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肿瘤细胞中腺苷酸降解与再合成的机制及调控

Mechanism and control of degradation and resynthesis of adenylates in tumour cells.

作者信息

Kovacević Z, Brkljac O, Jerance D

机构信息

Department of Biochemistry, Medical Faculty, Novi Sad, Yugoslavia.

出版信息

Biochem J. 1991 Jan 15;273(Pt 2)(Pt 2):277-81. doi: 10.1042/bj2730277.

Abstract

A comparative study revealed that Ehrlich ascites carcinoma (EAC) cells use glutamine plus inosine for regeneration of adenylates via the purine nucleotide cycle, whereas AS 30D hepatoma cells use adenosine instead. This observation can be correlated with the very low production of aspartate from glutamine in hepatoma cells. Although glucose is an important energy fuel for EAC, it cannot maintain a high enough level of adenylates unless glutamine is also present. Kinetic analysis of hydrolysis of ATP and ADP in the presence of rotenone suggests that deamination of AMP does not maintain a high enough ATP/ADP ratio and probably does not act as energy buffer after inhibition of cell respiration. It seems that, compared with normal cells, malignant cells have the ability for a very rapid regeneration of adenylates. It is proposed that instability of the adenine nucleotide pool, owing to frequent aerobic-anaerobic transitions, represents an essential feature of neoplasia, with profound impact on the whole metabolism of tumour cells.

摘要

一项比较研究表明,艾氏腹水癌细胞(EAC)通过嘌呤核苷酸循环利用谷氨酰胺和肌苷来再生腺苷酸,而AS 30D肝癌细胞则利用腺苷来进行再生。这一观察结果与肝癌细胞中谷氨酰胺生成天冬氨酸的产量极低相关。尽管葡萄糖是EAC的重要能量燃料,但除非同时存在谷氨酰胺,否则它无法维持足够高的腺苷酸水平。在鱼藤酮存在的情况下对ATP和ADP水解的动力学分析表明,AMP的脱氨基作用无法维持足够高的ATP/ADP比值,并且在细胞呼吸受到抑制后可能无法作为能量缓冲物质。与正常细胞相比,恶性细胞似乎具有非常快速地再生腺苷酸的能力。有人提出,由于频繁的有氧-无氧转换导致腺嘌呤核苷酸库不稳定,这是肿瘤形成的一个基本特征,对肿瘤细胞的整体代谢有着深远影响。

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