞的瞬时表达分析中,既没有复制也没有T抗原合成发生,多瘤病毒晚期启动子的功能忠实,甚至比猿猴病毒40早期启动子更有效。令人惊讶地,不需要主要转录起始位点上游的DNA序列来获得观察到的高mRNA水平。它似乎是由A增强子域内的基础启动子元件和位于VP3内含子中并与晚期剪接供体邻接的更下游元件的联合作用导致的。我们还表明,尽管需要增强子区域,但增强子功能本身不是必需的。取而代之的是,似乎只有增强子功能所必需的DNA-蛋白质相互作用的确定子集参与了晚期启动子活性。

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