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Multiple cis-acting sequence elements are required for efficient splicing of simian virus 40 small-t antigen pre-mRNA.

机译:猿病毒40 small-t抗原pre-mRNA的有效剪接需要多个顺式作用序列元件。

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摘要

We have determined the effects of a number of mutations in the small-t antigen mRNA intron on the alternative splicing pattern of the simian virus 40 early transcript. Expansion of the distance separating the small-t pre-mRNA lariat branch point and the shared large T-small t 3' splice site from 18 to 29 nucleotides (nt) resulted in a relative enhancement of small-t splicing in vivo. This finding, coupled with the observation that large-T pre-RNA splicing in vitro was not affected by this expansion, suggests that small-t splicing is specifically constrained by a short branch point-3' splice site distance. Similarly, the distance separating the 5' splice site and branch point (48 nt) was found to be at or near a minimum for small-t splicing, because deletions in this region as small as 2 nt dramatically reduced the ratio of small-t to large-T mRNA that accumulated in transfected cells. Finally, a specific sequence within the small-t intron, encompassing the upstream branch sites used in large-T splicing, was found to be an important element in the cell-specific pattern of early alternative splicing. Substitutions within this region reduced the ratio of small-t to large-T mRNA produced in HeLa cells but had only minor effects in human 293 cells.
机译:我们已经确定了小t抗原mRNA内含子中许多突变对猿猴病毒40早期转录本的选择性剪接模式的影响。小t-mRNA前套索分支点和共享的大T-小t 3'剪接位点从18到29个核苷酸(nt)的距离扩大,导致体内小t剪接的相对增强。这一发现,加上观察到大T的pre-RNA体外剪接不受此扩展的影响,表明小T剪接受到一个短的分支点3'剪接位点距离的特别限制。类似地,发现5'剪接位点和分支点之间的距离(48 nt)等于或接近于小t剪接的最小值,因为该区域的缺失(最小至2 nt)大大降低了小t剪接的比例。到转染细胞中积累的大T mRNA。最后,发现小t内含子内的特定序列,包括大T剪接中使用的上游分支位点,是早期交替剪接的细胞特异性模式中的重要元素。该区域内的取代降低了HeLa细胞中产生的小T与大T mRNA的比例,但对人293细胞的影响却很小。

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