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U2/U6螺旋Ib在5'剪接位点选择中的作用。

A role for U2/U6 helix Ib in 5' splice site selection.

作者信息

Luukkonen B G, Séraphin B

机构信息

European Molecular Biology Laboratory, Heidelberg, Germany.

出版信息

RNA. 1998 Aug;4(8):915-27. doi: 10.1017/s1355838298980591.

Abstract

Selection of pre-mRNA splice sites is a highly accurate process involving many trans-acting factors. Recently, we described a role for U6 snRNA position G52 in selection of the first intron nucleotide (+1G). Because some U2 alleles suppress U6-G52 mutations, we investigated whether the corresponding U2 snRNA region also influenced 5' splice site selection. Our results demonstrate that U2 snRNAs mutated at position U23, but not adjacent nucleotides, specifically affect 5' splice site cleavage. Furthermore, all U2 position U23 mutations are synthetic lethal with the thermosensitive U6-G52U allele. Interestingly, the U2-U23C substitution has an unprecedented hyperaccurate splicing phenotype in which cleavage of introns with a +1G substitution is reduced, whereas the strain grows with wild-type kinetics. U2 position U23 forms the first base pair with U6 position A59 in U2/U6 helix Ib. Restoration of the helical structure suppresses 5' splice site cleavage defects, showing an important role for the helix Ib structure in 5' splice site selection. U2/U6 helix Ib and helix II have recently been described as being functionally redundant. This report demonstrates a unique role for helix Ib in 5' splice site selection that is not shared with helix II.

摘要

前体mRNA剪接位点的选择是一个高度精确的过程,涉及许多反式作用因子。最近,我们描述了U6 snRNA的G52位点在第一个内含子核苷酸(+1G)选择中的作用。由于一些U2等位基因可抑制U6-G52突变,我们研究了相应的U2 snRNA区域是否也影响5'剪接位点的选择。我们的结果表明,在U23位点发生突变但相邻核苷酸未突变的U2 snRNAs会特异性影响5'剪接位点的切割。此外,所有U2的U23位点突变与温度敏感型U6-G52U等位基因都是合成致死的。有趣的是,U2-U23C替代具有前所未有的超精确剪接表型,其中+1G替代的内含子切割减少,而该菌株以野生型动力学生长。U2的U23位点在U2/U6螺旋Ib中与U6的A59位点形成第一个碱基对。螺旋结构的恢复可抑制5'剪接位点切割缺陷,表明螺旋Ib结构在5'剪接位点选择中起重要作用。最近有人描述U2/U6螺旋Ib和螺旋II在功能上是冗余的。本报告证明了螺旋Ib在5'剪接位点选择中具有独特作用,这是螺旋II所不具备的。

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