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哺乳动物检查点基因RCC1的酵母同源物的过表达抑制了因微管过多而停滞的α-微管蛋白突变类型。

Overexpression of yeast homologs of the mammalian checkpoint gene RCC1 suppresses the class of alpha-tubulin mutations that arrest with excess microtubules.

作者信息

Kirkpatrick D, Solomon F

机构信息

Department of Biology, Massachusetts Institute of Technology, Cambridge 02139.

出版信息

Genetics. 1994 Jun;137(2):381-92. doi: 10.1093/genetics/137.2.381.

Abstract

Microtubules in eukaryotic cells participate in a variety of nuclear and cytoplasmic structures, reflecting functional requirements and cell cycle position. We are studying the cellular regulation of microtubule assembly and organization in the yeast Saccharomyces cerevisiae. We screened for genes that when overexpressed suppress the growth phenotype of conditional mutants in alpha-tubulin that arrest with excess microtubules at the nonpermissive temperature (class 2 mutations). Here we describe one such suppressing element, called ATS1 (for Alpha Tubulin Suppressor). Overexpression of this gene rescues both the growth and microtubule phenotypes of all class 2 mutations, but not the cold-sensitive mutations that arrest with no microtubules (class 1 mutations). Deletion of ATS1 confers a modest slow growth phenotype which is slightly enhanced in strains containing both a deletion of ATS1 and a class 2 tub 1 mutation. The predicted ATS1 protein contains 333 amino acids and has considerable structural homology to the products of both the mammalian mitotic control gene RCC1 and the S. cerevisiae gene SRM1/PRP20. Overexpression of SRM1/PRP20 also suppresses class 2 mutants. The results suggest that this family of genes may participate in regulatory interactions between microtubules and the cell cycle.

摘要

真核细胞中的微管参与多种细胞核和细胞质结构,反映了功能需求和细胞周期阶段。我们正在研究酿酒酵母中微管组装和组织的细胞调控。我们筛选了一些基因,这些基因在过表达时可抑制α-微管蛋白条件突变体的生长表型,这些突变体在非允许温度下因微管过多而停滞(2类突变)。在此,我们描述一种这样的抑制元件,称为ATS1(α-微管蛋白抑制因子)。该基因的过表达可挽救所有2类突变的生长和微管表型,但不能挽救因无微管而停滞的冷敏感突变(1类突变)。删除ATS1会导致适度的生长缓慢表型,在同时缺失ATS1和2类tub1突变的菌株中这种表型会略有增强。预测的ATS1蛋白含有333个氨基酸,与哺乳动物有丝分裂控制基因RCC1和酿酒酵母基因SRM1/PRP20的产物具有相当的结构同源性。SRM1/PRP20的过表达也可抑制2类突变体。结果表明,该基因家族可能参与微管与细胞周期之间的调控相互作用。

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