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首页> 外文期刊>European Journal of Cell Biology: Journal of Deutsche Gesellschaft fur Elektronenmikroskopie: Journal of Deutsche Gesellschaft fur Zellbiologie >Microtubule acetylation regulates dynamics of KIF1C-powered vesicles and contact of microtubule plus ends with podosomes
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Microtubule acetylation regulates dynamics of KIF1C-powered vesicles and contact of microtubule plus ends with podosomes

机译:微管乙酰化调节KIF1C驱动的囊泡的动力学以及微管正端与足囊的接触

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摘要

Microtubule dynamics are important for a variety of key cellular functions such as intracellular trafficking, adjustment of the cell surface proteome, or adhesion structure turnover. In the current study, we investigate the effects of altered microtubule acetylation levels on the subcellular distribution of kinesins and actin cytoskeletal architecture in primary human macrophages. Microtubule acetylation was altered by overexpression or siRNA-induced depletion of the acetylase MEC-17, or by blocking a-tubulin deacetylation by addition of the inhibitor tubacin. We show that microtubule acetylation influences the subcellular distribution of vesicles associated with the kinesin KIF1C, as well as their directionality, velocity and run length. Moreover, tubulin acetylation alters the targeting frequency of microtubule plus ends on podosomes and influences the number of podosomes per cell and thus the matrix-degrading capacity of macrophages. Collectively, our results point to a-tubulin acetylation as an important modification that impacts on kinesin vesicle dynamics, actin cytoskeletal architecture and cellular function of macrophages. (C) 2014 Elsevier GmbH. All rights reserved.
机译:微管动力学对于多种关键细胞功能(例如细胞内运输,细胞表面蛋白质组的调节或粘附结构更新)很重要。在当前的研究中,我们调查了改变的微管乙酰化水平对原代人巨噬细胞中驱动蛋白亚细胞分布和肌动蛋白细胞骨架结构的影响。微管乙酰化可通过过表达或siRNA诱导的乙酰酶MEC-17耗尽来改变,或通过添加抑制剂微蛋白来阻止α-微管蛋白脱乙酰作用来改变。我们显示微管乙酰化影响与驱动蛋白KIF1C相关的囊泡的亚细胞分布,以及它们的方向性,速度和游程长度。此外,微管蛋白乙酰化改变了微管的靶标频率和足小体上的末端,并影响每个细胞中足小体的数目,从而影响巨噬细胞的基质降解能力。总的来说,我们的研究结果表明,微管蛋白乙酰化是一种重要的修饰,可影响驱动蛋白囊泡动力学,肌动蛋白细胞骨架结构和巨噬细胞的细胞功能。 (C)2014 Elsevier GmbH。版权所有。

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