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Motor protein-driven unidirectional transport of micrometer-sized cargoes across isopolar microtubule arrays

机译:电机蛋白驱动的等离子微管阵列中微米级货物的单向运输。

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Conventional kinesin is a motor protein which translocates organelles from cell centre to cell periphery along specialized filamentous tracks, called microtubules. The direction of translocation is determined by microtubule polarity. This process of biological force generation can be simulated outside cells with kinesin-coated particles actively moving along immobilized microtubules. The in vitro approaches of kinesin-mediated transport described so far had the disadvantage that concerning their polarity the microtubles were randomly distributed resulting in random transport direction. The present paper demonstrates the unidirectional translocation of kinesin-coated cargoes across arrays of microtubules aligned not only in a geometrically parallel but also in an isopolar fashion. As cargo, glass, gold, and polystyrene beads with diameters between 1 and 10 #mu#m were used. Independent of material and size, these beads were observed to move unidirectionally with average velocities of 0.3-1.0 #mu#m s~(-1) over distances up to 2.2 mm. Moreover, the isopolar microtubule arrays even enabled the transport of large flat glass particles with an area of up to 24 #mu#m X 12 #mu#m and 2-5 #mu#m thickness which obviously contacted more than one microtubule. The controlling transport direction is considered to be an essential step for future developments of motor protein-based microdevices working in nanometer steps.
机译:常规的驱动蛋白是一种运动蛋白,沿着特定的丝状径迹(称为微管)将细胞器从细胞中心转移到细胞外围。易位的方向由微管极性决定。可以在细胞外用驱动蛋白包被的颗粒沿着固定的微管主动移动来模拟这种生物力生成过程。迄今为止描述的驱动蛋白介导的运输的体外方法具有的缺点是,关于其极性,微管是随机分布的,从而导致随机的运输方向。本文证明了驱动蛋白包被的货物在微管阵列上的单向转运不仅以几何平行而且以等极性方式排列。作为货物,使用直径在1到10#μm之间的玻璃,金和聚苯乙烯珠。不受材料和尺寸的影响,观察到这些珠子以0.3-1.0#mu#m s〜(-1)的平均速度在最大2.2 mm的距离上单向移动。而且,等极性微管阵列甚至能够输送面积最大为24#mu#m X 12#mu#m和2-5#mu#m厚度的大型平板玻璃颗粒,显然它们接触了一个以上的微管。控制运输方向被认为是纳米级工作的基于运动蛋白的微器件未来发展的必不可少的步骤。

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