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微管动力学可能体现了一种与原核生物分裂位点机制(极对极振荡)相关的固定双极性形成机制。

Microtubule Dynamics may Embody a Stationary Bipolarity Forming Mechanism Related to the Prokaryotic Division Site Mechanism (Pole-to-Pole Oscillations).

作者信息

Hunding A

机构信息

Chemistry Laboratory III, Department of Chemistry C116, H. C. Ørsted Institute, University of Copenhagen, Universitetsparken 5, DK-2100 Copenhagen, Denmark.

出版信息

J Biol Phys. 2004 Jan;30(4):325-44. doi: 10.1007/s10867-004-3387-7.

Abstract

Cell division mechanisms in eukaryotes and prokaryotes have until recently been seen as being widely different. However, pole-to-pole oscillations of proteins like MinE in prokaryotes are now known to determine the division plane. These protein waves arise through spontaneous pattern forming reaction-diffusion mechanisms, based on cooperative binding of the proteins to a quasistationary matrix (like the cell membrane or DNA). Rather than waves, stationary bipolar pattern formation may arise as well. Some of the involved proteins have eukaryotic homologs (e.g. FtsZ and tubulin), pointing to a possible ancient shared mechanism. Tubulin polymerizes to microtubules in the spindle. Mitotic microtubules are in a highly dynamical state, frequently undergoing rapid shortening (catastrophe), and fragments formed from the microtubule ends are inferred to enhance the destabilization. Here, we show that cooperative binding of such fragments to microtubules may set up a similar pattern forming mechanism as seen in prokaryotes. The result is a spontaneously formed, well controllable, bipolar state of microtubule dynamics in the cell, which may contribute to defining the bipolar spindle.

摘要

直到最近,真核生物和原核生物的细胞分裂机制仍被认为有很大差异。然而,现在已知原核生物中像MinE这样的蛋白质的极到极振荡决定了分裂平面。这些蛋白质波通过自发的模式形成反应-扩散机制产生,该机制基于蛋白质与准静态基质(如细胞膜或DNA)的协同结合。除了波,也可能出现静态双极模式形成。一些相关蛋白质有真核生物同源物(如FtsZ和微管蛋白),这表明可能存在古老的共同机制。微管蛋白在纺锤体中聚合成微管。有丝分裂微管处于高度动态状态,经常经历快速缩短(灾难),并且从微管末端形成的片段被推断会增强去稳定化。在这里,我们表明这些片段与微管的协同结合可能建立一种与原核生物中所见类似的模式形成机制。结果是在细胞中自发形成一种可控的微管动力学双极状态,这可能有助于确定双极纺锤体。

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