脊椎动物多聚腺苷酸聚合酶的羧基末端与U2AF 65相互作用,以耦合3'末端加工和剪接。
The carboxyl terminus of vertebrate poly(A) polymerase interacts with U2AF 65 to couple 3'-end processing and splicing.
作者信息
Vagner S, Vagner C, Mattaj I W
机构信息
European Molecular Biology Laboratory (EMBL), 69117 Heidelberg, Germany.
出版信息
Genes Dev. 2000 Feb 15;14(4):403-13.
Abstract
Although it has been established that the processing factors involved in pre-mRNA splicing and 3'-end formation can influence each other positively, the molecular basis of this coupling interaction was not known. Stimulation of pre-mRNA splicing by an adjacent cis-linked cleavage and polyadenylation site in HeLa cell nuclear extract is shown to occur at an early step in splicing, the binding of U2AF 65 to the pyrimidine tract of the intron 3' splice site. The carboxyl terminus of poly(A) polymerase (PAP) previously has been implicated indirectly in the coupling process. We demonstrate that a fusion protein containing the 20 carboxy-terminal amino acids of PAP, when tethered downstream of an intron, increases splicing efficiency and, like the entire 3'-end formation machinery, stimulates U2AF 65 binding to the intron. The carboxy-terminal domain of PAP makes a direct and specific interaction with residues 17-47 of U2AF 65, implicating this interaction in the coupling of splicing and 3'-end formation.
摘要
虽然已经确定参与前体mRNA剪接和3'末端形成的加工因子可以相互产生正向影响,但这种偶联相互作用的分子基础尚不清楚。研究表明,在HeLa细胞核提取物中,相邻的顺式连接的切割和聚腺苷酸化位点对前体mRNA剪接的刺激发生在剪接的早期步骤,即U2AF 65与内含子3'剪接位点的嘧啶序列结合时。聚腺苷酸聚合酶(PAP)的羧基末端先前已间接参与偶联过程。我们证明,当一个含有PAP 20个羧基末端氨基酸的融合蛋白连接在内含子下游时,可提高剪接效率,并且与整个3'末端形成机制一样,刺激U2AF 65与内含子结合。PAP的羧基末端结构域与U2AF 65的17 - 47位残基直接且特异性相互作用,表明这种相互作用参与了剪接和3'末端形成的偶联。
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