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烟草BY-2细胞中M/G1界面处皮层微管重组期间γ-微管蛋白的分布

Gamma-tubulin distribution during cortical microtubule reorganization at the M/G1 interface in tobacco BY-2 cells.

作者信息

Kumagai Fumi, Nagata Toshiyuki, Yahara Natsuko, Moriyama Yohsuke, Horio Tetsuya, Naoi Kuniko, Hashimoto Takashi, Murata Takashi, Hasezawa Seiichiro

机构信息

Department of Integrated Biosciences, Graduate School of Frontier Sciences, The University of Tokyo, Kashiwa, Chiba, Japan.

出版信息

Eur J Cell Biol. 2003 Jan;82(1):43-51. doi: 10.1078/0171-9335-00292.

Abstract

Cortical microtubules are considered to regulate the direction of cellulose microfibril deposition. Despite their significant role in determining cell morphology, cortical microtubules completely disappear from the cell cortex during M phase and become reorganized at G1 phase. The mechanism by which these microtubules become properly formed again is, however, still unclear. We have proposed that the origin of cortical microtubules is on the daughter nuclear surface, but further cortical microtubule reorganization occurs at the cell cortex. Hence it is probable that the locations of microtubule organizing centers (MTOCs) are actively changing. However, the actual MTOC sites of cortical microtubules were not clearly determined. In this paper, we have examined the distribution of gamma-tubulin, one of the key molecules of MTOCs in various organisms, during cortical microtubule reorganization using both immunofluorescence and a GFP reporter system. Using a monoclonal antibody (clone G9) that recognizes highly conserved residues in y-tubulin, y-tubulin was found to be constitutively expressed and to be clearly localized to microtubule structures, such as the preprophase bands, spindles, and phragmoplasts, specific to each cell cycle stage. This distribution pattern was confirmed by the GFP reporter system. During cortical microtubule reorganization at the M to G1 transition phase, gamma-tubulin first accumulated at the daughter nuclear surfaces, and then seemed to spread onto the cell cortex along with microtubules elongating from the daughter nuclei. Based on the results, it was confirmed that daughter nuclear surfaces acted as origins of cortical microtubules, and that further reorganization occurred on the cell cortex.

摘要

皮层微管被认为可调节纤维素微纤丝沉积的方向。尽管它们在决定细胞形态方面发挥着重要作用,但皮层微管在M期会从细胞皮层完全消失,并在G1期重新组织。然而,这些微管再次正确形成的机制仍不清楚。我们曾提出皮层微管起源于子核表面,但进一步的皮层微管重组发生在细胞皮层。因此,微管组织中心(MTOC)的位置很可能在积极变化。然而,皮层微管的实际MTOC位点尚未明确确定。在本文中,我们使用免疫荧光和GFP报告系统,研究了MTOC的关键分子之一γ-微管蛋白在皮层微管重组过程中的分布。使用一种识别γ-微管蛋白中高度保守残基的单克隆抗体(克隆G9),发现γ-微管蛋白持续表达,并明确定位于每个细胞周期阶段特有的微管结构,如前期带、纺锤体和成膜体。这种分布模式通过GFP报告系统得到了证实。在从M期到G1期转变阶段的皮层微管重组过程中,γ-微管蛋白首先在子核表面积累,然后似乎随着从子核延伸出的微管扩散到细胞皮层。基于这些结果,证实了子核表面是皮层微管的起源,并且进一步的重组发生在细胞皮层。

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