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Complete human gene structure of obscurin: implications for isoform generation by differential splicing

机译:obscurin的完整人类基因结构:通过差异剪接产生同工型的意义

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摘要

The complete gene giant muscle protein obscurin, a modular protein composed largely of tandem Ig-domains, GDP/GTP exchange factor domains (GEF) for small G-proteins, and differentially spliced kinase domains, was analysed. The splice donor and acceptor sites of the 117 exons give important clues for potential splice pathways. The fusion of the conventional obscurin A, containing only the GEF domain, and obscurin B, fusing into the 3′ kinase exons, was experimentally confirmed and analysed. The linker between the two kinases contains multiple predicted phosphorylation sites, as well as a predicted NFX zinc finger domain. Both kinases show only weak homology to either myosin light chain kinases or other giant muscle protein kinases, suggesting that they are functionally distinct.
机译:分析了完整的基因巨肌蛋白obscurin,一种由串联Ig结构域,小G蛋白的GDP / GTP交换因子结构域(GEF)和差异剪接的激酶结构域组成的模块化蛋白。 117个外显子的剪接供体和受体位点为潜在的剪接途径提供了重要线索。通过实验证实并分析了仅包含GEF结构域的常规obscurin A与融合到3'激酶外显子中的obscurin B的融合。两种激酶之间的接头包含多个预测的磷酸化位点,以及一个预测的NFX锌指结构域。两种激酶与肌球蛋白轻链激酶或其他巨型肌肉蛋白激酶均仅显示弱同源性,表明它们在功能上是不同的。

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  • 来源
    《Journal of Muscle Research and Cell Motility》 |2005年第8期|427-434|共8页
  • 作者单位

    The Randall Division of Cell and Molecular Biophysics and The Cardiovascular Division New Hunt’s House King’s College London;

    The Randall Division of Cell and Molecular Biophysics and The Cardiovascular Division New Hunt’s House King’s College London;

    The Randall Division of Cell and Molecular Biophysics and The Cardiovascular Division New Hunt’s House King’s College London;

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