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β-微管蛋白突变在体外抑制微管动力学,并在体内减缓有丝分裂。

beta-Tubulin mutation suppresses microtubule dynamics in vitro and slows mitosis in vivo.

作者信息

Sage C R, Davis A S, Dougherty C A, Sullivan K, Farrell K W

机构信息

Department of Biological Sciences, University of California, Santa Barbara 93106, USA.

出版信息

Cell Motil Cytoskeleton. 1995;30(4):285-300. doi: 10.1002/cm.970300406.

Abstract

Microtubule (MT) dynamics vary both spatially and temporally within cells and are thought to be important for proper MT cellular function. Because MT dynamics appear to be closely tied to the guanosine triphosphatase (GTPase) activity of beta-tubulin subunits, we examined the importance of MT dynamics in the budding yeast S. cerevisiae by introducing a T107K point mutation into a region of the single beta-tubulin gene, TUB2, known to affect the assembly-dependent GTPase activity of MTs in vitro. Analysis of MT dynamic behavior by video-enhanced differential interference contrast microscopy, revealed that T107K subunits slowed both the growth rates and catastrophic disassembly rates of individual MTs in vitro. In haploid cells tub2-T107K is lethal; but in tub2-T107K/tub2-590 heterozygotes the mutation is viable, dominant, and slows cell-cycle progression through mitosis, without causing wholesale disruption of cellular MTs. The correlation between the slower growing and shortening rates of MTs in vitro, and the slower mitosis in vivo suggests that MT dynamics are important in budding yeast and may regulate the rate of nuclear movement and segregation. The slower mitosis in mutant cells did not result in premature cytokinesis and cell death, further suggesting that cell-cycle control mechanisms "sense" the mitotic slowdown, possibly by monitoring MT dynamics directly.

摘要

微管(MT)动力学在细胞内随空间和时间而变化,并且被认为对微管的正常细胞功能很重要。由于微管动力学似乎与β-微管蛋白亚基的鸟苷三磷酸酶(GTPase)活性密切相关,我们通过在单个β-微管蛋白基因TUB2的一个区域引入T107K点突变,来研究微管动力学在出芽酵母酿酒酵母中的重要性,该区域已知在体外会影响微管的组装依赖性GTPase活性。通过视频增强微分干涉相差显微镜对微管动态行为进行分析,结果显示T107K亚基在体外减慢了单个微管的生长速率和灾难性解聚速率。在单倍体细胞中,tub2-T107K是致死的;但在tub2-T107K/tub2-590杂合子中,该突变是可行的、显性的,并且减缓了通过有丝分裂的细胞周期进程,而不会导致细胞微管的全面破坏。体外微管生长和缩短速率较慢与体内有丝分裂较慢之间的相关性表明,微管动力学在出芽酵母中很重要,并且可能调节核运动和分离的速率。突变细胞中有丝分裂较慢并未导致过早的胞质分裂和细胞死亡,这进一步表明细胞周期控制机制可能通过直接监测微管动力学来“感知”有丝分裂的减缓。

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