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腺嘌呤核苷酸对转化的小鼠成纤维细胞的生长抑制是通过细胞外腺苷的产生来实现的。

Growth inhibition of transformed mouse fibroblasts by adenine nucleotides occurs via generation of extracellular adenosine.

作者信息

Weisman G A, Lustig K D, Lane E, Huang N N, Belzer I, Friedberg I

机构信息

Section of Biochemistry, Molecular and Cell Biology, Cornell University, Ithaca, New York 14853.

出版信息

J Biol Chem. 1988 Sep 5;263(25):12367-72.

PMID:2842330
Abstract

The growth of transformed mouse fibroblasts (3T6 cells) in medium containing 5% fetal bovine serum was inhibited after treatment with concentrations greater than 50 microM ATP, ADP, or AMP. Adenosine, the common catabolite of the nucleotides, had no effect on cell growth at concentrations below 1 mM. However, the following results indicate that the toxicity of ATP, ADP, and AMP is mediated by serum- and cell-associated hydrolysis of the nucleotides to adenosine. 1) ADP and AMP, but not ATP, were toxic to 3T6 cells grown in serum-free medium or medium in which phosphohydrolase activity of serum was inactivated. Under these conditions, the cells exhibited cell-associated ADPase and 5'-nucleotidase activity, but little ecto-ATPase activity. 2) Inhibition of adenosine transport in 3T6 cells by dipyridamole or S-(p-nitrobenzyl)-6-thioinosine prevented the toxicity of ATP in serum-containing medium and of ADP and AMP in serum-free medium. 3) A 16-24-h exposure to 125 microM AMP or ATP was needed to inhibit cell growth under conditions where serum- and cell-associated hydrolysis of the nucleotides generated adenosine in the medium continuously over the same time period. In contrast, 125 microM adenosine was completely degraded to inosine and hypoxanthine within 8-10 h. Furthermore, multiple doses of adenosine added to the cells at regular intervals over a 16-h period were significantly more toxic than an equivalent amount of adenosine added in one dose. Treatment of 3T6 cells with AMP elevated intracellular ATP and ADP levels and reduced intracellular UTP levels, effects which were inhibited by extracellular uridine. Uridine also prevented growth inhibition by ATP, ADP, and AMP. These and other results indicate that serum- and cell-associated hydrolysis of adenine nucleotides to adenosine suppresses growth by adenosine-dependent pyrimidine starvation.

摘要

在用浓度大于50微摩尔/升的ATP、ADP或AMP处理后,转化的小鼠成纤维细胞(3T6细胞)在含有5%胎牛血清的培养基中的生长受到抑制。腺苷是核苷酸的常见分解代谢产物,在浓度低于1毫摩尔/升时对细胞生长没有影响。然而,以下结果表明,ATP、ADP和AMP的毒性是由血清和细胞相关的核苷酸水解为腺苷介导的。1)ADP和AMP对生长在无血清培养基或血清磷酸水解酶活性失活的培养基中的3T6细胞有毒性,但ATP没有。在这些条件下,细胞表现出细胞相关的ADP酶和5'-核苷酸酶活性,但外切ATP酶活性很低。2)双嘧达莫或S-(对硝基苄基)-6-硫代肌苷对3T6细胞中腺苷转运的抑制作用可防止含血清培养基中ATP以及无血清培养基中ADP和AMP的毒性。3)在血清和细胞相关的核苷酸水解在同一时间段内持续在培养基中产生腺苷的条件下,需要16 - 24小时暴露于125微摩尔/升的AMP或ATP才能抑制细胞生长。相比之下,125微摩尔/升的腺苷在8 - 10小时内完全降解为肌苷和次黄嘌呤。此外,在16小时内定期向细胞添加多剂量的腺苷比一次性添加等量腺苷的毒性要大得多。用AMP处理3T6细胞会提高细胞内ATP和ADP水平,并降低细胞内UTP水平,细胞外尿苷可抑制这些作用。尿苷还可防止ATP、ADP和AMP对生长的抑制。这些以及其他结果表明,腺嘌呤核苷酸经血清和细胞相关水解为腺苷会通过腺苷依赖性嘧啶饥饿抑制生长。

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