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人类淋巴细胞在体外接触低浓度的 p,p'-DDT 及其代谢物(p,p'-DDE 和 p,p'-DDD)后的细胞遗传学状态。

Cytogenetic status of human lymphocytes after exposure to low concentrations of p,p'-DDT, and its metabolites (p,p'-DDE, and p,p'-DDD) in vitro.

机构信息

Mutagenesis Unit, Institute for Medical Research and Occupational Health, Ksaverska cesta 2, 10000 Zagreb, Croatia.

出版信息

Chemosphere. 2012 Jun;87(11):1288-94. doi: 10.1016/j.chemosphere.2012.01.037. Epub 2012 Feb 20.

DOI:10.1016/j.chemosphere.2012.01.037
PMID:22354074
Abstract

Despite that the use of DDT has been restricted for more than 40 years to malaria affected areas, low doses of this pesticide and its metabolites DDE and DDD can be found in the environment around the world. Although it has been shown that these pollutants induce cell and DNA damage, the mechanisms of their cytogenotoxic activity remains largely unknown. This study looks into their possible genotoxic effects, at doses that can be found in body fluids, on human lymphocytes using the cytokinesis-block micronucleus assay and the comet assay. After exposure for 1, 6, and 24 h compounds p,p'-DDT (0.1 μg mL(-1)), p,p'-DDE (4.1 μg mL(-1)), and p,p'-DDD (3.9 μg mL(-1)) showed increase in DNA damage. The most significant results were observed at exposure period of 24 h where number of micronucleated cells increased from control 2.5±0.71 to 23.5±3.54, 13.5±0.71, and 16.5±6.36 for DDT, DDE, and DDD, respectively. Similar effect was observed using comet test where the percentage of DNA in comets tail increased from control 1.81±0.16 to 17.24±0.55, 11.21±0.56 and 9.28±0.50 for each compound, respectively. At the same time Fpg-comet assay failed to report induction of oxidative DNA damage of these pollutants. Additionally, the type of cell death was determined using diffusion assay and necrosis dominated. Our findings suggest that even at low concentrations, these pesticides could induce cytogenetic damage to human peripheral blood lymphocytes and in that manner have the impact on human health as well.

摘要

尽管滴滴涕(DDT)的使用已在疟疾疫区被限制超过 40 年,但在世界各地的环境中仍能检测到这种杀虫剂及其代谢物 DDE 和 DDD 的低剂量存在。尽管已经表明这些污染物会导致细胞和 DNA 损伤,但它们的细胞遗传毒性活性的机制在很大程度上仍然未知。本研究使用细胞分裂阻断微核试验和彗星试验,在可在体液中检测到的剂量下,研究了这些污染物对人类淋巴细胞的潜在遗传毒性作用。在暴露 1、6 和 24 小时后,化合物 p,p'-DDT(0.1μg mL(-1))、p,p'-DDE(4.1μg mL(-1))和 p,p'-DDD(3.9μg mL(-1))显示出 DNA 损伤增加。在 24 小时暴露期内观察到最显著的结果,微核细胞数量从对照的 2.5±0.71 增加到 23.5±3.54、13.5±0.71 和 16.5±6.36,分别用于 DDT、DDE 和 DDD。使用彗星试验也观察到类似的效果,彗星尾巴中 DNA 的百分比从对照的 1.81±0.16 增加到 17.24±0.55、11.21±0.56 和 9.28±0.50,分别用于每种化合物。同时,Fpg-彗星试验未能报告这些污染物诱导的氧化 DNA 损伤。此外,使用扩散试验确定细胞死亡的类型,以坏死为主。我们的研究结果表明,即使在低浓度下,这些杀虫剂也可能对人外周血淋巴细胞造成细胞遗传损伤,从而对人类健康产生影响。

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