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Massive expansions of Dscam splicing diversity via staggered homologous recombination during arthropod evolution

机译:节肢动物进化过程中通过交错同源重组Dscam剪接多样性的大规模扩展。

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摘要

The arthropod Down syndrome cell adhesion molecule (Dscam) gene can generate tens of thousands of protein isoforms via combinatorial splicing of numerous alternative exons encoding immunoglobulin variable domains organized into three clusters referred to as the exon 4, 6, and 9 clusters. Dscam protein diversity is important for nervous system development and immune functions. We have performed extensive phylogenetic analyses of Dscam from 20 arthropods (each containing between 46 and 96 alternative exons) to reconstruct the detailed history of exon duplication and loss events that built this remarkable system over 450 million years of evolution. Whereas the structure of the exon 4 cluster is ancient, the exon 6 and 9 clusters have undergone massive, independent expansions in each insect lineage. An analysis of nearly 2000 duplicated exons enabled detailed reconstruction of the timing, location, and boundaries of these duplication events. These data clearly show that new Dscam exons have arisen continuously throughout arthropod evolution and that this process is still occurring in the exon 6 and 9 clusters. Recently duplicated regions display boundaries corresponding to a single exon and the adjacent intron. The boundaries, homology, location, clustering, and relative frequencies of these duplication events strongly suggest that staggered homologous recombination is the major mechanism by which new Dscam exons evolve. These data provide a remarkably detailed picture of how complex gene structure evolves and reveal the molecular mechanism behind this process.
机译:节肢动物唐氏综合症细胞粘附分子(Dscam)基因可通过编码免疫球蛋白可变域的众多替代外显子的组合剪接,生成成千上万的蛋白质同工型,这些外显子组织为三个簇,分别称为外显子4、6和9。 Dscam蛋白多样性对于神经系统发育和免疫功能很重要。我们已经对20个节肢动物(每个昆虫中包含46至96个替代外显子)的Dscam进行了广泛的系统发育分析,以重建详细的外显子复制和丢失事件历史,这些事件在4.5亿年的进化过程中建立了这一非凡的系统。外显子4簇的结构很古老,而外显子6和9簇在每个昆虫谱系中都经历了巨大的独立扩展。对近2000个重复外显子的分析使得能够详细重建这些重复事件的时间,位置和边界。这些数据清楚地表明,在节肢动物的整个进化过程中,新的Dscam外显子不断出现,并且这一过程仍在外显子6和9簇中发生。最近复制的区域显示对应于单个外显子和相邻内含子的边界。这些复制事件的边界,同源性,位置,聚类和相对频率强烈表明,交错的同源重组是新Dscam外显子进化的主要机制。这些数据提供了非常复杂的基因结构如何演化的非常详尽的图片,并揭示了该过程背后的分子机制。

著录项

  • 来源
    《RNA》 |2010年第1期|91-105|共15页
  • 作者单位

    Department of Chemistry and Biochemistry, Center for Computational Biology, Institute for Genomics and Proteomics, Molecular Biology Institute, University of California at Los Angeles, Los Angeles, California 90095-1570, USA;

    Department of Chemistry and Biochemistry, Center for Computational Biology, Institute for Genomics and Proteomics, Molecular Biology Institute, University of California at Los Angeles, Los Angeles, California 90095-1570, USA;

    Department of Chemistry and Biochemistry, Center for Computational Biology, Institute for Genomics and Proteomics, Molecular Biology Institute, University of California at Los Angeles, Los Angeles, California 90095-1570, USA;

    Department of Genetics and Developmental Biology, University of Connecticut Stem Cell Institute, University of Connecticut Health Center, Farmington, Connecticut 06030-3301, USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    alternative splicing; Dscam; evolution;

    机译:选择性剪接;Dscam;演化;

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