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磷酸二酯酶抑制剂SQ 20006可选择性地阻断p70S6k的丝裂原激活以及细胞分裂周期向S期的转变,而不影响eIF-4E的稳态磷酸化。

The phosphodiesterase inhibitor SQ 20006 selectively blocks mitogen activation of p70S6k and transition to S phase of the cell division cycle without affecting the steady state phosphorylation of eIF-4E.

作者信息

Frost V, Morley S J, Mercep L, Meyer T, Fabbro D, Ferrari S

机构信息

Department of Biochemistry, School of Biological Sciences, University of Sussex, Falmer, Brighton, United Kingdom.

出版信息

J Biol Chem. 1995 Nov 3;270(44):26698-706. doi: 10.1074/jbc.270.44.26698.

DOI:10.1074/jbc.270.44.26698
PMID:7592897
Abstract

In quiescent cells high levels of protein synthesis are required in order to re-enter the cell cycle upon stimulation. Initiation of polypeptide synthesis is the step most often subject to regulation, controlled in part by phosphorylation of 40 S ribosomal protein S6 and a number of initiation factors. The kinase responsible for S6 phosphorylation is p70S6k. We now show that the p70S6k pathway can be selectively blocked by the aminopurine analogue, SQ 20006. This agent is known to raise cAMP levels, resulting in activation of protein kinase A. We present evidence that the increase in cAMP is not responsible for the inhibitory effect observed. We also show that SQ 20006 can prevent the activation of p70S6k in a rapid and reversible manner. The compound does not exert its inhibitory activity on p70S6k but can inhibit in vitro two protein kinase C isozymes (alpha and gamma). In a B lymphoblastoid cell line, treatment with SQ 20006 results in inhibition of protein synthesis at the initiation stage. In contrast, when tested directly upon the translational machinery in the reticulocyte lysate, inhibition is manifest at both the level of initiation and elongation. The role of protein kinase A in the modulation of p70S6k and the rate of translation is discussed.

摘要

在静止细胞中,为了在受到刺激时重新进入细胞周期,需要高水平的蛋白质合成。多肽合成的起始是最常受到调控的步骤,部分受40S核糖体蛋白S6和一些起始因子磷酸化的控制。负责S6磷酸化的激酶是p70S6k。我们现在表明,氨基嘌呤类似物SQ 20006可以选择性地阻断p70S6k途径。已知该试剂可提高cAMP水平,从而导致蛋白激酶A的激活。我们提供的证据表明,cAMP的增加与所观察到的抑制作用无关。我们还表明,SQ 20006可以快速且可逆地阻止p70S6k的激活。该化合物对p70S6k不发挥抑制活性,但可以在体外抑制两种蛋白激酶C同工酶(α和γ)。在B淋巴母细胞系中,用SQ 20006处理会导致起始阶段的蛋白质合成受到抑制。相比之下,当直接在网织红细胞裂解物中的翻译机制上进行测试时,抑制作用在起始和延伸水平均有体现。本文讨论了蛋白激酶A在调节p70S6k和翻译速率中的作用。

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The phosphodiesterase inhibitor SQ 20006 selectively blocks mitogen activation of p70S6k and transition to S phase of the cell division cycle without affecting the steady state phosphorylation of eIF-4E.磷酸二酯酶抑制剂SQ 20006可选择性地阻断p70S6k的丝裂原激活以及细胞分裂周期向S期的转变,而不影响eIF-4E的稳态磷酸化。
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