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No induction of structural chromosomal aberrations in cylindrospermopsin-treated CHO-K1 cells without and with metabolic activation

机译:在没有和有代谢激活的情况下,没有诱导圆柱形精子蛋白酶处理的CHO-K1细胞中的结构染色体畸变

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Cylindrospermopsin (CYN) is a cyanobacterial alkaloid that has been implicated in outbreaks of human morbidity and animal mortality. The principal mode of action for CYN is inhibition of protein and glutathione synthesis, and its toxicity seems to be mediated by cytochrome P-450-generated metabolites. It was also shown that CYN might be responsible for tumor initiation in animals; nevertheless, mechanisms leading to CYN-induced carcinogenesis are scarce and equivocal. The aim of the present study was to investigate the impact of metabolic activation on CYN-induced DNA damage. The effect of different doses of CYN (0.05-2 mu g/ml) on DNA damage was determined in CHO-K1 cells after 3, 16 and 21 h of the treatment. The chromosome aberration assay with and without metabolic activation was applied to evaluate the clastogenic activity of CYN and its metabolite(s). In addition, the occurrence of apoptosis and necrosis was estimated by the annexin method using flow cytometry. The results revealed that CYN is not clastogenic in CHO-K1 cells irrespective of S9 fraction-induced metabolic activation. However, CYN significantly decreases the frequencies of mitotic indices and decreases proliferation irrespective of metabolic activation system. CYN increases the frequency of necrotic cells in a dose- and time-dependent manner, whereas it has a very slight impact on apoptosis. Moreover, the presence of metabolic activation influences a susceptibility to necrotic cell death but not an apoptotic one. (c) 2007 Elsevier Ltd. All rights reserved.
机译:Cylindrospermopsin(CYN)是一种蓝藻生物碱,与人类发病率和动物死亡率暴发有关。 CYN的主要作用方式是抑制蛋白质和谷胱甘肽的合成,其毒性似乎是由细胞色素P-450生成的代谢物介导的。研究还表明,CYN可能是导致动物肿瘤发展的原因。但是,导致CYN致癌作用的机制却很少且模棱两可。本研究的目的是研究代谢活化对CYN诱导的DNA损伤的影响。在处理3、16和21小时后,在CHO-K1细胞中确定不同剂量的CYN(0.05-2μg / ml)对DNA损伤的影响。使用具有和不具有代谢活化的染色体畸变测定法来评估CYN及其代谢产物的致裂活性。另外,通过流式细胞术通过膜联蛋白法估计凋亡和坏死的发生。结果表明,与S9分数诱导的代谢激活无关,CYN在CHO-K1细胞中不是致死的。但是,CYN显着降低了有丝分裂指数的频率并降低了增殖,而与代谢激活系统无关。 CYN以剂量和时间依赖性方式增加坏死细胞的频率,而对细胞凋亡的影响却很小。而且,代谢活化的存在影响坏死细胞死亡的易感性而不影响凋亡的易感性。 (c)2007 Elsevier Ltd.保留所有权利。

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