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大鼠3Y1细胞温度敏感突变体从G1期和G0期阻滞释放后进入S期所需时间的延长和缩短。

Elongation and shortening of time required for entry into S phase after release from G1 and G0 arrests in temperature-sensitive mutants of rat 3Y1 cells.

作者信息

Zaitsu H, Tanaka H, Kimura G

出版信息

Exp Cell Res. 1987 Jun;170(2):310-21. doi: 10.1016/0014-4827(87)90309-0.

Abstract

Temperature-sensitive (ts) mutants of rat 3Y1 fibroblasts representing four separate complementation groups (3Y1tsD123, 3Y1tsF121, 3Y1tsG125, and 3Y1tsH203) are arrested mainly in the G1 phase when cells of randomly proliferating population at 33.8 degrees C are shifted to 39.8 degrees C (temperature arrest). We examined the time lag of the cellular entry into the S phase after release at 33.8 degrees C, both from the temperature arrest and from the arrest at 33.8 degrees C at a confluent cell density (density arrest). In the temperature-arrested cells, as the duration of temperature arrest increased, the time lag of entry into S phase after shift down to 33.8 degrees C was prolonged, in all four mutants. These observations suggest that the four different functional lesions, each causing arrest in the G1 phase, are also responsible for prolongation of the time lag of entry into the S phase in cells arrested in the G1 phase. The prolongation of the time lag in the temperature-arrested cultures was accelerated at a higher cell density, in medium supplemented with a lower concentration of serum, and at a higher restrictive temperature. In the density-arrested cells, as the duration of pre-exposure to 39.8 degrees C was increased, the time lag of entry into S phase at 33.8 degrees C after release from the arrest was drastically prolonged, in all four mutants. In 3Y1tsF121, 3Y1tsG125, and 3Y1tsH203, when the density-arrested cells were prestimulated by serum at 39.8 degrees C for various periods of time, the time lag of entry into S phase after release from the density arrest at 33.8 degrees C was initially shortened, and then, prolonged progressively as the period of prestimulation increased. These findings, taken together with other data, show that all four ts defects affect cells in states ranging from the deeper resting to mid- or late-G1 phase. It is suggested that events represented by these four mutants are required for entry into the S phase and normally operate in parallel but not in sequence in cells in states ranging from the deeper resting to the mid- or late-G1 phases, though they may affect each other.

摘要

代表四个不同互补组(3Y1tsD123、3Y1tsF121、3Y1tsG125和3Y1tsH203)的大鼠3Y1成纤维细胞温度敏感(ts)突变体,当处于33.8摄氏度随机增殖状态的细胞转移至39.8摄氏度时(温度阻滞),主要停滞在G1期。我们研究了在33.8摄氏度释放后,细胞从温度阻滞以及在汇合细胞密度下于33.8摄氏度阻滞(密度阻滞)进入S期的时间间隔。在温度阻滞的细胞中,随着温度阻滞持续时间增加,在所有四个突变体中,转移至33.8摄氏度后进入S期的时间间隔均延长。这些观察结果表明,这四个不同功能损伤各自导致G1期阻滞,同时也导致处于G1期阻滞的细胞进入S期的时间间隔延长。在温度阻滞培养物中,时间间隔的延长在更高细胞密度、补充较低浓度血清的培养基以及更高限制温度下会加速。在密度阻滞的细胞中,随着预先暴露于39.8摄氏度的持续时间增加,在所有四个突变体中,从阻滞释放后在33.8摄氏度进入S期的时间间隔急剧延长。在3Y1tsF121、3Y1tsG125和3Y1tsH203中,当密度阻滞的细胞在39.8摄氏度用血清预刺激不同时间段时,从33.8摄氏度密度阻滞释放后进入S期的时间间隔最初缩短,然后随着预刺激时间延长而逐渐延长。这些发现与其他数据一起表明,所有四个ts缺陷影响从深度静止到G1期中期或后期等不同状态的细胞。提示这些四个突变体所代表的事件是进入S期所必需的,并且在从深度静止到G1期中期或后期状态的细胞中通常并行而非顺序发挥作用,尽管它们可能相互影响。

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