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首页> 外文期刊>Toxicology and Applied Pharmacology >Uptake of inorganic and organic derivatives of arsenic associated with induced cytotoxic and genotoxic effects in Chinese hamster ovary (CHO) cells.
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Uptake of inorganic and organic derivatives of arsenic associated with induced cytotoxic and genotoxic effects in Chinese hamster ovary (CHO) cells.

机译:摄入砷的无机和有机衍生物与中国仓鼠卵巢(CHO)细胞的诱导的细胞毒性和遗传毒性相关。

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Humans are exposed to arsenic and their organic derivatives, which are widely distributed in the environment, via food, water, and to a lesser extent, via air. Following uptake, inorganic arsenic undergoes biotransformation to mono- and dimethylated metabolites. Recent findings suggest that the methylation reactions represent a toxification rather than a detoxification pathway. In the present study, the genotoxic effects and the cellular uptake of inorganic arsenic [arsenate, As(i)(V); arsenite, As(i)(III)] and the methylated arsenic species monomethylarsonic acid [[MMA(V)], monomethylarsonous acid [MMA(III)], dimethylarsinic acid [DMA(V)], dimethylarsinous acid [DMA(III)], trimethylarsenic oxide [TMAO(V)] were investigated in Chinese hamster ovary (CHO-9) cells. The chemicals were applied at different concentrations (0.1 muM to 10 mM) for 30 min and 1 h, respectively. Cytotoxic effects were investigated by the trypan blue extrusion test and genotoxic effects by the assessment of micronucleus (MN) induction, chromosome aberrations (CA), and sister chromatid exchanges (SCE). Intracellular arsenic concentrations were determined by ICP-MS techniques. Our results show that MMA(III) and DMA(III) induce cytotoxic and genotoxic effects to a greater extent than MMA(V) or DMA(V). Viability was significantly decreased after incubation (1 h) of the cells with >/= 1 muM As(i)(III), >/= 1 muM As(i)(V), >/= 500 muM MMA(III), >/= 100 muM MMA(V), and 500 muM DMA(V) and >/= 0.1 muM DMA(III). TMAO(V) was not cytotoxic at concentrations up to 10 mM. A significant increase of the number of MN, CA and SCE was found for DMA(III) and MMA(III). As(i)(III + V) induced CA and SCE but no MN. TMAO(V), MMA(V) and DMA(V) were not genotoxic in the concentration range tested (up to 5 mM). The nuclear division index (NDI) was not affected by any of the tested arsenic compounds after a recovery period of 14 to 35 h. When the uptake of the chemicals was measured by ICP-MS analysis, it was found that only 0.03% MMA(V) and DMA(V), and 2% MMA(III), As(i)(III) and (V) were taken up by the cells. In comparison, 10% of the DMA(III) dose was taken up. The total intracellular concentration of all arsenic compounds increased with increasing arsenic concentrations in the culture medium. Taken together, these data demonstrate that arsenic compounds in the trivalent oxidation state exhibit the strongest genotoxic effects. Trivalent organoarsenic compounds are more membrane permeable than the pentavalent species. The potency of the DNA damage decreases in the order DMA(III) > MMA(III) > As(i)(III and V) > MMA(V) > DMA(V) > TMAO(V). We postulate that the induction of genotoxic effects caused by the methylated arsenic species is primarily dependent upon their ability to penetrate cell membranes.
机译:人类会接触到砷及其有机衍生物,这些砷及其有机衍生物通过食物,水以及在较小程度上通过空气在环境中广泛分布。摄取后,无机砷经历生物转化为单和二甲基化的代谢物。最近的发现表明,甲基化反应代表了一种毒化而不是一种解毒途径。在本研究中,遗传毒性作用和无机砷[砷,砷(i)(V);的细胞摄取。亚砷酸盐,As(i)(III)和甲基化的砷物质单甲基ar酸[[MMA(V)],单甲基ar酸[MMA(III)],二甲基ar酸[DMA(V)],二甲基ar酸[DMA(III) ],在中国仓鼠卵巢(CHO-9)细胞中研究了三甲基氧化砷[TMAO(V)]。将化学药品分别以不同浓度(0.1μM至10 mM)施用30分钟和1小时。通过台盼蓝挤压试验研究了细胞毒性作用,并通过评估了微核(MN)诱导,染色体畸变(CA)和姐妹染色单体交换(SCE)评估了遗传毒性作用。细胞内砷浓度通过ICP-MS技术测定。我们的结果表明,与MMA(V)或DMA(V)相比,MMA(III)和DMA(III)诱导的细胞毒性和遗传毒性作用更大。将细胞与> / = 1μMAs(i)(III),> / = 1μMAs(i)(V),> / = 500μMMMA(III)孵育(1 h)后,活力显着降低。 > / = 100μMMMA(V)和500μMDMA(V)和> / = 0.1μMDMA(III)。 TMAO(V)在浓度高达10 mM时无细胞毒性。发现DMA(III)和MMA(III)的MN,CA和SCE数量显着增加。 As(i)(III + V)诱导CA和SCE,但没有MN。在测试的浓度范围内(最高5 mM),TMAO(V),MMA(V)和DMA(V)没有遗传毒性。恢复时间为14至35小时后,核分裂指数(NDI)不受任何测试的砷化合物的影响。通过ICP-MS分析测量化学物质的吸收率时,发现只有0.03%的MMA(V)和DMA(V),以及2%的MMA(III),As(i)(III)和(V)被牢房占用了。相比之下,DMA(III)剂量占10%。所有砷化合物的总细胞内浓度随培养基中砷浓度的增加而增加。综上所述,这些数据表明三价氧化态的砷化合物具有最强的遗传毒性作用。三价有机砷化合物比五价物质更具膜渗透性。 DNA损伤的效力按DMA(III)> MMA(III)> As(i)(III和V)> MMA(V)> DMA(V)> TMAO(V)的顺序降低。我们假设由甲基化砷物质引起的遗传毒性作用的诱导主要取决于它们穿透细胞膜的能力。

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