首页> 美国卫生研究院文献>Journal of Virology >Production of polyomavirus late mRNAs requires sequences near the 5 end of the leader but does not require leader-to-leader splicing.
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Production of polyomavirus late mRNAs requires sequences near the 5 end of the leader but does not require leader-to-leader splicing.

机译:多瘤病毒后期mRNA的产生需要在前导序列5末端附近的序列但不需要前导序列至前导序列的剪接。

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摘要

Polyomavirus late mRNAs contain multiple copies of a 57-nucleotide leader sequence derived by splicing from multigenome-length late transcripts. Inefficient termination of transcription and inefficient polyadenylation allow accumulation of these giant transcripts. In this report, we show that a viable mutant virus, ins5, which contains an efficient rabbit beta-globin polyadenylation signal, produced late mRNAs whose vast majority contains only one leader. ins5 virus nevertheless produced as much late mRNA as did wild-type virus and grew as well as did wild-type virus in mouse cells. These results demonstrate that leader-to-leader splicing per se is not required for efficient production of late mRNAs or for efficient virus replication. However, we also found that RNAs lacking critical sequences near the 5' end of the leader did not accumulate as mRNAs and that most late transcripts made during the early part of the late phase, when few late mRNAs are produced, initiated downstream of the 5' end of the leader. These results indicate that a sequence element near the 5' end of the leader is required for proper processing, transport, or stability of late mRNAs and that the control of late mRNA production depends in part on the choice of transcription initiation sites at the late promoter.
机译:多瘤病毒晚期mRNA包含多拷贝的57个核苷酸的前导序列,该序列是通过剪接多基因组长度的晚期转录本而得来的。无效的转录终止和无效的聚腺苷酸化允许这些巨大转录物的积累。在此报告中,我们显示了一种可行的突变病毒ins5,它包含有效的兔β-球蛋白聚腺苷酸化信号,产生了晚期mRNA,其绝大多数只包含一个前导序列。然而,ins5病毒与野生型病毒一样能产生尽可能多的晚期mRNA,并且在小鼠细胞中的生长和野生型病毒一样好。这些结果表明,对于后期mRNA的有效产生或有效的病毒复制,并不需要先对先的剪接。但是,我们还发现,在前导序列5'末端附近缺少关键序列的RNA不会以mRNA的形式积累,并且大多数晚期转录物是在晚期阶段的早期生成的,此时产生的后期mRNA很少,因此在5的下游开始领袖的尽头。这些结果表明,在晚期mRNA的正确加工,运输或稳定性中,前导序列5'末端附近需要一个序列元件,并且对晚期mRNA产生的控制部分取决于晚期启动子上转录起始位点的选择。 。

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