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三氯乙烯反应中的物种差异。II. 大鼠和小鼠体内的生物转化

Species differences in response to trichloroethylene. II. Biotransformation in rats and mice.

作者信息

Green T, Prout M S

出版信息

Toxicol Appl Pharmacol. 1985 Jul;79(3):401-11. doi: 10.1016/0041-008x(85)90138-3.

Abstract

Detailed analysis of urine from two strains of rats and mice dosed po with trichloroethylene at four doses from 10 to 2000 mg/kg failed to detect any major species or strain differences in the metabolism of trichloroethylene. Although a greater proportion of the dose was metabolized in mice than in rats, the relative proportions of the major metabolites were very similar in both strains and were unaffected by the dose amount. Analysis of the same urine samples for minor metabolites failed to establish a major species difference. Small amounts of dichloroacetic acid (less than 1% of the dose) were present in both rat and mouse urine and were not considered significant. Monochloroacetic acid accounted for less than 0.1% of the dose. Daily dosing of trichloroethylene (1000 mg/kg po) for 180 days did not induce the overall metabolism of trichloroethylene but did double the urinary excretion of trichloroacetic acid. This finding was accompanied by an equivalent percentage decrease in the concentration of trichloroethanol. CO2 has been shown to be a major metabolite of trichloroacetic acid, suggesting that this is the source of trichloroethylene-derived CO2. Trichloroacetic acid was also excreted in bile in both rats and mice suggesting possible conjugation of this metabolite in the liver. Very little evidence was found for the formation of chemically reactive species from trichloroethylene in either rats or mice and none that could be the basis of a major species difference. The increased rate of metabolism in the mouse, the resulting high blood concentrations of trichloroacetic acid, and stimulation of hepatic peroxisome proliferation in this species appears to be the major species difference possibly related to tumor formation in the liver. The conjugation of trichloroacetic acid and its metabolism to CO2 may be related to peroxisome proliferation.

摘要

对两组分别经口给予10至2000mg/kg四个剂量三氯乙烯的大鼠和小鼠的尿液进行详细分析,未发现三氯乙烯代谢方面存在任何主要的物种或品系差异。虽然小鼠体内代谢的剂量比例高于大鼠,但两种品系中主要代谢物的相对比例非常相似,且不受剂量大小的影响。对相同尿液样本中的次要代谢物进行分析,未发现主要的物种差异。大鼠和小鼠尿液中均存在少量二氯乙酸(剂量的1%以下),认为不具有显著性。一氯乙酸占剂量的比例不到0.1%。每日经口给予三氯乙烯(1000mg/kg),持续180天,并未诱导三氯乙烯的整体代谢,但使三氯乙酸的尿排泄量增加了一倍。这一发现伴随着三氯乙醇浓度同等百分比的下降。二氧化碳已被证明是三氯乙酸的主要代谢产物,表明这是三氯乙烯衍生二氧化碳的来源。三氯乙酸在大鼠和小鼠的胆汁中也有排泄,提示该代谢物可能在肝脏中发生结合。在大鼠或小鼠中,几乎没有证据表明三氯乙烯会形成化学反应性物种,也没有任何证据表明这可能是主要物种差异的基础。小鼠代谢率的增加、由此导致的三氯乙酸高血药浓度以及该物种肝脏过氧化物酶体增殖的刺激,似乎是可能与肝脏肿瘤形成相关的主要物种差异。三氯乙酸的结合及其向二氧化碳的代谢可能与过氧化物酶体增殖有关。

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