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转运蛋白-SR2介导磷酸化SR蛋白的核输入。

Transportin-SR2 mediates nuclear import of phosphorylated SR proteins.

作者信息

Lai M C, Lin R I, Tarn W Y

机构信息

Institute of Biomedical Sciences, Academia Sinica, Nankang, Taipei 11529, Taiwan.

出版信息

Proc Natl Acad Sci U S A. 2001 Aug 28;98(18):10154-9. doi: 10.1073/pnas.181354098. Epub 2001 Aug 21.

Abstract

Serine/arginine-rich proteins (SR proteins) are a family of nuclear factors that play important roles in both constitutive and regulated precursor mRNA splicing. The domain rich in arginine/serine (RS) repeats (RS domain) serves as both a nuclear and subnuclear localization signal. We previously identified an importin beta family protein, transportin-SR2 (TRN-SR2), that specifically interacts with phosphorylated RS domains. A TRN-SR2 mutant deficient in Ran binding colocalizes with SR proteins in nuclear speckles, suggesting a role of TRN-SR2 in nuclear targeting of SR proteins. Using in vitro import assays, we here show that nuclear import of SR protein fusions requires cytosolic factors, and that the RS domain becomes phosphorylated in the import reaction. Reconstitution of SR protein import by using recombinant transport factors clearly demonstrates that TRN-SR2 is capable of targeting phosphorylated, but not unphosphorylated, SR proteins to the nucleus. Therefore, RS domain phosphorylation is critical for TRN-SR2-mediated nuclear import. Interestingly, we found that the RNA-binding activity of SR proteins confers temperature sensitivity to their nuclear import. Finally, we show that TRN-SR2 interacts with a nucleoporin and is targeted not only to the nuclear envelope but also to nuclear speckles in vitro. Thus, TRN-SR2 may perhaps escort SR protein cargoes to nuclear subdomains.

摘要

富含丝氨酸/精氨酸的蛋白质(SR蛋白)是一类核因子,在组成型和调控型前体mRNA剪接中均发挥重要作用。富含精氨酸/丝氨酸(RS)重复序列的结构域(RS结构域)兼具核定位信号和亚核定位信号的功能。我们之前鉴定出一种importin β家族蛋白——转运蛋白-SR2(TRN-SR2),它能特异性地与磷酸化的RS结构域相互作用。一种缺乏Ran结合能力的TRN-SR2突变体与SR蛋白在核斑点中共定位,这表明TRN-SR2在SR蛋白的核靶向定位中发挥作用。通过体外导入实验,我们在此表明SR蛋白融合体的核导入需要胞质因子,并且RS结构域在导入反应中会发生磷酸化。利用重组转运因子对SR蛋白导入进行重构,清楚地证明TRN-SR2能够将磷酸化而非未磷酸化的SR蛋白靶向转运至细胞核。因此,RS结构域的磷酸化对于TRN-SR2介导的核导入至关重要。有趣的是,我们发现SR蛋白的RNA结合活性赋予其核导入温度敏感性。最后,我们表明TRN-SR2与一种核孔蛋白相互作用,并且在体外不仅靶向核膜,还靶向核斑点。因此,TRN-SR2或许能护送SR蛋白货物至核亚结构域。

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