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β-微管蛋白中的突变会破坏秀丽隐杆线虫早期胚胎中的纺锤体定向和微管动力学。

Mutations in a beta-tubulin disrupt spindle orientation and microtubule dynamics in the early Caenorhabditis elegans embryo.

作者信息

Wright Amanda J, Hunter Craig P

机构信息

Department of Molecular and Cellular Biology, Harvard University, Cambridge, Massachusetts 02138, USA.

出版信息

Mol Biol Cell. 2003 Nov;14(11):4512-25. doi: 10.1091/mbc.e03-01-0017. Epub 2003 Aug 22.

DOI:10.1091/mbc.e03-01-0017
PMID:12937270
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC268303/
Abstract

The early Caenorhabditis elegans embryo contains abundant transcripts for two alpha- and two beta-tubulins, raising the question of whether each isoform performs specialized functions or simply contributes to total tubulin levels. Our identification of two recessive, complementing alleles of a beta-tubulin that disrupt nuclear-centrosome centration and rotation in the early embryo originally suggested that this tubulin, tbb-2, has specialized functions. However, embryos from tbb-2 deletion worms do not have defects in nuclear-centrosome centration and rotation suggesting that the complementing alleles are not null mutations. Both complementing alleles have distinct effects on microtubule dynamics and show allele-specific interactions with the two embryonically expressed alpha-tubulins: One of the alleles causes microtubules to be cold stable and resistant to the microtubule-depolymerizing drug benomyl, whereas the other causes cell cycle-specific defects in microtubule polymerization. Gene-specific RNA interference targeting all four embryonically expressed tubulin genes singly and in all double combinations showed that the tubulin isoforms in the early embryo are largely functionally redundant with the exception of tbb-2. tbb-2 is required for centrosome stabilization during anaphase of the first cell division, suggesting that tbb-2 may be specialized for interactions with the cell cortex.

摘要

早期秀丽隐杆线虫胚胎含有大量两种α - 微管蛋白和两种β - 微管蛋白的转录本,这就引发了一个问题:每种亚型是执行特定功能,还是仅仅对微管蛋白总量有贡献。我们鉴定出一种β - 微管蛋白的两个隐性互补等位基因,它们在早期胚胎中破坏核 - 中心体的集中和旋转,这最初表明这种微管蛋白tbb - 2具有特定功能。然而,来自tbb - 2缺失蠕虫的胚胎在核 - 中心体集中和旋转方面没有缺陷,这表明互补等位基因不是无效突变。这两个互补等位基因对微管动力学有不同影响,并与两种胚胎表达的α - 微管蛋白表现出等位基因特异性相互作用:其中一个等位基因使微管对冷稳定,并对微管解聚药物苯菌灵有抗性,而另一个则在微管聚合中导致细胞周期特异性缺陷。针对所有四个胚胎表达的微管蛋白基因单独以及所有双重组合进行的基因特异性RNA干扰表明,早期胚胎中的微管蛋白亚型在功能上基本冗余,tbb - 2除外。tbb - 2在第一次细胞分裂后期对于中心体稳定是必需的,这表明tbb - 2可能专门用于与细胞皮层相互作用。

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本文引用的文献

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PAR proteins regulate microtubule dynamics at the cell cortex in C. elegans.PAR蛋白在秀丽隐杆线虫的细胞皮层调节微管动力学。
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LET-99 determines spindle position and is asymmetrically enriched in response to PAR polarity cues in C. elegans embryos.LET-99决定纺锤体位置,并在秀丽隐杆线虫胚胎中响应PAR极性线索而不对称富集。
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beta-Tubulin C354 mutations that severely decrease microtubule dynamics do not prevent nuclear migration in yeast.严重降低微管动力学的β-微管蛋白C354突变不会阻止酵母中的核迁移。
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