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Beauvericin and ochratoxin A genotoxicity evaluated using the alkaline comet assay: single and combined genotoxic action.

机译:用碱性彗星试验评估了白僵菌素和A曲霉毒素A的遗传毒性:单一和联合遗传毒性作用。

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摘要

This study was aimed at investigating the genotoxic potential of single beauvericin (BEA) and ochratoxin A (OTA) as well as their interaction in porcine kidney epithelial PK15 cells and human leukocytes using the alkaline comet assay. IC(50) of BEA (5.0 +/- 0.6) and OTA (15.8 +/- 1.5) estimated by MTT reduction assay shows that BEA is three times more toxic than OTA. BEA (0.1 and 0.5 microM) and OTA (1 and 5 microM) were applied alone or in combination of these concentrations for 1 and 24 h in PK15 cells and human leukocytes. Genotoxicity of these toxins to PK15 cells was time- and concentration dependent. After 1 h, significant increase in tail length, tail intensity, tail moment, and abnormal sized tails (AST) was noted upon exposure to 1 muM of OTA alone and BEA + OTA combinations. Single BEA (0.5 microM) and OTA (1 and 5 microM) and their combinations evoked significant DNA damage in PK15 cells, considering all comet tail parameters measured after 24 h of treatment. Human leukocytes were slightly concentration but not time dependent. After 1 h of exposure, there were no significant changes in the tail length. Tail intensity, tail moment, and/or incidence of AST were significantly higher in cells treated with single OTA or BEA and their combinations than in control cells. DNA damage in leukocytes was significantly higher after 24 h of exposure to single toxins and their combinations, considering all comet tail parameters, but these changes were less pronounced than in PK15 cells. Combined toxins showed additive and synergistic effects in PK15 cells, while only additive effects were observed in human leukocytes. Combined prolonged exposure to BEA and OTA in subcytotoxic concentrations through food consumption could induce DNA damage contributing to the carcinogenicity in animals and humans.
机译:这项研究的目的是使用碱性彗星试验研究单一金黄色葡萄球菌素(BEA)和曲毒素A(OTA)的遗传毒性潜力,以及它们在猪肾上皮PK15细胞和人白细胞中的相互作用。通过MTT还原测定法估计的BEA(5.0 +/- 0.6)和OTA(15.8 +/- 1.5)的IC(50)表明BEA的毒性是OTA的三倍。 BEA(0.1和0.5 microM)和OTA(1和5 microM)单独或以这些浓度组合应用在PK15细胞和人白细胞中1和24小时。这些毒素对PK15细胞的遗传毒性取决于时间和浓度。 1小时后,仅接触1μMOTA和BEA + OTA组合,就会发现尾巴长度,尾巴强度,尾巴力矩和异常大小的尾巴(AST)显着增加。考虑到在处理24小时后测得的所有彗尾参数,单个BEA(0.5 microM)和OTA(1和5 microM)及其组合在PK15细胞中引起了明显的DNA损伤。人白细胞浓度稍高,但与时间无关。暴露1小时后,尾巴长度无明显变化。在用单个OTA或BEA及其组合处理的细胞中,尾部强度,尾部力矩和/或AST的发生率显着高于对照细胞。考虑到所有彗星尾巴参数,暴露于单一毒素及其组合24小时后,白细胞中的DNA损伤明显更高,但这些变化不如PK15细胞明显。组合毒素在PK15细胞中表现出加和协同作用,而在人白细胞中仅观察到加和作用。通过食用食物而长时间暴露于亚细胞毒性浓度的BEA和OTA共同可能导致DNA损伤,从而对动物和人类致癌。

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