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光katanin,一种用于局部微管解聚的光遗传学工具。

Opto-katanin, an optogenetic tool for localized, microtubule disassembly.

机构信息

Cell Biology, Neurobiology and Biophysics, Department of Biology, Faculty of Science, Utrecht University, Padualaan, Utrecht 3584 CS, the Netherlands.

Cell Biology, Neurobiology and Biophysics, Department of Biology, Faculty of Science, Utrecht University, Padualaan, Utrecht 3584 CS, the Netherlands; Center for Living Technologies, Eindhoven-Wageningen-Utrecht Alliance, UMC Utrecht, Utrecht 3584 CB, the Netherlands.

出版信息

Curr Biol. 2022 Nov 7;32(21):4660-4674.e6. doi: 10.1016/j.cub.2022.09.010. Epub 2022 Sep 28.

Abstract

Microtubules are cytoskeletal polymers that separate chromosomes during mitosis and serve as rails for intracellular transport and organelle positioning. Manipulation of microtubules is widely used in cell and developmental biology, but tools for precise subcellular spatiotemporal control of microtubules are currently lacking. Here, we describe a light-activated system for localized recruitment of the microtubule-severing enzyme katanin. This system, named opto-katanin, uses targeted illumination with blue light to induce rapid, localized, and reversible microtubule depolymerization. This tool allows precise clearing of a subcellular region of microtubules while preserving the rest of the microtubule network, demonstrating that regulation of katanin recruitment to microtubules is sufficient to control its severing activity. The tool is not toxic in the absence of blue light and can be used to disassemble both dynamic and stable microtubules in primary neurons as well as in dividing cells. We show that opto-katanin can be used to locally block vesicle transport and to clarify the dependence of organelle morphology and dynamics on microtubules. Specifically, our data indicate that microtubules are not required for the maintenance of the Golgi stacks or the tubules of the endoplasmic reticulum but are needed for the formation of new membrane tubules. Finally, we demonstrate that this tool can be applied to study the contribution of microtubules to cell mechanics by showing that microtubule bundles can exert forces constricting the nucleus.

摘要

微管是细胞骨架聚合物,在有丝分裂过程中分离染色体,并作为细胞内运输和细胞器定位的轨道。微管的操纵广泛应用于细胞和发育生物学,但目前缺乏用于精确亚细胞时空控制微管的工具。在这里,我们描述了一种用于局部招募微管切割酶katanin 的光激活系统。该系统名为 opto-katanin,使用蓝色光进行靶向照明,以诱导快速、局部和可逆的微管解聚。该工具允许精确清除微管的亚细胞区域,同时保留其余的微管网络,表明调节katanin 对微管的招募足以控制其切割活性。在没有蓝光的情况下,该工具没有毒性,可用于分解原代神经元和分裂细胞中的动态和稳定微管。我们表明,opto-katanin 可用于局部阻断囊泡运输,并阐明细胞器形态和动力学对微管的依赖。具体而言,我们的数据表明,微管对于高尔基体堆叠或内质网的小管的维持不是必需的,但对于新的膜小管的形成是必需的。最后,我们通过表明微管束可以施加收缩核的力来证明,该工具可用于研究微管对细胞力学的贡献。

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