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大鼠和人类体内叔丁基乙醚的生物转化及排泄动力学

Biotransformation and kinetics of excretion of ethyl tert-butyl ether in rats and humans.

作者信息

Amberg A, Rosner E, Dekant W

机构信息

Institut für Toxikologie, Universität Würzburg, Germany.

出版信息

Toxicol Sci. 2000 Feb;53(2):194-201. doi: 10.1093/toxsci/53.2.194.

Abstract

Ethyl tert-butyl ether (ETBE) may be used in the future as an additive to gasoline to increase oxygen content and reduce tailpipe emissions of pollutants. Therefore, widespread human exposure may occur. To contribute to the characterization of potential adverse effects of ETBE, its biotransformation was compared in humans and rats after inhalation exposure. Human volunteers (3 males and 3 females) and rats (5 males and 5 females) were exposed to 4 (4.5+/-0.6) and 40 (40.6+/-3.0) ppm ETBE for 4 h in a dynamic exposure system. Urine samples from rats and humans were collected for 72 h at 6-h intervals, and blood samples were taken in regular intervals for 48 h. In urine, ETBE and the ETBE-metabolites tert-butanol (t-butanol), 2-methyl-1,2-propane diol, and 2-hydroxyisobutyrate were quantified; ETBE and t-butanol were determined in blood samples. After the end of the exposure period to inhalation of 40-ppm ETBE, blood concentrations of ETBE were found at 5.3+/-1.2 microM in rats and 12.1+/-4.0 microM in humans. The ETBE blood concentrations, after inhalation of 4-ppm ETBE, were 1.0+/-0.7 microM in rats and 1.3+/-0.7 microM in humans. ETBE was rapidly cleared from blood. After the end of the 40-ppm ETBE exposure period, the blood concentrations of t-butanol were 13.9+/-2.2 microM in humans and 21.7+/-4.9 microM in rats. After 4-ppm ETBE exposure, blood concentrations of t-butanol were 1.8+/-0.2 microM in humans and 5.7+/-0.8 microM in rats. t-Butanol was cleared from human blood with a half-life of 9.8+/-1.4 h in humans after 40-ppm ETBE exposure. In urine samples from controls and in samples collected from the volunteers and rats before the exposure, low concentrations of t-butanol, 2-methyl-1,2-propane diol, and 2-hydroxyisobutyrate were present. In the urine of both humans and rats exposed to ETBE, the concentrations of these compounds were significantly increased. 2-Hydroxy-isobutyrate was recovered in urine as the major excretory product formed from ETBE; t-butanol and 2-methyl-1,2-propane diol were minor metabolites. All metabolites of ETBE excreted with urine were rapidly eliminated in both species after the end of the ETBE exposure. Excretion half-lives for the different urinary metabolites of ETBE were between 10.2 and 28.3 h in humans and 2.6 and 4.7 h in rats. The obtained data indicate that ETBE biotransformation and excretion are similar for rats and humans, and that ETBE and its metabolites are rapidly excreted by both species. Between 41 and 53% of the ETBE retained after the end of the exposure was recovered as metabolites in the urine of both humans and rats.

摘要

乙基叔丁基醚(ETBE)未来可能用作汽油添加剂,以增加含氧量并减少汽车尾气污染物排放。因此,人类可能会广泛接触到ETBE。为了有助于了解ETBE潜在的不良影响,对吸入暴露后ETBE在人和大鼠体内的生物转化情况进行了比较。人类志愿者(3名男性和3名女性)和大鼠(5只雄性和5只雌性)在动态暴露系统中分别暴露于4(4.5±0.6)ppm和40(40.6±3.0)ppm的ETBE中4小时。大鼠和人类的尿液样本在72小时内每隔6小时收集一次,血液样本在48小时内定期采集。在尿液中,对ETBE及其代谢产物叔丁醇(t-丁醇)、2-甲基-1,2-丙二醇和2-羟基异丁酸进行了定量分析;在血液样本中测定了ETBE和t-丁醇的含量。在吸入40 ppm ETBE的暴露期结束后,大鼠血液中ETBE的浓度为5.3±1.2微摩尔/升,人类为12.1±4.0微摩尔/升。吸入4 ppm ETBE后,大鼠血液中ETBE的浓度为1.0±0.7微摩尔/升,人类为1.3±0.7微摩尔/升。ETBE能迅速从血液中清除。在40 ppm ETBE暴露期结束后,人类血液中t-丁醇的浓度为13.9±2.2微摩尔/升,大鼠为21.7±4.9微摩尔/升。吸入4 ppm ETBE后,人类血液中t-丁醇的浓度为1.8±0.2微摩尔/升,大鼠为5.7±0.8微摩尔/升。40 ppm ETBE暴露后,t-丁醇在人类血液中的清除半衰期为9.8±1.4小时。在对照组的尿液样本以及志愿者和大鼠暴露前采集的样本中,存在低浓度的t-丁醇、2-甲基-1,2-丙二醇和2-羟基异丁酸。在暴露于ETBE的人和大鼠的尿液中,这些化合物的浓度均显著增加。2-羟基异丁酸是ETBE形成的主要排泄产物;t-丁醇和2-甲基-1,2-丙二醇是次要代谢产物。ETBE暴露结束后,两种物种随尿液排出的所有ETBE代谢产物均迅速被清除。ETBE不同尿液代谢产物的排泄半衰期在人类中为10.2至28.3小时,在大鼠中为2.6至4.7小时。所得数据表明,ETBE在大鼠和人类中的生物转化和排泄情况相似,并且ETBE及其代谢产物在两种物种中均能迅速排泄。暴露结束后保留的ETBE中有41%至53%在人和大鼠的尿液中作为代谢产物被回收。

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