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A family of splice variants of CstF-64 expressed in vertebrate nervous systems

机译:在脊椎动物神经系统中表达的CstF-64剪接变体家族

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Background Alternative splicing and polyadenylation are important mechanisms for creating the proteomic diversity necessary for the nervous system to fulfill its specialized functions. The contribution of alternative splicing to proteomic diversity in the nervous system has been well documented, whereas the role of alternative polyadenylation in this process is less well understood. Since the CstF-64 polyadenylation protein is known to be an important regulator of tissue-specific polyadenylation, we examined its expression in brain and other organs. Results We discovered several closely related splice variants of CstF-64 – collectively called βCstF-64 – that could potentially contribute to proteomic diversity in the nervous system. The βCstF-64 splice variants are found predominantly in the brains of several vertebrate species including mice and humans. The major βCstF-64 variant mRNA is generated by inclusion of two alternate exons (that we call exons 8.1 and 8.2) found between exons 8 and 9 of the CstF-64 gene, and contains an additional 147 nucleotides, encoding 49 additional amino acids. Some variants of βCstF-64 contain only the first alternate exon (exon 8.1) while other variants contain both alternate exons (8.1 and 8.2). In mice, the predominant form of βCstF-64 also contains a deletion of 78 nucleotides from exon 9, although that variant is not seen in any other species examined, including rats. Immunoblot and 2D-PAGE analyses of mouse nuclear extracts indicate that a protein corresponding to βCstF-64 is expressed in brain at approximately equal levels to CstF-64. Since βCstF-64 splice variant family members were found in the brains of all vertebrate species examined (including turtles and fish), this suggests that βCstF-64 has an evolutionarily conserved function in these animals. βCstF-64 was present in both pre- and post-natal mice and in different regions of the nervous system, suggesting an important role for βCstF-64 in neural gene expression throughout development. Finally, experiments in representative cell lines suggest that βCstF-64 is expressed in neurons but not glia. Conclusion This is the first report of a family of splice variants encoding a key polyadenylation protein that is expressed in a nervous system-specific manner. We propose that βCstF-64 contributes to proteomic diversity by regulating alternative polyadenylation of neural mRNAs.
机译:背景技术选择性剪接和聚腺苷酸化是创建神经系统履行其特定功能所必需的蛋白质组多样性的重要机制。替代剪接对神经系统蛋白质组学多样性的贡献已得到充分证明,而替代多聚腺苷酸化在此过程中的作用则鲜为人知。由于已知CstF-64聚腺苷酸蛋白是组织特异性聚腺苷酸化的重要调节剂,因此我们检查了其在脑和其他器官中的表达。结果我们发现了几个紧密相关的CstF-64剪接变体(统称为βCstF-64),它们可能有助于神经系统的蛋白质组多样性。 βCstF-64剪接变体主要存在于几种脊椎动物的大脑中,包括小鼠和人类。主要的βCstF-64变异mRNA是通过在CstF-64基因的第8和第9外显子之间包含两个替代外显子(我们分别称为第8.1和8.2外显子)而产生的,并包含147个核苷酸,编码49个氨基酸。 βCstF-64的某些变体仅包含第一个备用外显子(外显子8.1),而其他变体同时包含两个备用外显子(8.1和8.2)。在小鼠中,βCstF-64的主要形式还含有第9外显子的78个核苷酸的缺失,尽管该变异在包括大鼠在内的任何其他物种中均未见。小鼠核提取物的免疫印迹和2D-PAGE分析表明,对应于βCstF-64的蛋白质在脑中的表达水平与CstF-64大致相等。由于在所有检查的脊椎动物物种(包括海龟和鱼类)的大脑中都发现了βCstF-64剪接变体家族成员,因此表明βCstF-64在这些动物中具有进化保守的功能。 βCstF-64存在于出生前和出生后的小鼠中以及神经系统的不同区域,这暗示了βCstF-64在整个发育过程中在神经基因表达中的重要作用。最后,在代表性细胞系中的实验表明,βCstF-64在神经元中表达,但在胶质细胞中不表达。结论这是编码以神经系统特异性方式表达的关键聚腺苷酸化蛋白的剪接变体家族的首次报道。我们建议,βCstF-64通过调节神经mRNA的多聚腺苷酸来促进蛋白质组学多样性。

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