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首页> 外文期刊>Journal of molecular cell biology >Fenton reactions drive nucleotide and ATP syntheses in cancer
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Fenton reactions drive nucleotide and ATP syntheses in cancer

机译:Fenton反应驱动核苷酸和ATP合成癌症

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We present a computational study of tissue transcriptomic data of 14 cancer types to address: what may drive cancer cell division? Our analyses point to that persistent disruption of the intracellular pH by Fenton reactions may be at the root of cancer development. Specifically, we have statistically demonstrated that Fenton reactions take place in cancer cytosol and mitochondria across all the 14 cancer types, based on cancer tissue gene-expression data integrated via the Michaelis-Menten equation. In addition, we have shown that (i) Fenton reactions in cytosol of the disease cells will continuously increase their pH, to which the cells respond by generating net protons to keep the pH stable through a combination of synthesizing glycolytic ATPs and consuming them by nucleotide syntheses, which may drive cell division to rid of the continuously synthesized nucleotides; and (ii) Fenton reactions in mitochondria give rise to novel ways for ATP synthesis with electrons ultimately coming from H2O2, largely originated from immune cells. A model is developed to link these to cancer development, where some mutations may be selected to facilitate cell division at rates dictated by Fenton reactions.
机译:我们介绍了14种癌症类型的组织转录组数据的计算研究:有什么可能推动癌细胞划分?我们的分析指向FENTON反应的细胞内pH的持续破坏可能是癌症发育的根本。具体而言,我们在统计上证明,基于通过Michaelis-Menten方程集成的癌症组织基因表达数据,在所有14种癌症类型中发生芬顿反应在所有14种癌症类型中发生。此外,我们已经表明,(i)疾病细胞的细胞溶溶胶中的芬顿反应将连续增加它们的pH,细胞通过产生净质子来响应细胞通过合成糖酵母ATP和核苷酸消耗它们的组合来保持pH稳定。合成,可以驱使细胞分裂以除去连续合成的核苷酸; (ii)线粒体中的芬顿反应产生了ATP合成的新方法,即最终来自H2O2的电子,主要来自免疫细胞。开发了一种模型,以将这些癌症联系起来,可以选择一些突变以促进由芬顿反应规定的速率下的细胞分裂。

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