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环磷酸腺苷(cAMP)对酿酒酵母应激诱导型p118表达的调节。II. cAMP级联反应突变体中p118表达的研究

Modulation of expression of the stress-inducible p118 of Saccharomyces cerevisiae by cAMP. II. A study of p118 expression in mutants of the cAMP cascade.

作者信息

Verma R, Iida H, Pardee A B

机构信息

Department of Pharmacology, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

J Biol Chem. 1988 Jun 25;263(18):8576-82.

PMID:2837458
Abstract

In the preceding paper, we have identified a protein of Mr = 118,000 which is induced by stress conditions that lead to cessation of DNA synthesis and cell division (Verma, R., Iida, H., and Pardee, A.B. (1988) J. Biol. Chem. 263, 8569-8575). In the current study, we have investigated the possible role this protein may play in cellular proliferation by studying p118 expression in mutants of the cAMP metabolic pathway. The cyr 1-2 mutant gene encodes a thermolabile adenylate cyclase whose activity is only 7% of wild type even at permissive temperatures (23 degrees C). We have found that at 23 degrees C, the G1 period was 5-fold longer in cyr 1-2 than in CYR1+ cells and that p118 was constitutively expressed in these slow cycling mutants. Addition of 8-bromo-cAMP to cyr 1-2 mutants restored growth at both the restrictive and permissive temperatures and resulted in a shut-off in the synthesis of p118. The effect of the analog on p118 expression was rapid, preceding the increase in cell number and percentage-budded cells. In contrast to wild type cells, p118 synthesis was not induced by sulfur starvation in RAS2val19 mutants possessing high levels of adenylate cyclase activity and bcy1 mutants defective in the regulatory subunit of cAMP-dependent protein kinase. A large body of evidence exists supporting a role of cAMP in positive control of cell proliferation. It is therefore possible that conditions which decrease cAMP arrest growth through a chain of events that include p118 induction.

摘要

在前一篇论文中,我们鉴定出一种分子量为118,000的蛋白质,它由导致DNA合成和细胞分裂停止的应激条件所诱导(Verma, R., Iida, H., and Pardee, A.B. (1988) J. Biol. Chem. 263, 8569 - 8575)。在当前的研究中,我们通过研究cAMP代谢途径突变体中的p118表达,来探究这种蛋白质在细胞增殖中可能发挥的作用。cyr 1 - 2突变基因编码一种热不稳定的腺苷酸环化酶,即使在允许温度(23摄氏度)下,其活性也仅为野生型的7%。我们发现,在23摄氏度时,cyr 1 - 2中的G1期比CYR1 +细胞长5倍,并且p118在这些慢循环突变体中组成性表达。向cyr 1 - 2突变体中添加8 - 溴 - cAMP可在限制温度和允许温度下恢复生长,并导致p118合成的关闭。该类似物对p118表达的影响迅速,先于细胞数量和出芽细胞百分比的增加。与野生型细胞相反,在具有高水平腺苷酸环化酶活性的RAS2val19突变体和cAMP依赖性蛋白激酶调节亚基缺陷的bcy1突变体中,p118合成不会被硫饥饿诱导。有大量证据支持cAMP在细胞增殖的正调控中发挥作用。因此,有可能通过包括p118诱导在内的一系列事件,降低cAMP的条件会阻止生长。

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