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Pby1 is a direct partner of the Dcp2 decapping enzyme

机译:PBY1是DCP2衰减酶的直接合作伙伴

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摘要

Most eukaryotic mRNAs harbor a characteristic 5' m(7)GpppN cap that promotes pre-mRNA splicing, mRNA nucleocytoplasmic transport and translation while also protecting mRNAs from exonucleolytic attacks. mRNA caps are eliminated by Dcp2 during mRNA decay, allowing 5'-3' exonucleases to degrade mRNA bodies. However, the Dcp2 decapping enzyme is poorly active on its own and requires binding to stable or transient protein partners to sever the cap of target mRNAs. Here, we analyse the role of one of these partners, the yeast Pby1 factor, which is known to co-localize into P-bodies together with decapping factors. We report that Pby1 uses its C-terminal domain to directly bind to the decapping enzyme. We solved the structure of this Pby1 domain alone and bound to the Dcp1-Dcp2-Edc3 decapping complex. Structure-based mutant analyses reveal that Pby1 binding to the decapping enzyme is required for its recruitment into P-bodies. Moreover, Pby1 binding to the decapping enzyme stimulates growth in conditions in which decapping activation is compromised. Our results point towards a direct connection of Pby1 with decapping and P-body formation, both stemming from its interaction with the Dcp1-Dcp2 holoenzyme.
机译:大多数真核mRNAS含有特征5'M(7)GPPPN帽,其促进mRNA剪接,mRNA核细胞间转运和翻译,同时保护MRNA免受外核溶解的发作。在mRNA衰减期间DCP2消除mRNA帽,允许5'-3'外切核酶降解mRNA体。然而,DCP2拆下酶在其自身上效应很差,并且需要与稳定或瞬态蛋白质合作伙伴结合以切断靶MRNA的帽。在这里,我们分析了这些合作伙伴之一的作用,酵母PBy1因子,已知与卷积因子一起将其与p-体定位成p-体。我们报告称Py1使用其C末端域直接与卷取酶结合。我们独自解决了该PBY1域的结构并与DCP1-DCP2-EDC3拆下复合物结合。基于结构的突变分析表明,其募集成对p-体需要与拆解酶结合的py1。此外,与卷积酶结合的PBy1刺激拆下激活受损的条件下的生长。我们的结果朝向Py1的直接连接,具有折叠和p体形成,源于其与DCP1-DCP2全酶的相互作用。

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  • 来源
    《Nucleic Acids Research》 |2020年第11期|共14页
  • 作者单位

    Ecole Polytech CNRS IP Paris Lab Biol Struct Cellule BIOC F-91128 Palaiseau France;

    Inst Genet &

    Biol Mol &

    Cellulaire IGBMC Illkirch Graffenstaden France;

    Ecole Polytech CNRS IP Paris Lab Biol Struct Cellule BIOC F-91128 Palaiseau France;

    Ecole Polytech CNRS IP Paris Lab Biol Struct Cellule BIOC F-91128 Palaiseau France;

    Ecole Polytech CNRS IP Paris Lab Biol Struct Cellule BIOC F-91128 Palaiseau France;

    Inst Genet &

    Biol Mol &

    Cellulaire IGBMC Illkirch Graffenstaden France;

    Ecole Polytech CNRS IP Paris Lab Biol Struct Cellule BIOC F-91128 Palaiseau France;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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