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依赖动力蛋白的膜收集定义了微管星状体在无细胞提取物的隔离、几何受限体积中的结构和位置。

Dynein-dependent collection of membranes defines the architecture and position of microtubule asters in isolated, geometrically confined volumes of cell-free extracts.

机构信息

Department of Molecular Biology, University of Wyoming, Laramie, WY 82071.

Cell Division & Organization Group, Marine Biological Laboratory, Woods Hole, MA 02543.

出版信息

Mol Biol Cell. 2022 Sep 15;33(11):br20. doi: 10.1091/mbc.E22-03-0074. Epub 2022 Aug 17.

Abstract

It is well established that changes in the underlying architecture of the cell's microtubule (MT) network can affect organelle organization within the cytoplasm, but it remains unclear whether the spatial arrangement of organelles reciprocally influences the MT network. Here we use a combination of cell-free extracts and hydrogel microenclosures to characterize the relationship between membranes and MTs during MT aster centration. We found that initially disperse ER membranes are collected by the aster and compacted near its nucleating center, all while the whole ensemble moves toward the geometric center of its confining enclosure. Once there, aster MTs adopt a bull's-eye pattern with a high-density annular ring of MTs surrounding the compacted membrane core of lower MT density. Formation of this pattern was inhibited when dynein-dependent transport was perturbed or when membranes were depleted from the extracts. Asters in membrane-depleted extracts were able to move away from the most proximal wall but failed to center in cylindrical enclosures with diameters greater than or equal to 150 µm. Taken as whole, our data suggest that the dynein-dependent transport of membranes buttresses MTs near the aster center and that this plays an important role in modulating aster architecture and position.

摘要

众所周知,细胞微管(MT)网络的基础结构的变化会影响细胞质中细胞器的组织,但尚不清楚细胞器的空间排列是否会反过来影响 MT 网络。在这里,我们使用无细胞提取物和水凝胶微室的组合来表征 MT 星状体集中过程中膜和 MT 之间的关系。我们发现,最初分散的 ER 膜被星状体收集并在其成核中心附近压缩,同时整个集合体向其约束室的几何中心移动。一旦到达那里,星状体 MT 采用一种靶心图案,具有高密度的 MT 环形环围绕着 MT 密度较低的压缩膜核心。当依赖于动力蛋白的运输受到干扰或从提取物中耗尽膜时,这种模式的形成会受到抑制。在膜耗尽的提取物中,星状体能够远离最近的壁移动,但在直径大于或等于 150 µm 的圆柱形容器中无法居中。总的来说,我们的数据表明,膜的依赖于动力蛋白的运输在星状体中心附近支撑 MT,并在调节星状体结构和位置方面发挥重要作用。

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