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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >An evaluation of the feasibility of using cytogenetic damage as a biomarker for alachlor exposure.
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An evaluation of the feasibility of using cytogenetic damage as a biomarker for alachlor exposure.

机译:使用细胞遗传学损伤作为甲草胺暴露生物标志物的可行性评估。

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Alachlor is a widely used herbicide for which there is significant human exposure, principally through groundwater contamination and inhalation. Because alachlor is purported to be carcinogenic and mutagenic, we initiated studies to determine if induced cytogenetic damage could be used as a biomarker for exposure to this herbicide. Both isolated and whole blood human lymphocytes were exposed to alachlor using several protocols. The lymphocytes were cultured for analysis of sister chromatid exchange (SCE), chromosome aberrations (CAs), micronuclei (MN) in cytochalasin B-induced binucleated cells, and proliferation kinetics using the replicative index (RI). In addition, CD rats were injected with either 10 or 50 mg kg-1 of alachlor, 2-chloro-N-(2,6-diethylphenyl) acetamide (CDEPA) or 2, 6-diethylanaline (DEA). After 24 h, the peripheral blood lymphocytes were removed and cultured for SCE and RI analysis. Alachlor did induce a concentration-related increase in SCE in vitro, but neither it nor its metabolites (CDEPA or DEA) induced a significant increase in SCEs or an alteration of RI in vivo. At the highest in vitro concentration tested, alachlor induced a statistically-significant increase in MN, but no concomitant increase in CAs was seen. From analyses of our data and the literature on alachlor clastogenicity and exposure levels, we concluded that cytogenetic damage may not be an adequately sensitive marker for evaluating human exposure to alachlor. Copyright 1999 Elsevier Science B.V.
机译:甲草胺是一种广泛使用的除草剂,人体主要通过地下水污染和吸入来与之接触。由于甲草胺被认为具有致癌性和致突变性,因此我们启动了研究以确定诱导的细胞遗传学损伤是否可用作暴露于该除草剂的生物标记。使用几种方案将分离的人血和全血人淋巴细胞都暴露于甲草胺。培养淋巴细胞以分析细胞松弛素B诱导的双核细胞中的姐妹染色单体交换(SCE),染色体畸变(CAs),微核(MN),并使用复制指数(RI)分析增殖动力学。此外,给CD大鼠注射10或50 mg kg-1的甲草胺,2-氯-N-(2,6-二乙基苯基)乙酰胺(CDEPA)或2,6-二乙基苯胺(DEA)。 24小时后,除去外周血淋巴细胞并培养用于SCE和RI分析。甲草胺确实在体外诱导了SCE浓度相关的增加,但无论是它还是它的代谢产物(CDEPA或DEA)都没有引起体内SCE的显着增加或RI的改变。在测试的最高体外浓度下,甲草胺诱导了MN的统计学显着增加,但未观察到CA的伴随增加。通过对我们数据的分析以及关于草甘膦致死性和接触水平的文献分析,我们得出结论,细胞遗传学损害可能不是评估人类对甲草胺暴露的足够敏感的标记。版权所有1999 Elsevier Science B.V.

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