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合胞体胚胎中核的动态排列:细胞骨架网络作用的定量分析。

Dynamic ordering of nuclei in syncytial embryos: a quantitative analysis of the role of cytoskeletal networks.

机构信息

Institute for Biochemistry, Medical School, University of Göttingen, 37077 Göttingen, Germany.

出版信息

Integr Biol (Camb). 2011 Nov;3(11):1112-9. doi: 10.1039/c1ib00059d. Epub 2011 Oct 14.

Abstract

In syncytial embryos nuclei undergo cycles of division and rearrangement within a common cytoplasm. It is presently unclear to what degree and how the nuclear array maintains positional order in the face of rapid cell divisions. Here we establish a quantitative assay, based on image processing, for analysing the dynamics of the nuclear array. By tracking nuclear trajectories in Drosophila melanogaster embryos, we are able to define and evaluate local and time-dependent measures for the level of geometrical order in the array. We find that after division, order is re-established in a biphasic manner, indicating the competition of different ordering processes. Using mutants and drug injections, we show that the order of the nuclear array depends on cytoskeletal networks organised by centrosomes. While both f-actin and microtubules are required for re-establishing order after mitosis, only f-actin is required to maintain the stability of this arrangement. Furthermore, f-actin function relies on myosin-independent non-contractile filaments that suppress individual nuclear mobility, whereas microtubules promote mobility and attract adjacent nuclei. Actin caps are shown to act to prevent nuclear incorporation into adjacent microtubule baskets. Our data demonstrate that two principal ordering mechanisms thus simultaneously contribute: (1) a passive crowding mechanism in which nuclei and actin caps act as spacers and (2) an active self-organisation mechanism based on a microtubule network.

摘要

合胞胚胎中的核经历在共同细胞质内的分裂和重排循环。目前尚不清楚核阵列在面对快速细胞分裂时保持位置顺序的程度和方式。在这里,我们建立了一种基于图像处理的定量分析方法,用于分析核阵列的动力学。通过在黑腹果蝇胚胎中追踪核轨迹,我们能够定义和评估阵列中局部和时间相关的几何有序性度量。我们发现,分裂后,以双相方式重新建立了秩序,表明存在不同的排序过程的竞争。使用突变体和药物注射,我们表明核阵列的顺序取决于由中心体组织的细胞骨架网络。虽然微管和肌动蛋白都需要重新建立有丝分裂后的秩序,但只有肌动蛋白需要维持这种排列的稳定性。此外,肌动蛋白功能依赖于肌球蛋白非收缩丝,该丝抑制单个核的流动性,而微管促进流动性并吸引相邻的核。已经表明肌动蛋白帽可防止核并入相邻的微管篮中。我们的数据表明,两个主要的排序机制同时起作用:(1)一种被动拥挤机制,其中核和肌动蛋白帽作为间隔物;(2)一种基于微管网络的主动自组织机制。

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