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Susceptibility of lung epithelial cells to alkylating genotoxic insult

机译:肺上皮细胞对烷基化遗传毒性损伤的敏感性

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Alkylation is one of the most common types of DNA damage that can lead to mutations and cancer. Lung is the primary target organ of airborne alkylators such as ethylene oxide (EO). However, the ability of EO to cause lung cancer has not been clearly demonstrated yet. The aim of this study was to investigate the susceptibility of lung cells to alkylating DNA insult by detecting EO-mediated DNA damage with the alkaline comet assay in human lung epithelial cells, peripheral blood lymphocytes, and keratinocytes. The susceptibility of these cell types toward the alkylating insult induced by EO was compared against the oxidative DNA insult induced by hydrogen peroxide (H2O2). Due to the volatility of EO, its active concentrations were monitored by gas chromatography during exposure and were found to decrease significantly in a time-dependent manner. EO induced a statistically significant genotoxic effect at the lowest concentration used (16.4 μM) in lung epithelial cells and in lymphocytes, while in keratinocytes, a genotoxic effect was not detected until 55.5 μM EO. However, lung epithelial cells demonstrated increased resistance to oxidative insult. In fact, oxidative DNA damage detectable by endonuclease treatment was minimal in lung cells compared with the other cell types. These results suggest an increased sensitivity of lung epithelial cells toward the alkylating effects of EO, which was not observed for oxidative DNA damage. Our findings point out the importance of DNA alkylation and the possible role of EO on the induction of lung cancer.
机译:烷基化是最常见的DNA损伤类型之一,可导致突变和癌症。肺是空气中烷基化器(例如环氧乙烷(EO))的主要目标器官。但是,尚未明确证明EO引起肺癌的能力。这项研究的目的是通过用碱性彗星试验检测人肺上皮细胞,外周血淋巴细胞和角质形成细胞中EO介导的DNA损伤,从而研究肺细胞对DNA损伤的烷基化敏感性。将这些细胞类型对由EO引起的烷基化损伤的敏感性与由过氧化氢(H2O2)引起的氧化DNA损伤进行比较。由于EO的挥发性,在暴露过程中通过气相色谱法监测了EO的活性浓度,发现其呈时间依赖性地显着降低。在肺上皮细胞和淋巴细胞中使用最低浓度(16.4μM)的EO,在统计学上具有显着的遗传毒性作用,而在角质形成细胞中,直到55.5μMEO才检测到遗传毒性作用。但是,肺上皮细胞显示出对氧化损伤的抵抗力增强。实际上,与其他细胞类型相比,通过核酸内切酶处理可检测到的氧化DNA损伤在肺细胞中微乎其微。这些结果表明,肺上皮细胞对EO烷基化作用的敏感性增加,而氧化DNA损伤未观察到。我们的发现指出了DNA烷基化的重要性以及EO在肺癌诱导中的可能作用。

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