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首页> 外文期刊>Journal of Virology >Characterization of the simian virus 40 late promoter: relative importance of sequences within the 72-base-pair repeats differs before and after viral DNA replication.
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Characterization of the simian virus 40 late promoter: relative importance of sequences within the 72-base-pair repeats differs before and after viral DNA replication.

机译:Simian病毒40晚期启动子的表征:72碱基对重复序列内的序列的相对重要性在病毒DNA复制之前和之后不同。

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We examined sequences involved in the simian virus 40 (SV40) late promoter in vivo, by using quantitative S1 nuclease analysis of a series of deletion mutants within the SV40 regulatory region. These mutants were constructed so as to place the altered promoter region in its normal position relative to the SV40 late genes. The effects of the deletions on late transcriptional activity were analyzed before and after viral DNA replication, by omitting or including SV40 large T antigen. The data show that (i) in the absence of large T antigen, the deletion of the 21-base-pair (bp) repeats results in a fourfold increase in late transcription, and (ii) the sequences within the 72-bp repeats are a component of the SV40 late promoter, acting not only before, but also after viral DNA replication. We identified two domains which contain sequences important for efficient late transcription. Domain I, at the late proximal end of each 72-bp repeat, was found to function before replication and was possibly also involved after replication. The contribution of domain II, at the late distal end of each 72-bp repeat, was much more significant after replication but only of minor importance before replication.
机译:通过使用SV40调节区内的一系列缺失突变体的定量S1核酸酶分析,我们检查体内辛安病毒40(SV40)后启动子涉及的序列。构建这些突变体以使改变的启动子区相对于SV40晚基因的正常位置。在病毒DNA复制之前和之后分析缺失对晚期转录活性的影响,通过省略或包括SV40大T抗原。数据显示(i)在没有大的T抗原的情况下,21-碱基对(BP)重复的缺失导致晚期转录的四倍增加,并且(ii)72-BP重复内的序列是SV40晚期启动子的组分,不仅以前而作用,还在病毒DNA复制后作用。我们鉴定了两个域,其含有序列对于有效晚期转录很重要。在每个72-BP重复的临时近端的域I被发现在复制之前运行,并且可能也涉及复制后。域II的贡献在每72bp重复的每次72-BP重复的晚期末端,在复制后的显着程度更为显着,但在复制之前只有很小的重要性。

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