首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >PNAS Plus: Kinesin-12 motors cooperate to suppress microtubule catastrophes and drive the formation of parallel microtubule bundles
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PNAS Plus: Kinesin-12 motors cooperate to suppress microtubule catastrophes and drive the formation of parallel microtubule bundles

机译:PNAS Plus:Kinesin-12电机可协同抑制微管灾难并驱动平行微管束的形成

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摘要

Human Kinesin-12 (hKif15) plays a crucial role in assembly and maintenance of the mitotic spindle. These functions of hKif15 are partially redundant with Kinesin-5 (Eg5), which can cross-link and drive the extensile sliding of antiparallel microtubules. Although both motors are known to be tetramers, the functional properties of hKif15 are less well understood. Here we reveal how single or multiple Kif15 motors can cross-link, transport, and focus the plus-ends of intersecting microtubules. During transport, Kif15 motors step simultaneously along both microtubules with relative microtubule transport driven by a velocity differential between motor domain pairs. Remarkably, this differential is affected by the underlying intersection geometry: the differential is low on parallel and extreme on antiparallel microtubules where one motor domain pair becomes immobile. As a result, when intersecting microtubules are antiparallel, canonical transport of one microtubule along the other is allowed because one motor is firmly attached to one microtubule while it is stepping on the other. When intersecting microtubules are parallel, however, Kif15 motors can drive (biased) parallel sliding because the motor simultaneously steps on both microtubules that it cross-links. These microtubule rearrangements will focus microtubule plus-ends and finally lead to the formation of parallel bundles. At the same time, Kif15 motors cooperate to suppress catastrophe events at polymerizing microtubule plus-ends, raising the possibility that Kif15 motors may synchronize the dynamics of bundles that they have assembled. Thus, Kif15 is adapted to operate on parallel microtubule substrates, a property that clearly distinguishes it from the other tetrameric spindle motor, Eg5.
机译:人驱动蛋白12(hKif15)在有丝分裂纺锤体的组装和维护中起着至关重要的作用。 hKif15的这些功能与Kinesin-5(Eg5)部分重叠,后者可以交联并驱动反平行微管的延伸滑动。尽管已知两个马达都是四聚体,但对hKif15的功能特性了解得很少。在这里,我们揭示了单个或多个Kif15电机如何交联,运输和聚焦相交微管的正端。在运输过程中,Kif15电机同时沿着两个微管运动,相对微管运输由电机畴对之间的速度差驱动。值得注意的是,这种差异受下面的相交几何形状的影响:平行时微分低,而一对运动域对不动的反平行微管则微分。结果,当相交的微管是反平行的时,允许一个微管沿着另一个微管的规范运输,因为一个马达在踩踏另一个微管时被牢固地附接到一个微管。但是,当相交的微管平行时,Kif15电机可以驱动(偏置)平行滑动,因为该电机同时踩在它交联的两个微管上。这些微管重排将聚焦于微管正端,并最终导致平行束的形成。同时,Kif15电机协同工作以抑制聚合微管末端的灾难性事件,从而增加了Kif15电机可能同步已组装的束的动力学的可能性。因此,Kif15适用于在平行微管基板上运行,这一特性使它明显区别于其他四聚体主轴电机Eg5。

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