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首页> 外文期刊>Life sciences >Synchronized generation of reactive oxygen species with the cell cycle.
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Synchronized generation of reactive oxygen species with the cell cycle.

机译:与细胞周期同步生成活性氧。

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摘要

A possible appearance of reactive oxygen species (ROS) with the normal cell cycle was studied to find how ROS are generated in cells in relation to the cell cycle. The production of ROS in relation to the cell cycle was examined by determining the changes in intracellular ROS concentrations at different phases of the cell cycle by culturing BALB 3T3 cells in the presence and absence of aphidicolin. The amounts of intracellular ROS and the cell population at specific phases (S and G2/M) were determined as the fluorescence of dichlorodihydrofluorescein and propidium iodide taken up simultaneously by the cells, respectively, by flow cytometry. Although intracellular ROS remained at the control levels when the cell growth was arrested with aphidicolin at the G1 phase, they increased when the arrest was released to result in the increase of the cell population at the S phase. Furthermore, ROS was shown to disturb/stop the cell cycle by means of the MTT (3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl tetrazolium bromide) assay. The cell cycle was regulated through oxidative stress by exposure to hydrogen peroxide and glutathione ethyl ester. The cell cycle was prevented more sensitively in metallothionein-null cells than in the wild type cells. Based on the present observations, we proposed for the first time that ROS are generated synchronously with the normal cell cycle, and that they have to be controlled at certain level for normal progress of the cell cycle.
机译:研究了正常细胞周期中活性氧(ROS)的可能出现,以发现与细胞周期相关的细胞中如何产生ROS。通过在存在和不存在蚜虫的情况下培养BALB 3T3细胞,通过确定细胞周期不同阶段的细胞内ROS浓度的变化来检查与细胞周期相关的ROS的产生。通过流式细胞术分别测定细胞同时摄取的二氯二氢荧光素和碘化丙啶的荧光,确定特定阶段(S和G2 / M)的细胞内ROS的量和细胞群。尽管当细胞生长被Aphidicolin阻止在G1期时,细胞内ROS仍保持在对照水平,但当释放被阻止时,ROS却增加了,导致S期细胞数量的增加。此外,通过MTT(3-(4,5-二甲基噻唑-2-基)-2,5-二苯基溴化四氮唑)测定,ROS被证明干扰/停止了细胞周期。通过暴露于过氧化氢和谷胱甘肽乙酯,通过氧化应激调节细胞周期。在金属硫蛋白无效的细胞中比在野生型细胞中更敏感地防止了细胞周期。基于目前的观察,我们首次提出了与正常细胞周期同步产生的ROS,并且必须将其控制在一定水平才能正常进行细胞周期。

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