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酿酒酵母中具有类E2F特性的新型DNA结合复合物的细胞周期调控

Cell cycle regulation of a novel DNA binding complex in Saccharomyces cerevisiae with E2F-like properties.

作者信息

Vemu S, Reichel R R

机构信息

Department of Pharmacology and Molecular Biology, Chicago Medical School, North Chicago, Illinois 60064, USA.

出版信息

J Biol Chem. 1995 Sep 1;270(35):20724-9. doi: 10.1074/jbc.270.35.20724.

Abstract

Using a biochemical approach, we have detected an activity in Saccharomyces cerevisiae extract that displays the same DNA binding specificity as the mammalian E2F transcription factor and interacts with TTTCGCGC promoter elements. Additional studies revealed that this factor, termed SCELA (S. cerevisiae E2F-like activity), also binds to the closely related SCB promoter sequences. SCB sites (consensus: TTTCGTG) are involved in the cell cycle regulation of several S. cerevisiae cyclin genes and have been shown to interact with the heterodimeric yeast Swi4-Swi6 complex. However, genetic studies clearly demonstrate that SCELA is not related to Swi4 or Swi6. These experiments imply that SCB sites are able to interact with at least two activities: Swi4-Swi6 and SCELA. Because SCB sites are critical for the periodic activation of cell cycle genes, we asked whether SCELA is regulated during yeast cell cycle. Employing a temperature-sensitive strain, we were able to demonstrate that the DNA binding activity of SCELA oscillates during the cell cycle and reaches its maximum at the transition between the G1 and S phases. Preliminary studies suggest that this fluctuation is mediated by phosphorylation/dephosphorylation events. Further characterization of SCELA by UV cross-linking experiments indicate a molecular mass of 47 kDa for this activity. In addition, we present evidence strongly suggesting that SCELA is actually the DNA binding moiety of a large 300-kDa protein complex. Together, these studies firmly indicate that SCELA (as part of a larger complex) plays a critical role in cell cycle regulation of SCB-containing genes, such as CLN cyclins and HO endonuclease. This hypothesis is consistent with other studies that conclude that the SCB-mediated cell cycle oscillation of CLN cyclins and HO requires activities that are distinct from Swi4-Swi6. Finally, it is worth mentioning that the similarities between SCELA and E2F, which is a crucial component in mammalian cell cycle regulation, extend well beyond the DNA binding specificity. In analogy to E2F, SCELA oscillates during the cell cycle, interacts with other cellular activities, and binds to promoter elements that are known mediators of cell cycle control. We will discuss possible functions for SCELA in yeast cell cycle regulation and its relationship to E2F.

摘要

我们采用生化方法,在酿酒酵母提取物中检测到一种活性,该活性表现出与哺乳动物E2F转录因子相同的DNA结合特异性,并与TTTCGCGC启动子元件相互作用。进一步研究表明,这种因子被称为SCELA(酿酒酵母E2F样活性),也与密切相关的SCB启动子序列结合。SCB位点(共有序列:TTTCGTG)参与了几种酿酒酵母细胞周期蛋白基因的细胞周期调控,并且已被证明与异源二聚体酵母Swi4-Swi6复合物相互作用。然而,遗传学研究清楚地表明SCELA与Swi4或Swi6无关。这些实验表明SCB位点能够与至少两种活性相互作用:Swi4-Swi6和SCELA。由于SCB位点对于细胞周期基因的周期性激活至关重要,我们询问SCELA在酵母细胞周期中是否受到调控。利用一个温度敏感菌株,我们能够证明SCELA的DNA结合活性在细胞周期中振荡,并在G1期和S期之间的转换点达到最大值。初步研究表明这种波动是由磷酸化/去磷酸化事件介导的。通过紫外线交联实验对SCELA的进一步表征表明该活性的分子量为47 kDa。此外,我们提供的证据强烈表明SCELA实际上是一个300 kDa大蛋白复合物的DNA结合部分。总之,这些研究坚定地表明SCELA(作为一个更大复合物的一部分)在含SCB基因(如CLN细胞周期蛋白和HO内切核酸酶)的细胞周期调控中起关键作用。这一假设与其他研究一致,这些研究得出结论,CLN细胞周期蛋白和HO的SCB介导的细胞周期振荡需要不同于Swi4-Swi6的活性。最后,值得一提的是,SCELA与E2F(哺乳动物细胞周期调控中的关键成分)之间的相似性远远超出了DNA结合特异性。与E2F类似,SCELA在细胞周期中振荡,与其他细胞活性相互作用,并与已知的细胞周期控制介质的启动子元件结合。我们将讨论SCELA在酵母细胞周期调控中的可能功能及其与E2F的关系。

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