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剪接因子SPF30介导前剪接体蛋白U2AF35与三小核核糖核蛋白hPrp3之间的相互作用。

Splicing factor SPF30 bridges an interaction between the prespliceosome protein U2AF35 and tri-small nuclear ribonucleoprotein protein hPrp3.

作者信息

Little John T, Jurica Melissa S

机构信息

Department of Molecular, Cell, and Developmental Biology and Center for Molecular Biology of RNA, University of California, Santa Cruz, CA 95064, USA.

出版信息

J Biol Chem. 2008 Mar 28;283(13):8145-52. doi: 10.1074/jbc.M707984200. Epub 2008 Jan 22.

DOI:10.1074/jbc.M707984200
PMID:18211889
Abstract

Spliceosome assembly is a dynamic process involving the sequential recruitment and rearrangement of small nuclear ribonucleoproteins (snRNPs) on a pre-mRNA substrate. Here we identify several spliceosome protein interactions with different domains of human splicing factor SPF30 that have the potential to mediate the addition of the tri-snRNP to the prespliceosome. In particular, we show that the C-terminal tails of SmD1, SmD3, and the protein Lsm4 interact with the central Tudor domain of SPF30. We identify a novel interaction between the N-terminal domain of SPF30 and U2AF35, a prespliceosome protein that has a role in recognizing the 3' splice site and recruiting U2 snRNP. We also show that the C terminus of SPF30 interacts with a middle domain of hPrp3, a component of U4/U6 di-snRNP and the tri-snRNP. Importantly, we show that the U2AF35 and hPrp3 interactions with SPF30 can occur simultaneously, thereby potentially linking 3' splice site recognition with tri-snRNP addition. Finally, we note that SPF30 and its partner-interacting domains are not conserved in yeast, suggesting this interaction network may play an important role in the complex splicing observed in higher eukaryotes.

摘要

剪接体组装是一个动态过程,涉及小核核糖核蛋白(snRNP)在mRNA前体底物上的顺序募集和重排。在此,我们鉴定了几种剪接体蛋白与人类剪接因子SPF30不同结构域的相互作用,这些相互作用有可能介导三snRNP添加到前剪接体中。特别地,我们发现SmD1、SmD3的C末端尾巴以及蛋白Lsm4与SPF30的中央Tudor结构域相互作用。我们鉴定出SPF30的N末端结构域与U2AF35之间存在一种新的相互作用,U2AF35是一种前剪接体蛋白,在识别3'剪接位点和募集U2 snRNP中发挥作用。我们还发现SPF30的C末端与hPrp3的中间结构域相互作用,hPrp3是U4/U6双snRNP和三snRNP的一个组成部分。重要的是,我们发现U2AF35和hPrp3与SPF30的相互作用可以同时发生,从而有可能将3'剪接位点识别与三snRNP添加联系起来。最后,我们注意到SPF30及其相互作用的结构域在酵母中并不保守,这表明这种相互作用网络可能在高等真核生物中观察到的复杂剪接过程中发挥重要作用。

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