Departament de Ciències Bàsiques, Facultat de Medicina i Ciències de la Salut, Universitat Internacional de Catalunya, Barcelona, Catalunya, Spain.
Mol Cell Biol. 2013 Apr;33(7):1273-84. doi: 10.1128/MCB.01556-12. Epub 2013 Jan 22.
G1 cyclins, in association with a cyclin-dependent kinase (CDK), are universal activators of the transcriptional G1-S machinery during entry into the cell cycle. Regulation of cyclin degradation is crucial for coordinating progression through the cell cycle, but the mechanisms that modulate cyclin stability to control cell cycle entry are still unknown. Here, we show that a lack of phosphate downregulates Cln3 cyclin and leads to G1 arrest in Saccharomyces cerevisiae. The stability of Cln3 protein is diminished in strains with low activity of Pho85, a phosphate-sensing CDK. Cln3 is an in vitro substrate of Pho85, and both proteins interact in vivo. More interestingly, cells that carry a CLN3 allele encoding aspartic acid substitutions at the sites of Pho85 phosphorylation maintain high levels of Cln3 independently of Pho85 activity. Moreover, these cells do not properly arrest in G1 in the absence of phosphate and they die prematurely. Finally, the activity of Pho85 is essential for accumulating Cln3 and for reentering the cell cycle after phosphate refeeding. Taken together, our data indicate that Cln3 is a molecular target of the Pho85 kinase that is required to modulate cell cycle entry in response to environmental changes in nutrient availability.
G1 周期蛋白与细胞周期蛋白依赖性激酶(CDK)结合,是细胞周期进入过程中 G1-S 转录机器的通用激活剂。细胞周期中周期蛋白降解的调控对于协调细胞周期的进展至关重要,但是调节细胞周期进入的周期蛋白稳定性的机制仍不清楚。在这里,我们表明缺乏磷酸盐会下调 Cln3 周期蛋白并导致酿酒酵母中的 G1 期停滞。在 Pho85 活性低的菌株中,Cln3 蛋白的稳定性降低,Pho85 是一种感知磷酸盐的 CDK。Cln3 是 Pho85 的体外底物,两种蛋白质在体内相互作用。更有趣的是,携带编码 Pho85 磷酸化位点天冬氨酸取代的 CLN3 等位基因的细胞独立于 Pho85 活性而保持高水平的 Cln3。此外,这些细胞在没有磷酸盐的情况下不能正确地在 G1 期停滞,并且过早死亡。最后,Pho85 的活性对于积累 Cln3 和在重新摄取磷酸盐后重新进入细胞周期是必不可少的。总之,我们的数据表明 Cln3 是 Pho85 激酶的分子靶标,它是响应营养物质可用性的环境变化来调节细胞周期进入所必需的。
