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SV40早期前体mRNA的可变剪接由分支位点选择决定。

Alternative splicing of SV40 early pre-mRNA is determined by branch site selection.

作者信息

Noble J C, Prives C, Manley J L

机构信息

Department of Biological Sciences, Columbia University, New York, New York 10027.

出版信息

Genes Dev. 1988 Nov;2(11):1460-75. doi: 10.1101/gad.2.11.1460.

Abstract

Splicing of SV40 early pre-mRNA to alternative large-T and small-t mRNAs involves the utilization of multiple lariat branch sites. To determine the functional significance of these sites, we constructed and analyzed a set of base substitution mutants in which the major branch acceptors were altered, either singly or in combination. The ratio of large-T to small-t mRNAs produced in vivo was found to vary by over 100-fold between different mutants. When splicing was assayed in vitro with a standard pre-RNA, which results in splicing almost exclusively to large-T mRNA, the patterns of branch site utilization were altered dramatically, although the mutations were essentially without effect on splicing efficiency. However, use of a 5' truncated pre-RNA, which results in a splicing pattern that reflects the in vivo alternative splicing potential of this pre-RNA, revealed a strong correlation between the effects of the base substitutions on branch site selection and alternative splice-site utilization. An RNase protection analysis of factor interactions with the 5' splice sites and branch sites in wild-type and mutant pre-RNAs suggests that a competition for different branch sites plays a crucial role in the assembly of 'alternative' spliceosomes, thereby controlling alternative splice-site selection.

摘要

SV40早期前体mRNA剪接产生不同的大T和小t mRNA涉及多个套索状分支位点的利用。为了确定这些位点的功能意义,我们构建并分析了一组碱基替代突变体,其中主要分支受体被单独或组合改变。发现在体内产生的大T与小t mRNA的比例在不同突变体之间变化超过100倍。当用标准前体RNA在体外检测剪接时,其结果几乎完全是剪接成大T mRNA,尽管这些突变对剪接效率基本没有影响,但分支位点利用模式却发生了显著改变。然而,使用5'端截短的前体RNA,其剪接模式反映了该前体RNA在体内的可变剪接潜力,这揭示了碱基替代对分支位点选择和可变剪接位点利用的影响之间存在很强的相关性。对野生型和突变型前体RNA中与5'剪接位点和分支位点相互作用的因子进行的核糖核酸酶保护分析表明,对不同分支位点的竞争在“可变”剪接体的组装中起关键作用,从而控制可变剪接位点的选择。

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