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首页> 外文期刊>Journal of Biophysical and Biochemical Cytology >Altered chemomechanical coupling causes impaired motility of the kinesin-4 motors KIF27 and KIF7
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Altered chemomechanical coupling causes impaired motility of the kinesin-4 motors KIF27 and KIF7

机译:改变的化学机械耦合导致Kinesin-4电机KIF27和KIF7的动力受损

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Kinesin-4 motors play important roles in cell division, microtubule organization, and signaling. Understanding how motors perform their functions requires an understanding of their mechanochemical and motility properties. We demonstrate that KIF27 can influence microtubule dynamics, suggesting a conserved function in microtubule organization across the kinesin-4 family. However, kinesin-4 motors display dramatically different motility characteristics: KIF4 and KIF21 motors are fast and processive, KIF7 and its Drosophila melanogaster homologue Costal2 (Cos2) are immotile, and KIF27 is slow and processive. Neither KIF7 nor KIF27 can cooperate for fast processive transport when working in teams. The mechanistic basis of immotile KIF7 behavior arises from an inability to release adenosine diphosphate in response to microtubule binding, whereas slow processive KIF27 behavior arises from a slow adenosine triphosphatase rate and a high affinity for both adenosine triphosphate and microtubules. We suggest that evolutionarily selected sequence differences enable immotile KIF7 and Cos2 motors to function not as transporters but as microtubule-based tethers of signaling complexes.
机译:Kinesin-4电机在细胞分裂,微管组织和信号传导中起重要作用。了解电机如何执行其功能需要了解其机械化学和运动性能。我们证明KIF27可以影响微管动态,表明在Kinesin-4家族中的微管组织中的保守功能。然而,Kinesin-4电机显着显示出不同的运动特性:KIF4和KIF21电动机快速且加工,KIF7及其果蝇黑素转酯同源性肋骨2(COS2)是Immotile,KIF27缓慢和加工。在团队中工作时,KIF7和KIF27都不能合作快速加工运输。 Immotile KIF7行为的机械基础产生响应于微管结合而无法释放腺苷二磷酸,而慢性加工KIF 27行为由缓慢的腺苷三磷酸酶速率和对腺苷三磷酸腺苷和微管的高亲和力。我们建议进化选择的序列差使得可实现ImpOxile KIF7和COS2电动机,以不作为运输器,而是作为基于微管的信号配合物。

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