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两种致癌有机卤代农药溴螨酯和滴滴涕在大鼠体内诱发的早期肝脏变化。

Early hepatic changes induced in rats by two hepatocarcinogenic organohalogen pesticides: bromopropylate and DDT.

作者信息

Kostka G, Kopeć-Szlezak J, Palut D

机构信息

Department of Environmental Toxicology, National Institute of Hygiene and Department of Physiopathology, Institute of Haematology and Blood Transfusion, Warsaw, Poland.

出版信息

Carcinogenesis. 1996 Mar;17(3):407-12. doi: 10.1093/carcin/17.3.407.

Abstract

The aim of the present studies was to describe the effect of two organohalogen pesticides: DDT and bromopropylate, on early changes in rat liver, proposed in the literature to be useful endpoints in screening of non-genotoxic hepatocarcinogens and/or liver tumor promoters. We investigated the effects on the following endpoints: hepatomegaly, mitogenesis (DNA synthesis, mitotic activity, percentage of binuclear cells) and cytochrome CYP2B1-dependent monooxygenase induction. The histological and cytochemical changes in the liver were also recorded. Male Wistar rats received bromopropylate in one, three or five daily oral doses of 125, 250, and 500 mg/kg body wt. day-1. DDT was applied as one, three, and five daily oral doses of 24 mg/kg body wt. day-1 (this dose is close to the mean hepatocarcinogenic dose in male Wistar rats: 34.1 mg/kg body wt. day-1). In the case of both pesticides the early effects observed consisted of hepatomegaly accompanied by an increase in the p-nitroanisole O-demethylase activity and hepatocyte proliferation. Hepatocyte proliferation was elevated during the total experimental period. Vacuolated cytoplasm and evident focal necrosis may suggest that the maximal increase in hepatocyte proliferation, preceding hepatomegaly, is at least partly related to a regenerative liver response to pesticides. In addition to the above-mentioned early changes, the present findings provide new evidence for the occurrence of dose-dependent abnormal mitoses (and c-mitoses) in the hepatocytes of the bromopropylate and DDT treated rats.

摘要

本研究的目的是描述两种有机卤代农药

滴滴涕(DDT)和溴螨酯,对大鼠肝脏早期变化的影响,文献中提出这些变化是筛选非遗传毒性肝癌致癌物和/或肝脏肿瘤促进剂的有用终点。我们研究了对以下终点的影响:肝肿大、有丝分裂(DNA合成、有丝分裂活性、双核细胞百分比)以及细胞色素CYP2B1依赖性单加氧酶诱导。还记录了肝脏的组织学和细胞化学变化。雄性Wistar大鼠每日口服溴螨酯,剂量分别为125、250和500mg/kg体重,给药1、3或5天。滴滴涕每日口服剂量分别为24mg/kg体重,给药1、3和5天(该剂量接近雄性Wistar大鼠的平均致癌剂量:34.1mg/kg体重·天)。对于这两种农药,观察到的早期影响包括肝肿大,同时对硝基苯甲醚O-脱甲基酶活性增加以及肝细胞增殖。在整个实验期间,肝细胞增殖均升高。空泡化细胞质和明显的局灶性坏死可能表明,在肝肿大之前肝细胞增殖的最大增加至少部分与肝脏对农药的再生反应有关。除上述早期变化外,本研究结果还为溴螨酯和滴滴涕处理的大鼠肝细胞中出现剂量依赖性异常有丝分裂(和c-有丝分裂)提供了新证据。

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