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转录因子干扰素调节因子-1在催乳素诱导的淋巴细胞细胞周期的G1早期和G1/S转换期间均有表达。

The transcription factor interferon regulatory factor-1 is expressed during both early G1 and the G1/S transition in the prolactin-induced lymphocyte cell cycle.

作者信息

Stevens A M, Yu-Lee L Y

机构信息

Department of Microbiology, Baylor College of Medicine, Houston, Texas 77030.

出版信息

Mol Endocrinol. 1992 Dec;6(12):2236-43. doi: 10.1210/mend.6.12.1491701.

Abstract

PRL induces quiescent Nb2 rat T-lymphoma cells to undergo mitogenesis. Upon PRL stimulation, the transcription factor interferon regulatory factor-1 (IRF-1) is induced as a novel T-cell activation gene in Nb2 cells. Surprisingly, IRF-1 is expressed twice during a single PRL-induced growth cycle: first during the early G1 phase, in an immediate transient peak from 15 min to 2 h, and second during the G1/S phase transition, in a broader peak beginning at 8 h. The unusual biphasic expression of IRF-1 mRNA is accompanied both times by de novo IRF-1 protein synthesis. However, the rate of IRF-1 protein turnover appears to be different in G1 and S phases. IRF-1 protein expressed in G1 exhibits a half-life of about 25 min, whereas in the S phase, the half-life is about 60 min. By washing out PRL at various times during G1, we found a direct correlation among the length of PRL exposure, the second peak of IRF-1 mRNA expression, and DNA synthesis. Our data suggest that PRL and one putative nuclear mediator, IRF-1, may be important in two distinct phases of the cell cycle: first in cell cycle activation, and then in S phase progression.

摘要

催乳素可诱导静止的Nb2大鼠T淋巴瘤细胞发生有丝分裂。在催乳素刺激下,转录因子干扰素调节因子-1(IRF-1)作为Nb2细胞中一种新的T细胞激活基因被诱导表达。令人惊讶的是,IRF-1在单个催乳素诱导的生长周期中表达两次:第一次在G1期早期,在15分钟至2小时内出现一个即时短暂峰值;第二次在G1/S期转换时,在8小时开始出现一个更宽的峰值。IRF-1 mRNA这种不寻常的双相表达在两个阶段均伴随着IRF-1蛋白的从头合成。然而,IRF-1蛋白的周转速度在G1期和S期似乎有所不同。在G1期表达的IRF-1蛋白半衰期约为25分钟,而在S期,半衰期约为60分钟。通过在G1期的不同时间洗脱催乳素,我们发现催乳素暴露时间的长短、IRF-1 mRNA表达的第二个峰值与DNA合成之间存在直接关联。我们的数据表明,催乳素和一种假定的核介质IRF-1可能在细胞周期的两个不同阶段起重要作用:首先在细胞周期激活阶段,然后在S期进展阶段。

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