Somatic cells undergo a permanent cell cycle arrest, called cellular senescence, after a limited number of cell divisions in vitro. Both the tumor suppressor protein p53 and the stress-response protein p66(shc) are suggested to regulate the molecular events associated with senescence. This study was undertaken to investigate the effect of different oxygen tensions and oxidative stress on cell longevity and to establish the role of p53 and p66(shc) in cells undergoing senescence. As a model of cellular senescence, primary fetal bovine fibroblasts were cultured in either 20% O(2) or 5% O(2) atmospheres until senescence was reached. Fibroblasts cultured under 20% O(2) tension underwent senescence after 30 population doublings (PD), whereas fibroblasts cultured under 5% O(2) tension did not exhibit signs of senescence. Oxidative stress, as measured by protein carbonyl content, was significantly elevated in senescent cells compared to their younger counterparts and to fibroblasts cultured under 5% O(2) at the same PD. p53 mRNA gradually decreased in 20% O(2) cultured fibroblasts until senescence was reached, whereas p53 protein levels were significantly increased as well as p53 phosphorylation on serine 20, suggesting that p53 might be stabilized by posttranslational modifications during senescence. Senescence was also associated with high levels of p66(shc) mRNA and protein levels, while the levels remained low and stable in dividing fibroblasts under 5% O(2) atmosphere. Taken together, our results show an effect of oxidative stress on the replicative life span of fetal bovine fibroblasts as well as an involvement of p53, serine 20-p53 phosphorylation and p66(shc) in senescence.

译文

体细胞在体外进行有限数量的细胞分裂后,会经历永久性的细胞周期停滞,称为细胞衰老。建议抑癌蛋白p53和应激反应蛋白p66(shc) 都可以调节与衰老相关的分子事件。本研究旨在研究不同氧张力和氧化应激对细胞寿命的影响,并确定p53和p66(shc) 在衰老细胞中的作用。作为细胞衰老的模型,在20% O(2) 或5% O(2) 气氛中培养原代胎牛成纤维细胞,直到达到衰老。在20% O(2) 张力下培养的成纤维细胞在30个群体倍增 (PD) 后经历衰老,而在5% O(2) 张力下培养的成纤维细胞没有表现出衰老迹象。与较年轻的对应物和在相同PD下在5% O(2) 下培养的成纤维细胞相比,通过蛋白羰基含量测量的氧化应激在衰老细胞中显着升高。在20% O(2) 培养的成纤维细胞中,p53 mRNA逐渐降低,直到达到衰老,而p53蛋白水平显着增加以及丝氨酸20上的p53磷酸化,这表明p53可能通过衰老过程中的翻译后修饰而稳定。衰老也与高水平的p66(shc) mRNA和蛋白质水平有关,而在5% O(2) 气氛下分裂成纤维细胞时,该水平保持较低且稳定。总之,我们的结果显示氧化应激对胎牛成纤维细胞复制寿命的影响,以及p53,丝氨酸20-p53磷酸化和p66(shc) 参与衰老。

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