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首页> 外文期刊>Molecular Microbiology >Mycobacterium tuberculosis proteasomal ATPase Mpa has a -grasp domain that hinders docking with the proteasome core protease
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Mycobacterium tuberculosis proteasomal ATPase Mpa has a -grasp domain that hinders docking with the proteasome core protease

机译:结核分枝杆菌蛋白酶体ATP酶MPa具有暗域,其阻碍与蛋白酶体核心蛋白酶的对接

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摘要

Mycobacterium tuberculosis (Mtb) has a proteasome system that is essential for its ability to cause lethal infections in mice. A key component of the system is the proteasomal adenosine triphosphatase (ATPase) Mpa, which captures, unfolds, and translocates protein substrates into the Mtb proteasome core particle for degradation. Here, we report the crystal structures of near full-length hexameric Mtb Mpa in apo and ADP-bound forms. Surprisingly, the structures revealed a ubiquitin-like -grasp domain that precedes the proteasome-activating carboxyl terminus. This domain, which was only found in bacterial proteasomal ATPases, buries the carboxyl terminus of each protomer in the central channel of the hexamer and hinders the interaction of Mpa with the proteasome core protease. Thus, our work reveals the structure of a bacterial proteasomal ATPase in the hexameric form, and the structure finally explains why Mpa is unable to stimulate robust protein degradation in vitro in the absence of other, yet-to-be-identified co-factors.
机译:结核分枝杆菌(MTB)具有一种蛋白酶体系,对于其在小鼠中引起致死感染的能力至关重要。该系统的一个关键组成部分是蛋白酶体三磷酸腺苷酶(ATP酶)MPA,其捕获,展,并进入用于降解的Mtb蛋白酶体核心颗粒易位蛋白底物。在这里,我们在APO和ADP绑定形式中报告了近全长六聚体MTB MPa的晶体结构。令人惊讶的是,该结构揭示了一种泛素状的 - 在蛋白酶体激活羧基末端的域。该域仅在细菌蛋白酶体ATP酶中均在六聚体的中央通道中掩盖了每个引体的羧基末端,并阻碍了MPa与蛋白酶体核心蛋白酶的相互作用。因此,我们的作品揭示了六种形式的细菌蛋白酶体ATP酶的结构,并且该结构最终解释了为什么在没有其他尚未识别的共同因子的情况下,MPA不能在体外刺激鲁棒蛋白质降解。

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  • 来源
    《Molecular Microbiology》 |2017年第2期|共15页
  • 作者

    Wu Yujie; Hu Kuan; Li Defeng; Bai Lin; Yang Shaoqing; Jastrab Jordan B.; Xiao Shuhao; Hu Yonglin; Zhang Susan; Darwin K. Heran; Wang Tao; Li Huilin;

  • 作者单位

    Southern Univ Sci &

    Technol Dept Biol 1088 Xueyuan Rd Shenzhen 518055 Peoples R China;

    Van Andel Res Inst CryoEM Struct Biol Lab Grand Rapids MI 49503 USA;

    Chinese Acad Sci Inst Biophys Natl Lab Biomacromol 15 Datun Rd Beijing 100101 Peoples R China;

    Van Andel Res Inst CryoEM Struct Biol Lab Grand Rapids MI 49503 USA;

    Van Andel Res Inst CryoEM Struct Biol Lab Grand Rapids MI 49503 USA;

    NYU Sch Med Dept Microbiol 450 East 29th St New York NY 10016 USA;

    Southern Univ Sci &

    Technol Dept Biol 1088 Xueyuan Rd Shenzhen 518055 Peoples R China;

    Chinese Acad Sci Inst Biophys Natl Lab Biomacromol 15 Datun Rd Beijing 100101 Peoples R China;

    NYU Sch Med Dept Microbiol 450 East 29th St New York NY 10016 USA;

    NYU Sch Med Dept Microbiol 450 East 29th St New York NY 10016 USA;

    Southern Univ Sci &

    Technol Dept Biol 1088 Xueyuan Rd Shenzhen 518055 Peoples R China;

    Van Andel Res Inst CryoEM Struct Biol Lab Grand Rapids MI 49503 USA;

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  • 正文语种 eng
  • 中图分类 细胞生物学;
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