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细胞培养模型中细胞外过氧化氢和过渡金属离子在抗坏血酸遗传毒性作用中的作用研究。

Investigation of the role of extracellular H2O2 and transition metal ions in the genotoxic action of ascorbic acid in cell culture models.

作者信息

Duarte Tiago L, Almeida Gabriela M, Jones George D D

机构信息

Radiation and Oxidative Stress Group, Department of Cancer Studies and Molecular Medicine, Biocentre, University of Leicester, Leicester LE1 7RH, UK.

出版信息

Toxicol Lett. 2007 Apr 5;170(1):57-65. doi: 10.1016/j.toxlet.2007.02.005. Epub 2007 Feb 20.

Abstract

In the presence of oxygen, ascorbic acid (AA) is unstable in aqueous media and oxidises to dehydroascorbate (DHA), generating reactive intermediates such as ascorbate free radical and H2O2. It is proposed that the cytotoxicity of AA is due to the extracellular production of H2O2 and that this is mediated by transition metal ions present in cell media. Here we investigate the role of extracellular H2O2 and metal ions in the genotoxicity of AA in cell culture models. Our preliminary results confirmed that physiological concentrations of AA were not toxic to confluent human fibroblasts, although they inhibited the proliferation of cells at low density. No inhibition was observed with ascorbic acid 2-phosphate (AA2P), a vitamin C derivative that remains stable in culture media. Furthermore, high concentrations of AA induced DNA strand breakage in a dose-dependent manner, whereas DHA and AA2P were not genotoxic. The genotoxic effect of AA was transient, required the formation of extracellular H2O2 and the presence of intracellular iron, but not of extracellular transition metal ions. These observations further clarify the pro-oxidant effect of AA solutions in cell culture models. The possibility that intravenous administration of high-dose AA may cause a similar genotoxic effect in vivo is discussed.

摘要

在有氧存在的情况下,抗坏血酸(AA)在水性介质中不稳定,会氧化为脱氢抗坏血酸(DHA),生成诸如抗坏血酸自由基和H2O2等反应性中间体。有人提出,AA的细胞毒性是由于细胞外产生H2O2,且这是由细胞培养基中存在的过渡金属离子介导的。在此,我们在细胞培养模型中研究细胞外H2O2和金属离子在AA遗传毒性中的作用。我们的初步结果证实,生理浓度的AA对汇合的人成纤维细胞无毒,尽管它们在低密度时会抑制细胞增殖。抗坏血酸2 - 磷酸酯(AA2P)是一种在培养基中保持稳定的维生素C衍生物,未观察到抑制作用。此外,高浓度的AA以剂量依赖的方式诱导DNA链断裂,而DHA和AA2P没有遗传毒性。AA的遗传毒性作用是短暂的,需要细胞外H2O2的形成和细胞内铁的存在,但不需要细胞外过渡金属离子。这些观察结果进一步阐明了AA溶液在细胞培养模型中的促氧化作用。讨论了静脉注射高剂量AA在体内可能引起类似遗传毒性作用的可能性。

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