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酿酒酵母起始特异性转录因子Swi4通过锚蛋白重复序列与有丝分裂Clb2/Cdc28激酶相互作用,并通过其保守的羧基末端与Swi6相互作用。

The Saccharomyces cerevisiae Start-specific transcription factor Swi4 interacts through the ankyrin repeats with the mitotic Clb2/Cdc28 kinase and through its conserved carboxy terminus with Swi6.

作者信息

Siegmund R F, Nasmyth K A

机构信息

Research Institute of Molecular Pathology, Vienna, Austria.

出版信息

Mol Cell Biol. 1996 Jun;16(6):2647-55. doi: 10.1128/MCB.16.6.2647.

Abstract

At a point in late G1 termed Start, yeast cells enter S phase, duplicate their spindle pole bodies, and form buds. These events require activation of Cdc28 kinase by G1 cyclins. Swi4 associates with Swi6 to form the SCB-binding factor complex which activates G1 cyclin genes CLN1 and CLN2 in late G1. In G2 and M phases, the transcriptional activity of SCB-binding factor is repressed by the mitotic Clb2/Cdc28 kinase. Mbp1, a transcription factor related to Swi4, forms the MCB-binding factor complex with Swi6, which activates DNA synthesis genes and S-phase cyclin genes CLB5 and CLB6 in late G1. Clb2/Cdc28 kinase is not required for the repression of MCB-binding factor transcriptional activity in G2 and M phase. We show here that the Swi4 carboxy terminus is sufficient for interaction with Swi6 in vitro. A carboxy-terminal domain of Swi6 is required and sufficient for interaction with Swi4. The carboxy terminus of Mbp1 is sufficient for interaction with Swi6, and the carboxy terminus of Swi6 is required for interaction with Mbp1. By coimmunoprecipitation, we show that Swi4 but not Mbp1 interacts with Clb2/Cdc28 kinase in vivo during the G2 and M phases of the cell cycle. We demonstrate that the ankyrin repeats of Swi4 mediate the interaction with Clb2/Cdc28 kinase. The ankyrin repeats constitute a domain by which a cell cycle-specific transcription factor can interact with cyclin-dependent kinase complexes, thus enabling it to link its transcriptional activity to cell cycle progression.

摘要

在G1晚期的一个称为起始点(Start)的时刻,酵母细胞进入S期,复制其纺锤体极体,并形成芽。这些事件需要G1期细胞周期蛋白激活Cdc28激酶。Swi4与Swi6结合形成SCB结合因子复合物,该复合物在G1晚期激活G1期细胞周期蛋白基因CLN1和CLN2。在G2期和M期,SCB结合因子的转录活性被有丝分裂期的Clb2/Cdc28激酶抑制。Mbp1是一种与Swi4相关的转录因子,它与Swi6形成MCB结合因子复合物,该复合物在G1晚期激活DNA合成基因以及S期细胞周期蛋白基因CLB5和CLB6。在G2期和M期抑制MCB结合因子转录活性不需要Clb2/Cdc28激酶。我们在此表明,Swi4的羧基末端在体外足以与Swi6相互作用。Swi6的一个羧基末端结构域对于与Swi4相互作用是必需的且足够的。Mbp1的羧基末端足以与Swi6相互作用,而Swi6的羧基末端对于与Mbp1相互作用是必需的。通过共免疫沉淀,我们表明在细胞周期的G2期和M期,Swi4而非Mbp1在体内与Clb2/Cdc28激酶相互作用。我们证明Swi4的锚蛋白重复序列介导了与Clb2/Cdc28激酶的相互作用。锚蛋白重复序列构成了一个结构域,通过该结构域细胞周期特异性转录因子能够与细胞周期蛋白依赖性激酶复合物相互作用,从而使其能够将其转录活性与细胞周期进程联系起来。

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