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Mutations in the yeast cyclin-dependent kinase Cdc28 reveal a role in the spindle assembly checkpoint

机译:酵母细胞周期蛋白依赖性激酶Cdc28中的突变揭示了纺锤体装配检查点的作用

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Anaphase onset and mitotic exit are regulated by the spindle assembly or kinetochore checkpoint, which inhibits the anaphase-promoting complex (APC), preventing the degradation of anaphase inhibitors and mitotic cyclins. As a result, cells arrest with high cyclin-dependent kinase (CDK) activity due to the accumulation of cyclins. Aside from this, a clear-cut demonstration of a direct role for CDKs in the spindle checkpoint response has been elusive. Cdc28 is the main CDK driving the cell cycle in budding yeast. In this report, mutations in cdc28 are described that confer specific checkpoint defects, supersensitivtiy towards microtubule poisons and chromosome loss. Two alleles encode single mutations in the N and C terminal regions, respectively (R10G and R288G), and one allele specifies two mutations near the C terminus (F245L, I284T). These cdc28 mutants are unable to arrest or efficiently prevent sister chromatid separation during treatment with nocodzaole. Genetic interactions with checkpoint and apc mutants suggest Cdc28 may regulate checkpoint arrest downstream of the MAD2 and BUB2 pathways. These studies identify a C-terminal domain of Cdc28 required for checkpoint arrest upon spindle damage that mediates chromosome stability during vegetative growth, suggesting that it has an essential surveillance function in the unperturbed cell cycle.
机译:后期的发生和有丝分裂的退出受纺锤体组件或线粒体检查点的调节,从而抑制后期促进复合物(APC),防止后期抑制剂和有丝分裂细胞周期蛋白的降解。结果,由于细胞周期蛋白的积累,细胞以高细胞周期蛋白依赖性激酶(CDK)活性停滞。除此之外,CDK在主轴检查点响应中直接作用的清晰演示还难以捉摸。 Cdc28是驱动发芽酵母中细胞周期的主要CDK。在此报告中,描述了cdc28中的突变,这些突变赋予特定的检查点缺陷,对微管中毒的超敏性和染色体丢失。两个等位基因分别在N和C末端区域编码单个突变(R10G和R288G),一个等位基因在C末端附近指定两个突变(F245L,I284T)。这些cdc28突变体无法阻止或有效预防用诺古达唑治疗期间姐妹染色单体分离。与检查点和apc突变体的遗传相互作用表明Cdc28可能调节MAD2和BUB2途径下游的检查点停滞。这些研究确定了纺锤体损伤后检查点停滞所需的Cdc28的C末端结构域,该结构域在营养生长过程中介导染色体的稳定性,这表明它在不受干扰的细胞周期中具有重要的监视功能。

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