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首页> 外文期刊>Molecular Microbiology >A role for Saccharomyces cerevisiae Saccharomyces cerevisiae Centrin (Cdc31) in mitochondrial function and biogenesis
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A role for Saccharomyces cerevisiae Saccharomyces cerevisiae Centrin (Cdc31) in mitochondrial function and biogenesis

机译:对线粒体功能和生物发生的酿酒酵母酿酒酵母CEREVISIAE CENTIN(CDC31)的作用

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摘要

Summary Centrins belong to a family of proteins containing calcium‐binding EF‐hand motifs that perform well‐established roles in centrosome and spindle pole body (SPB) duplication. Yeast encodes a single Centrin protein (Cdc31) that binds components in the SPB. However, further studies revealed a role for Centrins in mRNA export, and interactions with contractile filaments and photoreceptors. In addition, human Centrin‐2 can bind the DNA‐lesion recognition factor XPC, and improve the efficiency of nucleotide excision repair. Similarly, we reported that yeast Cdc31 binds Rad4, a functional counterpart of the XPC DNA repair protein. We also found that Cdc31 is involved in the ubiquitin/proteasome system, and mutations interfere with intracellular protein turnover. In this report, we describe new findings that indicate a role for Cdc31 in the energy metabolism pathway. Cdc31 and cdc31 mutant proteins showed distinct interactions with proteins in energy metabolism, and mutants showed sensitivity to oxidative stress and poor growth on non‐fermentable carbon. Significant alteration in mitochondrial morphology was also detected. Although it is unclear how Cdc31 contributes to so many unrelated mechanisms, we propose that by controlling SPB duplication Centrin proteins might link the cellular responses to DNA damage, oxidative load and proteotoxic stresses to growth control.
机译:总结中心属于含有钙的蛋白质系列,其钙结合的EF手图案,可在中心组和主轴杆体(SPB)复制中表现成熟的作用。酵母编码单个Centrin蛋白(CDC31),其结合SPB中的组分。然而,进一步的研究揭示了在MRNA导出中的中林的作用,以及与收缩丝和感光体的相互作用。此外,人Centrin-2可以结合DNA - 病变识别因子XPC,提高核苷酸切除修复的效率。类似地,我们报道了酵母CDC31结合RAD4,XPC DNA修复蛋白的功能对应物。我们还发现CDC31涉及泛素/蛋白酶体系,突变干扰细胞内蛋白质周转。在本报告中,我们描述了新发现,表明CDC31在能量代谢途径中的作用。 CDC31和CDC31突变蛋白显示出与能量代谢中的蛋白质不同的相互作用,突变体表现出对氧化应激的敏感性和不可发酵碳对较差的增长。还发现了线粒体形态的显着改变。虽然目前尚不清楚CDC31对如此多的无关机制有贡献,但我们提出通过控制SPB重复的Centrin蛋白质可以将细胞反应链接到DNA损伤,氧化载荷和蛋白毒性应力对生长控制。

著录项

  • 来源
    《Molecular Microbiology》 |2018年第5期|共16页
  • 作者单位

    Department of Pharmacology Robert Wood Johnson Medical SchoolRutgers University683 Hoes Lane SPH;

    Center for Advanced Proteomics ResearchNew Jersey Medical School Rutgers University185 S. Orange;

    Center for Advanced Proteomics ResearchNew Jersey Medical School Rutgers University185 S. Orange;

    Department of Pharmacology Robert Wood Johnson Medical SchoolRutgers University683 Hoes Lane SPH;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
  • 关键词

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