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Conservation of functional domains involved in RNA binding and protein-protein interactions in human and Saccharomyces cerevisiae pre-mRNA splicing factor SF1.

机译:在人类和酿酒酵母前mRNA剪接因子SF1中参与RNA结合和蛋白质-蛋白质相互作用的功能域的保守性。

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摘要

The modular structure of splicing factor SF1 is conserved from yeast to man and SF1 acts at early stages of spliceosome assembly in both organisms. The hnRNP K homology (KH) domain of human (h) SF1 is the major determinant for RNA binding and is essential for the activity of hSF1 in spliceosome assembly, supporting the view that binding of SF1 to RNA is essential for its function. Sequences N-terminal to the KH domain mediate the interaction between hSF1 and U2AF65, which binds to the polypyrimidine tract upstream of the 3' splice site. Moreover, yeast (y) SF1 interacts with Mud2p, the presumptive U2AF65 homologue in yeast, and the interaction domain is conserved in ySF1. The C-terminal degenerate RRMs in U2AF65 and Mud2p mediate the association with hSF1 and ySF1, respectively. Analysis of chimeric constructs of hSF1 and ySF indicates that the KH domain may serve a similar function in both systems, whereas sequences C-terminal to the KH domain are not exchangeable. Thus, these results argue for hSF1 and ySF1, as well as U2AF65 and Mud2p, being functional homologues.
机译:剪接因子SF1的模块结构从酵母到人都是保守的,并且SF1在两种生物体的剪接体组装的早期阶段起作用。人(h)SF1的hnRNP K同源性(KH)结构域是RNA结合的主要决定因素,对于剪接体组装中hSF1的活性至关重要,这支持以下观点:SF1与RNA的结合对其功能至关重要。 KH结构域的N端序列介导hSF1和U2AF65之间的相互作用,后者与3'剪接位点上游的多嘧啶束结合。此外,酵母(y)SF1与Mud2p(酵母中推测的U2AF65同源物)相互作用,并且相互作用域在ySF1中是保守的。 U2AF65和Mud2p中的C端简并RRM分别介导与hSF1和ySF1的关联。对hSF1和ySF的嵌合构建体的分析表明,KH结构域在两个系统中都可以发挥相似的功能,而KH结构域的C末端序列是不可交换的。因此,这些结果证明了hSF1和ySF1以及U2AF65和Mud2p是功能同源物。

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