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Organization of microtubule assemblies in Dictyostelium syncytia depends on the microtubule crosslinker, Ase1

机译:脉管盘菌合胞体中微管组件的组织取决于微管交联剂Ase1

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摘要

It has long been known that the interphase microtubule (MT) array is a key cellular scaffold that provides structural support and directs organelle trafficking in eukaryotic cells. Although in animal cells, a combination of centrosome nucleating properties and polymer dynamics at the distal microtubule ends is generally sufficient to establish a radial, polar array of MTs, little is known about how effector proteins (motors and crosslinkers) are coordinated to produce the diversity of interphase MT array morphologies found in nature. This diversity is particularly important in multinucleated environments where multiple MT arrays must coexist and function. We initiate here a study to address the higher ordered coordination of multiple, independent MT arrays in a common cytoplasm. Deletion of a MT crosslinker of the MAP65/Ase1/PRC1 family disrupts the spatial integrity of multiple arrays in Dictyostelium discoideum, reducing the distance between centrosomes and increasing the intermingling of MTs with opposite polarity. This result, coupled with previous dynein disruptions suggest a robust mechanism by which interphase MT arrays can utilize motors and crosslinkers to sense their position and minimize overlap in a common cytoplasm.
机译:早已知道,相间微管(MT)阵列是关键的细胞支架,可提供结构支持并指导真核细胞中的细胞器运输。尽管在动物细胞中,中心体成核特性和远端微管末端的聚合物动力学的组合通常足以建立径向,极性的MT阵列,但对于效应蛋白(电机和交联剂)如何协调产生多样性的了解很少自然界发现的相间MT阵列形态这种多样性在多个MT阵列必须共存并起作用的多核环境中尤其重要。我们在这里启动一项研究,以解决常见细胞质中多个独立MT阵列的更高阶协调性。删除MAP65 / Ase1 / PRC1家族的MT交联剂会破坏盘基网柄菌中多个阵列的空间完整性,从而缩短中心体之间的距离并增加极性相反的MT的混合。该结果与先前的动力蛋白破坏相结合,提出了一种稳健的机制,相间MT阵列可利用该机制利用马达和交联剂来感知其位置,并使在普通细胞质中的重叠最小化。

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