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芽殖酵母细胞周期突变体cdc25中的大分子合成

Macromolecular syntheses in the cell cycle mutant cdc25 of budding yeast.

作者信息

Martegani E, Vanoni M, Baroni M

出版信息

Eur J Biochem. 1984 Oct 15;144(2):205-10. doi: 10.1111/j.1432-1033.1984.tb08450.x.

Abstract

A major control point of the cell cycle in Saccharomyces cerevisiae is a G1 event called 'start'. At start a yeast cell integrates external and internal signals and decides to progress toward mitosis or to choose alternative pathways such as sporulation, conjugation etc. cdc25 is a class II temperature-sensitive start mutant that blocks at restrictive temperature in G1 as round unbudded cells. The arrest of the cell cycle appears to be independent of the carbon and nitrogen sources, and the cell wall of cdc25-arrested cells shows changes similar to those found in cells undergoing entry in to the stationary phase. After a shift to 36 degrees C the increase in cell number of cdc25 cultures is gradually inhibited. The nuclear division cycle appears to be inhibited immediately after the shift and the percentage of budded cells decreases, while cytoplasmic growth, monitored either as increase of adsorbance at 450 nm or as protein accumulation, continues for many hours leading to a progressive increase of mean cell volume and mean protein content per cell. The stable RNA accumulation instead is immediately inhibited and this is partially due to a 50% inhibition of ribosomal RNA synthesis, while the rate of synthesis of ds-killer RNA is relatively unaffected. These data suggest that the CDC25 gene product could be a part of a mechanism that leads yeast cells to choose between the progression towards DNA replication and cell division or to enter into the stationary phase. This mechanism appears to turn off both rRNA accumulation and cell-cycle progression and to activate differentiative pathways in response to environmental restriction.

摘要

酿酒酵母细胞周期的一个主要控制点是一个名为“起始”的G1期事件。在起始阶段,酵母细胞整合外部和内部信号,并决定是进入有丝分裂,还是选择其他途径,如孢子形成、接合等。cdc25是一种II类温度敏感型起始突变体,在限制温度下会在G1期停滞,细胞呈圆形且未出芽。细胞周期的停滞似乎与碳源和氮源无关,并且cdc25停滞细胞的细胞壁显示出与进入稳定期的细胞中发现的变化相似的变化。转移到36摄氏度后,cdc25培养物中细胞数量的增加逐渐受到抑制。转移后核分裂周期似乎立即受到抑制,出芽细胞的百分比下降,而以450nm处吸光度增加或蛋白质积累来监测的细胞质生长会持续数小时,导致平均细胞体积和每个细胞的平均蛋白质含量逐渐增加。相反,稳定RNA的积累立即受到抑制,这部分是由于核糖体RNA合成受到50%的抑制,而双链杀手RNA的合成速率相对不受影响。这些数据表明,CDC25基因产物可能是一种机制的一部分,该机制导致酵母细胞在向DNA复制和细胞分裂的进程之间做出选择,或者进入稳定期。这种机制似乎会关闭rRNA积累和细胞周期进程,并响应环境限制激活分化途径。

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