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首页> 外文期刊>Current Biology: CB >Myosin-18B Promotes the Assembly of Myosin II Stacks for Maturation of Contractile Actomyosin Bundles
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Myosin-18B Promotes the Assembly of Myosin II Stacks for Maturation of Contractile Actomyosin Bundles

机译:Myosin-18b促进肌球蛋白II堆叠的组装,以便收缩血小杂药束成熟

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摘要

Cell adhesion, morphogenesis, mechanosensing, and muscle contraction rely on contractile actomyosin bundles, where the force is produced through sliding of bipolar myosin II filaments along actin filaments. The assembly of contractile actomyosin bundles involves registered alignment of myosin II filaments and their subsequent fusion into large stacks. However, mechanisms underlying the assembly of myosin II stacks and their physiological functions have remained elusive. Here, we identified myosin-18B, an unconventional myosin, as a stable component of contractile stress fibers. Myosin-18B co-localized with myosin II motor domains in stress fibers and was enriched at the ends of myosin II stacks. Importantly, myosin-18B deletion resulted in drastic defects in the concatenation and persistent association of myosin II filaments with each other and thus led to severely impaired assembly of myosin II stacks. Consequently, lack of myosin-18B resulted in defective maturation of actomyosin bundles from their precursors in osteosarcoma cells. Moreover, myosin-18B knockout cells displayed abnormal morphogenesis, migration, and ability to exert forces to the environment. These results reveal a critical role for myosin-18B in myosin II stack assembly and provide evidence that myosin II stacks are important for a variety of vital processes in cells.
机译:细胞粘附,形态发生,机械沉积和肌肉收缩依赖于收缩型肌肌束,其中通过沿肌动蛋白长丝的双极肌蛋白II长丝滑动产生力。收缩肌肌素束的组装涉及肌球蛋白II长丝的登记对准及其随后的融合成大堆叠。然而,肌球蛋白II堆栈组合的机制及其生理职能仍然难以捉摸。在这里,我们鉴定了一种非常规肌球蛋白的肌蛋白-18b,作为收缩应激纤维的稳定成分。肌球蛋白-18b与霉菌纤维中的肌蛋白II电动机域共同定位,并在肌球蛋白II堆叠的末端富集。重要的是,肌苷-18b缺失导致肌蛋白II长丝彼此串联和持续关联的倾斜缺陷,从而导致肌球蛋白II堆叠的严重损害。因此,缺乏肌球蛋白-18b导致骨肉瘤细胞中的前体缺乏侵略性的肌瘤束的成熟。此外,肌苷-18b敲除细胞显示出异常的形态发生,迁移和施加到环境的能力。这些结果揭示了Myosin-18b在肌球蛋白II堆叠组件中的关键作用,并提供了肌霉素II堆叠对于细胞中各种重要过程很重要。

著录项

  • 来源
    《Current Biology: CB》 |2019年第1期|共17页
  • 作者单位

    Univ Helsinki Inst Biotechnol POB 56 FIN-00014 Helsinki Finland;

    Univ Helsinki Inst Biotechnol POB 56 FIN-00014 Helsinki Finland;

    Vanderbilt Univ Dept Cell &

    Dev Biol Sch Med Nashville TN 37232 USA;

    Harvard Med Sch Beth Israel Deaconess Med Ctr Dept Emergency Med Boston MA 02215 USA;

    Univ Helsinki Inst Biotechnol POB 56 FIN-00014 Helsinki Finland;

    Univ Helsinki Inst Biotechnol POB 56 FIN-00014 Helsinki Finland;

    Harvard Med Sch Beth Israel Deaconess Med Ctr Dept Emergency Med Boston MA 02215 USA;

    Vanderbilt Univ Dept Cell &

    Dev Biol Sch Med Nashville TN 37232 USA;

    Univ Helsinki Inst Biotechnol POB 56 FIN-00014 Helsinki Finland;

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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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