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首页> 外文期刊>Current Biology: CB >Pre-emptive Quality Control of a Misfolded Membrane Protein by Ribosome-Driven Effects
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Pre-emptive Quality Control of a Misfolded Membrane Protein by Ribosome-Driven Effects

机译:通过核糖体驱动效应预折叠膜蛋白的先发制物质控制

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摘要

Cells possess multiple mechanisms that protect against the accumulation of toxic aggregation-prone proteins. Here, we identify a pre-emptive pathway that reduces synthesis of membrane proteins that have failed to properly assemble in the endoplasmic reticulum (ER). We show that loss of the ER membrane complex (EMC) or mutation of the Sec61 translocon causes reduced synthesis of misfolded forms of the yeast ABC transporter Yor1. Synthesis defects are rescued by various ribosomal mutations, as well as by reducing cellular ribosome abundance. Genetic and biochemical evidence point to a ribosome-associated quality-control pathway triggered by ribosome collisions when membrane domain insertion and/or folding fails. In support of this model, translation initiation also contributes to synthesis defects, likely by modulating ribosome abundance on the message. Examination of translation efficiency across the yeast membrane proteome revealed that polytopic membrane proteins have relatively low ribosome abundance, providing evidence for translational tuning to balance protein synthesis and folding. We propose that by modulating translation rates of poorly folded proteins, cells can pre-emptively protect themselves from potentially toxic aberrant transmembrane proteins.
机译:细胞具有多种机制,可防止有毒聚集易蛋白的积累。这里,我们鉴定了一种预先挥发性途径,可减少未能适当地组装在内质网(ER)中的膜蛋白的合成。我们表明,SEC61摇合物的ER膜复合物(EMC)或突变的损失导致酵母ABC转运蛋白Yor1的错误折叠形式的合成。通过各种核糖体突变拯救合成缺陷,以及通过降低细胞核糖体丰度。当膜结构域插入和/或折叠发生故障时,遗传和生化证据指向由核糖体碰撞引发的核糖体相关的质量控制途径。为了支持这种模型,翻译起始也有助于合成缺陷,可能通过调节信息上的核糖体丰富。酵母膜蛋白质组的翻译效率检测显示,多种多纤膜蛋白具有相对低的核糖体丰度,为平移蛋白质合成和折叠提供平移调整的证据。我们提出通过调节折叠蛋白质不良的翻译率,细胞可以从潜在有毒的异常跨膜蛋白预先清空保护自己。

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  • 来源
    《Current Biology: CB》 |2020年第5期|共16页
  • 作者单位

    Columbia Univ Dept Biol Sci 1212 Amsterdam Ave New York NY 10027 USA;

    Med Res Council Lab Mol Biol Cambridge Biomed Campus Francis Crick Ave Cambridge CB2 0QH England;

    Med Res Council Lab Mol Biol Cambridge Biomed Campus Francis Crick Ave Cambridge CB2 0QH England;

    Med Res Council Lab Mol Biol Cambridge Biomed Campus Francis Crick Ave Cambridge CB2 0QH England;

    Univ Cambridge Cambridge Inst Med Res Keith Peters Bldg Hills Rd Cambridge CB2 0XY England;

    Univ Cambridge Cambridge Inst Med Res Keith Peters Bldg Hills Rd Cambridge CB2 0XY England;

    Columbia Univ Dept Biol Sci 1212 Amsterdam Ave New York NY 10027 USA;

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

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