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酿酒酵母中未复制染色体的分离揭示了一种新的G1/M期检查点。

Segregation of unreplicated chromosomes in Saccharomyces cerevisiae reveals a novel G1/M-phase checkpoint.

作者信息

Toyn J H, Johnson A L, Johnston L H

机构信息

Laboratory of Yeast Genetics, National Institute for Medical Research, Mill Hill, London, United Kingdom.

出版信息

Mol Cell Biol. 1995 Oct;15(10):5312-21. doi: 10.1128/MCB.15.10.5312.

Abstract

Saccharomyces cerevisiae dbf4 and cdc7 cell cycle mutants block initiation of DNA synthesis (i.e., are iDS mutants) at 37 degrees C and arrest the cell cycle with a 1C DNA content. Surprisingly, certain dbf4 and cdc7 strains divide their chromatin at 37 degrees C. We found that the activation of the Cdc28 mitotic protein kinase and the Dbf2 kinase occurred with the correct relative timing with respect to each other and the observed division of the unreplicated chromatin. Furthermore, the division of unreplicated chromatin depended on a functional spindle. Therefore, the observed nuclear division resembled a normal mitosis, suggesting that S. cerevisiae commits to M phase in late G1 independently of S phase. Genetic analysis of dbf4 and cdc7 strains showed that the ability to restrain mitosis during a late G1 block depended on the genetic background of the strain concerned, since the dbf4 and cdc7 alleles examined showed the expected mitotic restraint in other backgrounds. This restraint was genetically dominant to lack of restraint, indicating that an active arrest mechanism, or checkpoint, was involved. However, none of the previously described mitotic checkpoint pathways were defective in the iDS strains that carry out mitosis without replicated DNA, therefore indicating that the checkpoint pathway that arrests mitosis in iDS mutants is novel. Thus, spontaneous strain differences have revealed that S. cerevisiae commits itself to mitosis in late G1 independently of entry into S phase and that a novel checkpoint mechanism can restrain mitosis if cells are blocked in late G1. We refer to this as the G1/M-phase checkpoint since it acts in G1 to restrain mitosis.

摘要

酿酒酵母的dbf4和cdc7细胞周期突变体在37摄氏度时阻断DNA合成的起始(即它们是iDS突变体),并使细胞周期停滞在1C DNA含量状态。令人惊讶的是,某些dbf4和cdc7菌株在37摄氏度时会分裂其染色质。我们发现,Cdc28有丝分裂蛋白激酶和Dbf2激酶的激活在时间上相互之间以及与观察到的未复制染色质的分裂具有正确的相对顺序。此外,未复制染色质的分裂依赖于功能性纺锤体。因此,观察到的核分裂类似于正常有丝分裂,这表明酿酒酵母在G1晚期独立于S期进入M期。对dbf4和cdc7菌株的遗传分析表明,在G1晚期阻滞期间抑制有丝分裂的能力取决于相关菌株的遗传背景,因为所检测的dbf4和cdc7等位基因在其他背景中显示出预期的有丝分裂抑制作用。这种抑制在遗传上对缺乏抑制是显性的,表明涉及一种活跃的阻滞机制或检查点。然而,在不进行DNA复制就进行有丝分裂的iDS菌株中,先前描述的任何有丝分裂检查点途径都没有缺陷,因此表明在iDS突变体中阻滞有丝分裂的检查点途径是新的。因此,自发的菌株差异表明,酿酒酵母在G1晚期独立于进入S期而进入有丝分裂,并且如果细胞在G1晚期被阻滞,一种新的检查点机制可以抑制有丝分裂。我们将其称为G1/M期检查点,因为它在G1期起作用以抑制有丝分裂。

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