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在大鼠亚慢性喂养研究中,3,3',4,4',5-五氯联苯相对于2,3,7,8-四氯二苯并对二恶英的毒性效力及其联合毒性效力

Toxic potency of 3,3',4,4',5-pentachlorobiphenyl relative to and in combination with 2,3,7,8-tetrachlorodibenzo-p-dioxin in a subchronic feeding study in the rat.

作者信息

Van Birgelen A P, Van der Kolk J, Fase K M, Bol I, Poiger H, Brouwer A, Van den Berg M

机构信息

Research Institute of Toxicology, University of Utrecht, The Netherlands.

出版信息

Toxicol Appl Pharmacol. 1994 Aug;127(2):209-21. doi: 10.1006/taap.1994.1155.

DOI:10.1006/taap.1994.1155
PMID:8048064
Abstract

Toxic and biochemical potencies of 3,3',4,4',5-pentachlorobiphenyl (PCB 126) were studied relative to 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) in a 13-week feeding study in female Sprague-Dawley rats. To study possible interactive effects the combinations of both compounds were administered. The diets were supplemented with PCB 126 (7, 50, or 180 micrograms/kg diet), with TCDD (0.4 or 5 micrograms/kg diet), or with combinations of both compounds. An estimated daily intake of 0.47 micrograms PCB 126/kg body weight/day caused thymic atrophy, a dramatic loss in hepatic retinoids, and a marked induction in CYP1A1 and CYP1A2 activities. At a daily intake of 3.18 micrograms PCB 126/kg body weight/day a decrease in body weight gain, liver enlargement, and plasma thyroid hormone concentrations occurred. Based on a simultaneous subchronic feeding study with TCDD, a toxic equivalency factor range between 0.01 and 0.1 was estimated for PCB 126 for the mentioned effects. Antagonism was found between TCDD and PCB 126 for hepatic retinol levels and CYP1A2 activity. At the same time, TCDD and PCB 126 liver residue levels were slightly decreased by coadministration. However, these antagonistic effects occurred at maximum induction levels of CYP1A1 and CYP1A2, which are not likely to occur at levels relevant for humans.

摘要

在一项针对雌性斯普拉格 - 道利大鼠的为期13周的喂养研究中,研究了3,3',4,4',5 - 五氯联苯(PCB 126)相对于2,3,7,8 - 四氯二苯并 - p - 二恶英(TCDD)的毒性和生化效力。为了研究可能的相互作用,同时给予了两种化合物的组合。饮食中添加了PCB 126(7、50或180微克/千克饮食)、TCDD(0.4或5微克/千克饮食)或两种化合物的组合。估计每日摄入0.47微克PCB 126/千克体重/天会导致胸腺萎缩、肝脏类视黄醇显著减少以及CYP1A1和CYP1A2活性显著诱导。当每日摄入3.18微克PCB 126/千克体重/天时,体重增加减少、肝脏肿大和血浆甲状腺激素浓度出现变化。基于与TCDD同时进行的亚慢性喂养研究,对于上述影响,估计PCB 126的毒性当量因子范围在0.01至0.1之间。在肝脏视黄醇水平和CYP1A2活性方面,发现TCDD和PCB 126之间存在拮抗作用。同时,共同给药会使TCDD和PCB 126的肝脏残留水平略有降低。然而,这些拮抗作用发生在CYP1A1和CYP1A2的最大诱导水平,而在与人类相关的水平下不太可能发生。

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