Characterization of Cyclin L1 and L2 Interactions with CDK11 and Splicing Factors

细胞周期蛋白A2 RNA剪接 细胞周期蛋白 细胞周期蛋白D 生物 细胞周期蛋白B 细胞生物学 细胞周期蛋白依赖激酶复合物 选择性拼接 SR蛋白 周期素 细胞周期蛋白 剪接体 分子生物学 生物化学 基因亚型 细胞周期 基因 核糖核酸
作者
Pascal Loyer,Janeen H. Trembley,José Grenet,Adeline Busson,Anne Corlu,Wei Zhao,Mehmet Koçak,Vincent J. Kidd,Jill M. Lahti
出处
期刊:Journal of Biological Chemistry [Elsevier BV]
卷期号:283 (12): 7721-7732 被引量:126
标识
DOI:10.1074/jbc.m708188200
摘要

Although it has been reported that cyclin L1alpha and L2alpha proteins interact with CDK11(p110), the nature of the cyclin L transcripts, the formation of complexes between the five cyclin L and the three CDK11 protein isoforms, and the influence of these complexes on splicing have not been thoroughly investigated. Here we report that cyclin L1 and L2 genes generate 14 mRNA variants encoding six cyclin L proteins, one of which has not been described previously. Using cyclin L gene-specific antibodies, we demonstrate expression of multiple endogenous cyclin L proteins in human cell lines and mouse tissues. Moreover, we characterize interactions between CDK11(p110), mitosis-specific CDK11(p58), and apoptosis-specific CDK11(p46) with both cyclin Lalpha and -beta proteins and the co-elution of these proteins following size exclusion chromatography. We further establish that CDK11(p110) and associated cyclin Lalpha/beta proteins localize to splicing factor compartments and nucleoplasm and interact with serine/arginine-rich proteins. Importantly, we also determine the effect of CDK11-cyclin L complexes on pre-mRNA splicing. Preincubation of nuclear extracts with purified cyclin Lalpha and -beta isoforms depletes the extract of in vitro splicing activity. Ectopic expression of cyclin L1alpha, L1beta, L2alpha, or L2beta or active CDK11(p110) individually enhances intracellular intron splicing activity, whereas expression of CDK11(p58/p46) or kinase-dead CDK11(p110)represses splicing activity. Finally, we demonstrate that expression of cyclins Lalpha and -beta and CDK11(p110) strongly and differentially affects alternative splicing in vivo. Together, these data establish that CDK11(p110) interacts physically and functionally with cyclin Lalpha and -beta isoforms and SR proteins to regulate splicing.
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