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活细胞中微管屈曲的特征描述。

Characterization of microtubule buckling in living cells.

作者信息

Pallavicini Carla, Monastra Alejandro, Bardeci Nicolás González, Wetzler Diana, Levi Valeria, Bruno Luciana

机构信息

Departamento de Física, Facultad de Ciencias Exactas y Naturales, Universidad de Buenos Aires, Pabellón 1, Ciudad Universitaria, 1428, Buenos Aires, Argentina.

Instituto de Ciencias, Universidad Nacional de General Sarmiento, JM Gutiérrez 1150, Los Polvorines, 1613, Buenos Aires, Argentina.

出版信息

Eur Biophys J. 2017 Sep;46(6):581-594. doi: 10.1007/s00249-017-1207-9. Epub 2017 Apr 19.

Abstract

Microtubules are filamentous biopolymers involved in essential biological processes. They form key structures in eukaryotic cells, and thus it is very important to determine the mechanisms involved in the formation and maintenance of the microtubule network. Microtubule bucklings are transient and localized events commonly observed in living cells and characterized by a fast bending and its posterior relaxation. Active forces provided by molecular motors have been indicated as responsible for most of these rapid deformations. However, the factors that control the shape amplitude and the time scales of the rising and release stages remain unexplored. In this work, we study microtubule buckling in living cells using Xenopus laevis melanophores as a model system. We tracked single fluorescent microtubules from high temporal resolution (0.3-2 s) confocal movies. We recovered the center coordinates of the filaments with 10-nm precision and analyzed the amplitude of the deformation as a function of time. Using numerical simulations, we explored different force mechanisms resulting in microtubule bending. The simulated events reproduce many features observed for microtubules, suggesting that a mechanistic model captures the essential processes underlying microtubule buckling. Also, we studied the interplay between actively transported vesicles and the microtubule network using a two-color technique. Our results suggest that microtubules may affect transport indirectly besides serving as tracks of motor-driven organelles. For example, they could obstruct organelles at microtubule intersections or push them during filament mechanical relaxation.

摘要

微管是参与基本生物过程的丝状生物聚合物。它们在真核细胞中形成关键结构,因此确定微管网络形成和维持所涉及的机制非常重要。微管屈曲是活细胞中常见的瞬时局部事件,其特征是快速弯曲及其后续松弛。分子马达提供的主动力被认为是这些快速变形的主要原因。然而,控制形状幅度以及上升和释放阶段时间尺度的因素仍未得到探索。在这项工作中,我们以非洲爪蟾黑素细胞为模型系统,研究活细胞中的微管屈曲。我们从高时间分辨率(0.3 - 2秒)的共聚焦电影中追踪单个荧光微管。我们以10纳米的精度恢复了细丝的中心坐标,并分析了变形幅度随时间的变化。通过数值模拟,我们探索了导致微管弯曲的不同力机制。模拟事件重现了微管观察到的许多特征,表明一个机械模型捕捉到了微管屈曲背后的基本过程。此外,我们使用双色技术研究了主动运输的囊泡与微管网络之间的相互作用。我们的结果表明,微管除了作为马达驱动细胞器的轨道外,可能还会间接影响运输。例如,它们可能在微管交叉处阻碍细胞器,或在细丝机械松弛过程中推动它们。

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